- Email: [email protected]
The Etiology and Pathophysiology of Testicular Dysfunction in Man*
Vol. 29, No.5, May 1978 Printed in U.SA.
FERTILITY AND STERILITY Copyright • 1978 The American Fertility Society
THE ETIOLOGY AND PATHOPHYSIOLOGY OF TESTICULAR DYSFUNCTION IN MAN*
EMIL STEINBERGER, M.D.t
Department of Reproductive Medicine and Biology, The University of Texas Medical School at Houston, Houston, Texas 77025
As it will become apparent throughout this review, a peculiar phenomenon is occurring in the area of medicine dealing with the study of testicular disorders. More is being learned about pathophysiologic mechanisms of testicular disease than about its etiology. In other words, we are recognizing and uncovering physiologic mechanisms which, when disturbed, may easily serve as the basis of testicular disease; however, in many ifnot most instances, we'are unable to find the etiologic factors leading to the disturbance. Consequently, we are hampered in establishing specific diagnoses, and as a result therapy is frequently unsuccessful. In this brief review an attempt is made to correlate the available information concerning testicular pathophysiology with the possible etiologic factors involved in testicular dysfunction. The etiologic factors are arbitrarily divided into the following categories: (1) environmental, (2) systemic, (3) intratesticular, and (4) iatrogenic. ENVIRONMENTAL ETIOLOGY OF TESTICULAR DYSFUNCTION
Exposure to Noxious Substances The pathophysiology of testicular disorders resulting from exposure to noxious substances depends entirely on the type of agent causing the disturbance. Workers employed in the manufacture of stilbestrol (a synthetic estrogen capable of suppressing the hypothalami~-pituitary axis)
may inadvertently be exposed to sufficient quantities of this estrogen to develop impotence and testicular atrophy. Thus, the pathophysiology of testicular damage in these cases is hypogonadotropism, resulting in atrophy of both the Leydig cells and seminiferous epithelium. Numerous other· chemical agents-deuterium oxide, cadmium, fiuoroacetamide, various cytotoxic agents (e.g., nitrofurans,. dinitropyrroles, diamines, a-chlorohydrin, various insecticides, and rodenticides) (for review, see references 1 and 2)can produce testicular damage. The pathophysiology of the damage resulting from exposure to these agents varies depending upon the agent employed. Some cause microvascular damage with subsequent ischemia and necrosis of the seminiferous tubule and of the interstitial area (e.g., cadmium), while others produce arrest of spermatogenesis by direct action on the seminiferous tubules (e.g., nitrofurans, dinitropyrroles). Some still unidentified agents discharged into or created in the environment by modern technology may have similarly deleterious effects on the testes. Unfortunately, it is very difficult to establish such a relationship in a patient with testicular dysfunction. In most instances the affected individual may not even be aware of having been exposed to the offending agent. If the damage is due to a chronic low-dose exposure, the morphologic change in the testes subsequent to such a . long-term effect may be nonspecific and easily classified as "adult seminiferous tubule failure."
Received November 17, 1977. cited in this review, the experimental studies by the author were supporteq. by National Insitutes of Health Grants 5 P50 HD 08338 and HD 06316 and by grants from The Ford Foundation and The Clayton Foundation. tReprint requests: Emil Steinberger, M.D.; Department of Reproductive Medicine and Biology, University of Texas Medical School, P.O. Box 20708, Houston, Tex. 77025.
Exposure to Radiation
*As
The deleterious effects of various forms of irradiation on spermatogenesis have been clearly demonstrated both in experimental animals and in man (for review, see reference 3). The pathophysiology of testicular damage following ex-
481
482
STEINBERGER
posure to radiation, however, is still not clearly understood. Damage to chromatin material resulting from ionizations at the target sites may cause a variety of mutations, including "lethal mutation" which results in the death of the affected germ cell. If the "stem cells" of the germ cell line are affected, irreversible destruction of the seminiferous epithelium takes place, and no recovery will occur; At lower rates of radiation the stem cells may not be affected but the more mature cells may, and a maturation depletion of the seminiferous epithelium will occur; followed in time by repopulation of the seminiferous epithelium resulting from mitotic activity of the stem cells. Although the resulting gametes may exhibit normal fertilizing capacity, in some instances the resulting embryo dies and is resorbed in utero. In other instances an apparently normal offspring may result. The possibility that such an offspring may carry mutant genes as an effect of the exposure of the stem cell to radiation is ever-present, as has been demonstrated in experiments in lower species (for review, see reference 4). Emotional Stress Some authors have suggested the possibility that emotional stress may trigger testicular dysfunction. Most of the information in man, particularly as related to the effect of emotional stress on sperm production, is essentially anecdotal in nature. However, several well-documented recent studies have suggested that emotional stress may adversely affect androgen production by the testes. 5·9 It is not known whether the diminution of androgen production in these individuals is also associated with diminished sperm production. Experiments in animals have suggested that "social stress" related to excessive population densities may result in testicular dysfunction and diminished fertility, most likely via the adrenalpituitary-hypothalamic feedback mechanism. 1°-12 Consequently, if emotional factors are indeed involved in causing testicular dysfunction, the pathophysiology of this process most likely involves inadequate gonadotropin stimulation of testicular functions. In general, there is considerable evidence that environmental factors, whether chemical, physical, or emotional, may adversely affect testicular function in men. Unfortunately, in most instances it is extremely difficult to detect and/or to relate a specific environmental factor to the testicular dysfunction in a specific patient. On the other hand, in most patients with testicular disease character-
May 1978
ized by inadequate sperm production, neither can a specific diagnosis be established nor the etiologic factor uncovered. Most of these patients are placed in the diagnostic wastebasket of "adult seminiferous tubule failure." Environmental factors, so difficult to pinpoint, may indeed be the underlying etiologic factors in a segment of a patient population with the diagnosis of "adult seminiferous tubule failure." SYSTEMIC ETIOLOGY OF TESTICULAR DYSFUNCTION
Metabolic No overt and direct relationships have been established between well-defined metabolic-endocrine disorders (e.g., diabetes, hypo- or hyperthyroidism, hypo- or hyperadrenocorticism, disorders of calcium metabolism or lipid metabolism) and testicular dysfunction; however, numerous papers have been written suggesting deleterious effects of metabolic derangements on testicular function in lower species and men (for review, see reference 1). Both hypoglycemia13 and hyperglycemia l4 • 15 have been reported to cause seminiferous epithelium damage in rodents. No definite relationship has been shown between diabetes (whether uncontrolled with the hyperglycemic state prevailing or associated with frequent hypoglycemic episodes) and oligospermia. The possible negative effect of adrenal dysfunction on sperm production has been suggested, but no definite data are available to substantiate this possibility. Considerable attention has been devoted to the possible association of hypothyroidism and diminished sperm production. Although patients with severe hypothyroidism may also show testicular dysfunction, a definite relationship between levels of thyroid hormone and spermatogenesis has been difficult to establish. Again it must be emphasized that in the vast majority of patients with oligo- or azoospermia no serious metabolic disturbance can be detected. Infectious Mumps orchitis is the classic example of testicular dysfunction secondary to a specific infection. During the acute stage, a severe inflammatory response of the gonad associated with increased temperature of the organ, marked swelling, and pain is noted. Subsequently, variable degrees of testicular atrophy may occur,t6 primarily due to .destruction. of a portion or all of theseminiferous epithelium; usually the Leydig cells remain
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
functional. Characteristically the damage to the seminiferous tubules is patchy. Some crosssections of seminiferous tubules show complete spermatogenesis while others show varying degrees of spermatogenic arrest or complete destruction of the seminiferous epithelium. Depending on the severity of damage, the sperm output in these patients will be affected to varying degrees. In most instances, only one testis is severely affected, and sperm production by the other may be sufficient to result in an ejaculate with adequate sperm density. Although this condition is relatively common, the pathophysiology of the damage to the seminiferous epithelium is not clearly understood. There is no evidence that the seminiferous epithelium is directly affected by the virus. Most likely the infectious process is limited to the interstitial area of the testes, and the damage to the seminiferous tubules is due to increased temperature and intratesticular pressure secondary to the edema in the interstitial area. Possibly as a result of the inflammatory process, anatomical and physiologic changes occur in the interstitial tissue, resulting in disruption of normal relationships between the interstitial area and the seminiferous tubules. Although common systemic infections have not been demonstrated to produce clinical manifestations of orchitis or damage to the seminiferous epithelium, evidence in the clinical literature suggests that systemic infections as well as infections in the sex accessories (prostate, seminal vesicles) may be associated with transient (or at times even permanent) diminution of sperm output, possibly associated with subclinical testicular disease. 17-21 It is a distinct possibility that some cases of "adult seminiferous tubule failure" represent the end result of a series of subclinical orchidites secondary to systemic infections.
Vascular Ischemic. Interference with the blood supply to the testis results in severe damage, primarily to the seminiferous epithelium. It should be remembered, however, that the seminiferous epithelium has the potential for adequate recovery even after relatively prolonged periods of ischemia (60 to 90 minutes), but chronic ischemia causes irreversible damage. 22 , 23 Evidence for the possibility that arteriosclerotic changes affecting the intratesticular arterioles may cause seminiferous epithelium damage and gradual diminution of testicular function associated with aging has been reported. 24
483
Vascular Abnormalities. The most common vascular abnormality is the varicocele, sometimes associated with diminution of sperm production and sperm motility. At this time neither the pathophysiology of the spontaneously occurring varicocele nor the mechanism by which it produces testicular damage is clear. The dilatation of the pampiniform plexus of veins is due to the backflow of blood secondary to incompetent valves in the spermatic vein. 25- 29 The mechanism responsible for the valvular incompetence is unclear. The fact that the spermatic vein empties into the renal vein at a right angle has been suggested as a contributing factor, acting in concert with increased orthostatic pressure in the spermatic vein secondary to man's upright position. 28 While these suggestions are plausible, they have not been proved experimentally, and no explanation has been given for the fact that only a small segment of the population develops this problem in spite of the fact that these anatomical and postural relationships exist in most men. The mechanism by which varicocele exerts its postulated effect on the testes is similarly unclear. Originally it was suggested that the dilated veins simply insulate the testis, causing elevation of intratesticular temperature which in turn produces thermal damage to the testes. 30 ,31 This rather plausible suggestion has not been borne out in studies involving direct measurements of intratesticular temperature in patients with varicocele. 32 , 33 It has also been suggested that, since the spermatic vein empties into the renal vein in close proximity to the adrenal vein, the backflow of blood rich in adrenal secretions may expose the testes to high concentrations of adrenal hormones, particularly cortisol, which may be deleterious to testicular function. 27 Measurement of cortisol levels in the blood of the pampiniform plexus resulted in the accumulation of controversial data which at this time are difficult to interpret. 29 Clearly, products of adrenal secretion other than cortisol could also find their way to the testes, and this possibility awaits further study. Finally, the possibility that the pathophysiology of testicular damage in patients with varicocele may be based on physical rather than biochemical phenomena must be considered. Since the testis is surrounded by a relatively inelastic capsule and the testicular parenchyma is under slight pressure, inadequate venous drainage from the testes may induce an increase in intratesticular pressure. There is considerable
484
STEINBERGER
evidence suggesting that increased intratesticular pressure (as, for example, secondary to an inflammatory process) may induce seminiferous epithelium damage. This mechanism conceivably may be involved in the damage produced by a varicocele (for review, see reference 34). Neurologic The role of the nervous system in testicular function (both endocrine and exocrine) is not known. Although anatomical aspects of the nerve supply to the testes have been studied extensively and a relationship of the testes to the autonomic nervous system has been established, there is still controversy over whether the seminiferous epithelium has a nerve supply.35.36 Furthermore, no experimental studies have been conducted to demonstrate whether interruption of the nerve adversely affects the testis. Damage to the seminiferous epithelium and to the Leydig cells has been noted in patients with paraplegia. 37 . 38 Whether the damage is caused by the nerve lesions or other factors is unclear. Suggestions have been made that the anatomical relationships of the lower extremities in these patients cause elevation of temperature and that the lesions in the seminiferous epithelium are secondary to the relative hyperthermia. Developmental Testicular ectopia is the most common type of developmental abnormality affecting the testes. A discussion of the pathophysiology of this condition requires consideration of two factors: the mechanisms responsible for abnormal testicular descent and those responsible for damage to the seminiferous epithelium in the affected testis. Arrest of descent (abdominal, inguinal, or "high riding" testes) and inappropriate descent (crural, suprapubic, or perineal testes) have been considered to be the result of a developmental anatomical abnormality in the path of testicular descent. 39 The damage to the seminiferous epithelium is thought to be secondary to elevated ambient temperature. However, some authors have suggested that both faulty descent and germinal epithelium pathology are due to a congenital testicular abnormality.4°-42 One line of evidence frequently cited in support of this hypothesis is the presence of abnormalities of the seminiferous epithelium in the contralateral scrotal testis in patients with unilateral testicular ectopia. The other evidence to support a congenital etiology is
May 1978
the singularly limited success in preventing the development of abnormalities of the seminiferous epithelium in ectopic testes replaced surgically (orchidopexy) into the scrotums of young (4- to 6year-old) boys. Although thermal damage to the germinal epithelium of abdominal testes must be considered one of the pathophysiologic mechanisms responsible for spermatogenesis, underlying congenital or genetic defects may also be contributory in a least some instances. Genetic
Chromosomal. The classic example of this type of disorder is Klinefelter's syndrome. 43 The abnormality is characterized by the presence of supernumerary sex chromosomes, resulting most commonly in a 47,XXY karyotype. The testicular abnormality in these patients is expressed primarily by defective function of the seminiferous tubules, although a degree of interference with normal androgen production has also been noted. 44 Originally it was thought that the abnormalities in the seminiferous tubules were due to lack of male germ cell development in the embryo because of the "feminizing" effect of an X chromosome. However, studies of testes from prepuberal boys with the diagnosis of Klinefelter's syndrome revealed the presence of gonocytes (stem cells), which gradually diminished in numbers with age. 45 Furthermore, in the testes of adults with Klinefelter's syndrome, patchy areas of spermatogenesis have been noted. 46 . 47 These findings demonstrate that aspermatogenesis in Klinefelter's syndrome is not due to a lack of germ stem cells, but to the inability of most of these cells during testicular development to enter the spermatogenic process and form a mature seminiferous epithelium. Consequently, an abnormality of the spermatogenic process associated with degeneration of the stem cells is the underlying pathophysiology of aspermatogenesis in patients with Klinefelter's syndrome. The possibility that this defect may be related to local insufficiency of testosterone is unlikely: the capacity of testicular tissue from patients with Klinefelter's syndrome to form testosterone in vitro is actually greater than that of normal tissue,48 and the intratesticular concentration of testosterone is higher (although the production rate and ability to respond to gonadotropins is diminished48 . 49). No information is available concerning the biochemical basis for the defective development of the stem cells in testes from patients with Klinefelter's syndrome. Available
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
evidence suggests that in fetal gonads the supporting cells (which, in the male, are the precursors of the Sertoli cells) may play a determinant role in the development of gonadal sex. A possibility thus exists that in patients with an abnormal complement of sex chromosomes a resulting defect in the Sertoli cells may be the underlying pathology of the aspermatogenic state. Testicular pathology associated with other forms of chromosomal abnormalities has been reported. The pathophysiology in these states is understood even less than in Klinefelter's syndrome, and a direct relationship between the chromosomal abnormality and testicular damage has not been firmly established. Biochemical. The testicular feminization syndrome may fall under this category of genetically based systemic biochemical abnormalities associated with dysfunction of the seminiferous tubules. Patients with this syndrome are genetic males and their testes produce testosterone,50, 51 but the target tissues are unable to respond to it because of lack of androgen receptors. 52 These individuals have the physical appearance offemales but have male levels of circulating testosterone. The lack of appropriate development of the seminiferous epithelium may be a reflection of the inability of testosterone to exert its action on testicular tissue and could also be due to the ectopic position of the testes in patients with this syndrome.
Nutritional Testicular damage resulting from specific nutritional deficiencies has been demonstrated experimentally in a variety of mammals. In man there is definite evidence for testicular dysfunction only in cases of chronic starvation and malnutrition. Deleterious effects of vitamin (A and E) deficiency on the seminiferous epithelium have been shown in the rat, but in man no adequate evidence exists to suggest similar relationships.53 Hypothalamic-Pituitary No specific testicular lesions have been described in patients with failure of thyroid-stimulating hormone or adrenocorticotropic hormone. However, inadequate levels of circulating gonadotropins are associated with abnormalities of testicular function in patients with hypothalamic or pituitary disease. Gonadotropins are necessary
485
for both androgen production and formation of spermatozoa. The deficiency syndrome associated with hypogonadotropism is characterized in an adult male by atrophy of Leydig cells with the resulting lack of androgen production and arrest of spermatogenesis. Replacement therapy with both gonadotropins (interstitial cell-stimulating hormone [lCSH] and follicle-stimulating hormone [FSH]) results in stimulation of growth of the Leydig cells, stimulation of androgen production, and stimulation of spermatogenesis in both hypog~nadotropic eunuchs and in patients with hypogonadism secondary to hypophysectomy. 54, 55 Consequently, the pathophysiology of this disorder is simple hormonal (gonadotropin) deficiency. The best available data suggest that ICSH exerts its effect primarily if not exclusively on the Leydig cells. FSH, on the other hand, is apparently responsible for supporting the process of spermiogenesis in the developing immature testis and the process of reinitiation of spermatogenesis in adult testes. Testosterone maintains spermatogenesis in hypophysectomized animals. The administration of testosterone to hypophysectomized men or to hypogonadotropic eunuchs fails to maintain or initiate spermatogenesis. Species differences have been considered as a possible explanation for this phenomenon. However, this may not necessarily be the only explanation, or even a correct one. Maintenance of spermatogenesis in the hypophysectomized rat requires approximately 4 to 8 mg/kg/day of testosterone. Extrapolation to a 70-kg man suggests a dose of 300 to 600 mg/man! day. In no instance has such a high daily dose been administered to a human for a prolonged period of time. Recently it has been shown that the intratesticular levels of testosterone in man are 10- to 100-fold the circulating levels. 48 A similar relationship has been demonstrated in lower species. 56 The minimal intratesticular concentration of testosterone essential for maintaining spermatogenesis is considerably higher than the normal levels in circulation. These findings suggest that a relatively high intratesticular concentration of androgens is required for the spermatogenic process to proceed, and that below a minimal threshold level the spermatogenic process breaks down. Furthermore, the possibility exists that the threshold varies in different individuals. If this turns out to be the case and if methods are developed to determine the threshold, therapeutic approaches are available to increase androgens to the necessary levels (for review, see reference 57).
486
STEINBERGER INTRATESTICULAR ETIOLOGY OF TESTICULAR DYSFUNCTION
Environmental and systemic factors probably play an important etiologic role in only a small percentage of patients with oligo-azoospermia and/or infertility. This leads one to believe that primary intratesticular abnormalities could be responsible for defective spermatogenesis. In the past 5 to 10 years numerous possible sites for biochemically based pathologic processes capable of causing abnormalities of spermatogenesis have been identified in the dual testicular functions of steroidogenesis and spermatogenesis. Steroidogenesis The principal sites of androgen production in the testis are the Leydig cells. The embryonal origin of these cells and the details of their development are not clearly understood, particularly in man. They are probably of mesenchymal origin, 58. 59 and, if one can extrapolate from the lower species, undergo a complicated process of differentiation from both a morphologic60• 61 and a steroidogenic (for review, see reference 62) viewpoint. After attaining maturity they apparently do not divide actively, if at all. Their multiplication, maturation, and steroid biosynthetic activity are under direct control of ICSH, although some evidence has been presented suggesting that FSH may also playa role in this process (for review, see reference 63). Before examining the possible sites where pathophysiology may occur, one must first have a clear understanding of normal Leydig cell function. Although many gaps still exist in our knowledge, considerable advances have been made recently, and a simplified scheme of these processes can be proposed. A great deal of this information has been derived from lower species, although some of the key points have also been observed directly or indirectly to occur in human testes. The first molecular 'event in the chain of events leading to formation of androgens is the interaction of the gonadotropin horinone ICSH with a specific membrane recept-or. on a cell in the interstitial area of the testis, which ultimately will become a mature Leydig cell. The receptor is composed of two parts, .thereceptor site· and a transducer, adenyl cyclase. The message received by the receptor site activates adenyl cyclase to. stimulate production of cyclic adenosine 3':5'-monophosphate(cAMP). The end result of the increased production of this nucl!,!otjde Js
May 1978
to induce multiplication and differentiation of the Leydig cells. Mechanisms involved in this process are unknown, except for the fact that they are probably mediated via a nuclear transcriptional and translation mechanism leading to de novo RNA and protein synthesis. It is doubtful that a substantial proportion of patients with seminiferous tubule abnormalities has a disorder related to inappropriate somatic differentiation of Leydig cells, because in the vast majority of patients the Leydig cell can be seen and no morphologic abnormality in growth and differentiation can be detected. On the other hand, evidence has begun to accumulate that the biochemical events involved in the biogenesis of androgens may indeed be abnormal in some of these patients. Since androgens are essential for both initiation and maintenance of spermatogenesis, an abnormality in this process may be an etiologic factor in some of the cases of "idiopathic adult seminiferous tubule failure." The mechanism ICSH~receptor~cAMP stimulation is also involved in steroidogenesis. ICSH must be bound to the receptor before a steroidogenic effect is induced. Furthermore, a steroidogenic effect can be induced in the absence of ICSH by cAMP, implicating this nucleotide in the mechanism of ICSH action on steroidogenesis. The steps between the formation of cAMP and initiation of steroidogenesis, i.e., conversion of cholesterol to pregnenolone, are still unclear. However, it is fairly well established that the rate-limiting steps in the steroidogenic process under ICSH control involve the conversion of cholesterol to pregnenolone (for review, see reference 64). There are two major steroidogenic pathways leading to formation of androgens, the a4 and the a5 pathways. In some lower species (e.g., the rat) the a4 pathway predominates. In man, the a5 pathway appears to be predoininant. In a number of somatic androgen target tissues (e.g., prostate, seminal vesicles, and skin) a 5a-reduction of testosterone to dihydrotestosterone takes place. The 5a-reduced androgen is the active hormone. Whether the seminiferous epithelium also requires dihydrotestosterone is still unclear. Th~ available information, all of which has been ac~ quired in species other than man, suggests that the seminiferous epithelium may rl:)spond to t~stos terone as well as to 5a-reduced androgens. Nevertheless, Ii possibility exists that 5a-reductase deficiency may .be .responsible, for abnormal· spermatogenesis. A numbet:of enzymes are involved
Vol; 29, No.5·
TESTICULAR DYSFUNCTION IN MAN
in the process of androgen biogenesis. Consequently, deficiency of anyone enzyme can serve as the pathophysiologic basis of seminiferous epithelium abnormality. The maintenance of relatively normal peripheral levels of androgens could conceivably be achieved in the face of diminished androgen concentration in the testes. The range of circulating androgen levels is wide (250 to 1200 ng/100 ml) and depends not only on testicular production rates but also on the rates of peripheral metabolism and renal clearance. It is conceivable that a testis with an enzymic lesion in the steroidogenic pathway may not produce androgens in amounts sufficient to maintain the extremely high intratesticular concentrations, but the peripheral levels could remain within the normal range. Examples of specific enzymic deficiency have been published. Goebelsmann et al. 65 reported patients with 17,a-dehydrogenase deficiency and with deficiency of 17ahydroxylase. The deficiencies of these key enzymes produced an extremely severe deficiency of androgen production and resulted in pseudohermaphroditism. An excess of an enzyme involved in androgen biogenesis may also result·in inadequate androgen production. An excess of5a-reductase activity has been reported resulting in 5a-reduction of early intermediates in the steroidogenic pathway associated with a diminished testosterone production rate. 66 Under normal conditions, testicular tissue is relatively poor in 20a-reductase; 20a-dihydroprogesterone and 20a-dihydropregnenolone are normally only minor metabolites. This situation is in contradistinction to that in the ovaries, which produce great amounts of 20a-dihydroprogesterone. Evidence from in vitro studies suggests that a hydroxyl group in the 20a position interferes with further metabolism of the steroid, particularly with 17a-hydroxylation and with 17-20 lyase activity. Consequently, an excess of 20a-hydrogenase may .interfere .with· the normal progression .of. the androgen biogenetic pathway and thus with·the production of androgens. Recent studies . have demonstrated increased rates· of in vitro formation of 2Oa-hy- . droxylated C 21 steroids, in testicular tissue of some. patients with· severe oligospermia.67
Spermatogenesis Fundamental studies dealing with the phys.iology of Leydig ,cell function and with androgen biosynthesis have already led to palpable clinical
487
benefits. Elucidation of the pathophysiologic principles led to identification of specific pathologic states, thus to· diagnosis, and in some instances to selection of appropriate and successful therapy. Knowledge of the intricacies of the hormonal control of the seminiferous tubule and of the spermatogenic process has been· gained only in the past 5 to 10 years. These studies resulted· in the discovery of a series of basic phenomena dealing with the molecular aspects of hormone action. In analogy with ICSH, it has been demonstrated that FSH also requires specific receptors in the target cell for expression of its action (for review see reference 68). Although FSH has always been considered to be the "germinal cell" hormone, i.e., a hormone that specifically acts on the germinal cells (for review, see reference 69), .the specific receptors for FSH were found in the Sertoli cells. 7G-72 This finding made the Sertoli cell the center of attention 100 years after its discovery and only after numerous . attempts in the course of these years to find a role for FSH in the spermatogenic process. While studies on the binding of· FSH were in progress, several other molecular phenomena were discovered. A specific protein, androgenbinding protein (ABP), was shown to be pro-. duced by the testicular tissue in response to FSH stimulation:73 • 74 An FSH-dependent increase in the formation of cAMP was also demonstrated. 75- 77 . Both events were shown to occur in the Sertoli cell (for review, see reference 78). Androgen-binding protein was shown to be secre- . ted by the Sertoli cells into the lumen of the seminiferous tubules and transported into the epididymis, where it accumulates in concentrations higher than those found in the testes and is thought to be an important factor in providing a high concentration of androgens. locally in the epididymis. 79 This high concentration of androgens . is thought to be essential to the maturation of epididymal spermatozoa. Although no direct evidence has been given for the role of ABP in the testes, a hypothesis for its function there has been proposed and is discussed below. While data have accumulated demonstrating ,a dramatic effect ofFSH on cAMP production, RNA, and general and specific (ABP)·protein.synthesis, no direct evidence has' emerged to link these phenomena with the process of spermatogeBeSis. The ,data suggest that the various.· molecular events under FSH control can be. demonstrated more readily in developing testes or in posthypophysectomy-regressed testes.
488
May 1978
STEINBERGER
The fact that testosterone maintains spermatogenesis in adult animals in the absence of gonadotropins 80 led to the investigation of its effects on the various biochemical parameters discussed above. These studies demonstrated that testosterone, like FSH, will maintain and (under certain conditions) reinitiate ABP production in the testes of hypophysectomized rats. 81 Furthermore,specific testosterone receptors have been demonstrated in cytosol obtained from testicular tissue,82 and evidence has been provided for the translocation of the receptor-steroid complex into the nucleus. 83 It has recently been demonstrated that receptors are present in Sertoli cells in culture. 84 ,85 Furthermore, receptors for testosterone may be present in several types of germinal cells. 86·88 The demonstration of a chromatin acceptor for the receptor-testosterone complex in testicular tissue 89 ,90 added another crucial fragment to the evidence that spermatogenesis is controlled by the hormones through the molecular mechanisms postulated for other systems. It must be emphasized that most of the studies discussed above were conducted in lower species and should be extrapolated to man with caution. The extremely limited information derived from studies on human testicular tissue suggests that the androphilic protein isolated from the human testis may possess physicochemical characteristics identical with those of testosterone-binding globulin,91 a testosterone-transport protein found in blood. Thus, the human testis may not produce a specific testicular androgen-binding protein as does the rat testis. It appears that in the human testis mechanisms at least similar to, if not identical with, those found in lower species will be uncovered. If so, it is quite plausible that a biochemical lesion at any point in the complicated molecular mechanism governing spermatogenesis may result in abnormality of this process. Thus, the pathophysiology of testicular disease resulting in what we now call "adult seminiferous tubule failure" may be the result of fine changes or disturbances in molecular mechanisms governing spermatogenesis. Since some of these mechanisms are now amenable to laboratory scrutiny, appropriate tests will have to be devised to probe these mechanisms under clinical conditions. It is quite likely that as a result of such studies Sertoli cell dysfunction will emerge as a major pathophysiologic mechanism underlying the etiology of "adult seminiferous tubule failure."
The above discussion has centered primarily around the pathophysiology of two testicular components, the Leydig cells and the seminiferous epithelium. Examination of testicular biopsies from patients with disturbed sperm production frequently reveals abnormalities not only in the seminiferous epithelium but also in the limiting membrane of the seminiferous tubules. The two striking changes most easily detected in routine histologic preparations of testicular biopsies are "hyalinization" of the limiting membrane and hyperplasia of the fibroblastic elements, "peritubular fibrosis."
It is not known whether the etiologic factors responsible for the abnormality of the seminiferous epithelium also induce pathologic changes in the limiting membrane or whether the abnormality of the limiting membrane is a primary process which may actually be the cause of damage to the seminiferous epithelium. The available information concerning this question is controversial and confusing. Some investigators have published observations suggesting that treatment with testosterone may induce pathoologic changes in the limiting membrane; however, lack of gonadotropins has also been suggested as a cause for this abnormality, and apparently gonadotropin treatment reverses the lesion. It appears that, since the clinical approach utilized until now to resolve this question may not be adequate, an animal model may have to be developed to study this problem. Unfortunately, the most commonly used experimental animals--rats, mice, and guinea pigs-do not show the characteristic pathologic changes in the limiting membrane under any ofthe experimental conditions studied thus far.
IATROGENIC ETIOLOGY OF TESTICULAR DYSFUNCTION
Surgery Although rare, interference with the blood supply to the testes can occur in the course of hernia repair. Cases of testicular damage secondary to interference with blood vessels in the spermatic cord are occasionally seen. They probably are not as common as might be expected because of the collateral blood supply to the testes. However, if a testicular lesion is produced as a result of blood supply disturbance, it is ischemic in nature and after a period of time irreversible.
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
REFERENCES
Heat The application of heat to the scrotum in patients with various forms of orchidites is still an occasionally practiced form of palliative therapy. Similarly, heavy and tight dressings elevating the scrotum and testes close to the· body are sometimes employed. Such dressings result in elevation of intratesticular temperature and direct injury to the seminiferous epithelium. Although short-term exposure to heat produces reversible changes, chronic exposure will induce irreversible changes, the extent of which will depend on the duration of the exposure and the amount of heat (for review, see reference 92).
Chemotherapy Experimental studies in lower species clearly demonstrated the detrimental effects ofalkylating agents,antimetabolites, and a variety of cytotoxic substances on the seminiferous epithelium. The degree of damage and its reversibility depend greatly on the type of agent used and the dose and duration of treatment. Reports of studies in man are scarce; however, those which are available reveal results similar to those reported in lower species. The damage varies from complete and permanent sterility through subfertility to return of fertility with production of phenotypically normal offspring. The extent of reported data, however, is too limited to allow a definitive evaluation of the relationship between specific agents, dose, and duration of therapy on one hand and the severity and permanence of the damage on the other. Possible genetic abnormalities, not detectable by physical examination of the offspring, have been considered, but no data are available concerning this distinct possibility (for review, see reference 1).
Androgen Therapy The administration of androgens, whether for the purpose of treating impotence or the male climacteric or. for improvement of athletic performance in men. engaged in competitive sports, most likely causes only temporary interference with spermatogenesis. However, therapy with androgens in immature males for the purpose of induction of puberty or stimulation of growth may be detrimental to the normal development ofthe seminiferous epithelium. However, no adequate data are available to permit a definite conclusion about the safety of androgen therapy during puberty.
489
1. Gomes WR: Metabolic and regulatory hormones influenc-
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16. 17.
ing testis function. In The Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 68 Steinberger E: Recent advances in regulation of male fertility. In Regulation of Human Fertility, Edited by KS Moghissi, TN Evans. Detroit, Wayne State University Press, 1976, p 274 Oakberg EF: Effects of radiation on the testis. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 233 Leblond CP, Steinberger E, Roosen-Runge E: Spermatogenesis. In Mechanisms Concerned with Conception, Edited by C Hartman. New York, PergamonPress,1963, pI Rose RM, Bourne PG, Poe RO, Mougey EH, Collins DR, Mason JW: Androgen responses to stress. II. Excretion of testosterone, epitestosterone, androsterone, and etiocholanolone during basic combat training and under threat of attack. PsychosomMed 31:418, 1969 Matsumoto K, Takeyasu K, Mizutani S, Hamanaka Y, Uozumi T: Plasma testosterone levels following surgical stress in male patients. Acta Endocrinol (Kbh) 65:11, 1970 Kreuz LE, Rose RM, Jennings JR: Suppression of plasma testosterone levels and psychologic stress. Arch Gen Psychiatry 26:479, 1972 Monden Y, Koshiyama K, Tanaka H, Mizutani S, Aono T, Hamanaka Y, Uozumi T, Matsumoto K: Influence of major surgical stress on plasma testosterone, plasma LH and urinary steroids. Acta Endocrinol (Kbh) 69:542, 1972 Carstensen H, Amer B, Amer I, Wide L: The post-operative decrease of plasma testosterone in man, after major surgery, in relation to plasma FSH and LH. J Steroid Biochem 4:45, 1973 Christian JJ, Lloyd JA, Davis DE: The role of endocrines in the self regulation of mammalian population. Recent Prog Horm Res 21:501,1965 Lloyd JA: Weights of testes, thymi, and accessory reproductive glands in relation to rank in paired and grouped mice (Mus musculus). Proc Soc Exp BioI Med 137:16, 1971 Lloyd JA: Social structure and reproduction in two freelygrowing populations of house mice (Mus musculus). Anim Behav 23:413, 1975 Mancini RE, Penhos JC, Izquierdo lA, Heinrich JJ: Effects of acute hypoglycemia on rat testis.Proc Soc Exp BioI Med 104:699, 1960 Hunt EL, Bailey DW: The effect of alloxan diabetes on the reproductive system of young male rats. Acta Endocrinol (Kbh) 38:432, 1961 Lidell C, Hellman B: The influence of overeating on the endocrine testis function in mice. Metab Clin Exp 15: 444, 1966 Young DH: The effect of mumps and other factors on male fertility. Stud Fertil 5:27, 1953 Cordes H: Untersuchungen iiber den Einfluss acuter und chronischer Allgemeinerkrankungen auf die Testikel, speziell auf die Spermatogenese, BOwie Beobachtungen iiber das Auftreten von Fett in den Hoden. Arch Pathol Anat Physiol 151:402, 1898
490
May 1978
STEINBERGER
18. Koch K: Zwischenzellen und Hodenatrophie. Arch Pathol Anat Physiol 202:376, 1910 19. Mills RG: The pathological changes in the testes in epidemic pneumonia. J Exp Med 30:505, 1919 20. MacLeod J: Effect of chickenpox and of pneumonia on semen quality. Fertil Steril 2:523, 1951 21. Kar JK: Azoospermia. An analysis of 42 cases. Int J Sexol 7:42, 1953 22. Oettle AG, Harrison RG: Histological changes produced in the rat testis by temporary and permanent occlusion of the testicular artery. J Pathol Bacteriol 64:273, 1952 23. Steinberger E, Tjioe DJ: Spermatogenesis in rat testes after experimental ischemia. Fertil Steril 20:639, 1969 24. Sasano N, Ichijo S: Vascular pattern in the human testis with special reference to its senile changes. Tohoku J Exp Med 99:269, 1969 25. Javert CT, Clark RL: A combined operation for varicocele and inguinal hernia. Surg Gynecol Obstet 79:1,1944 26. EI-Sadr AR, Mina E: Anatomical and surgical aspects in the operative management of varicocele. Urol Cutan Rev 54:257,1950 27. MacLeod J: Seminal cytology in the presence of varicocele. Fertil Steril 16:735, 1965 28. Brown JS, Dubin L, Hotchkiss RS: The varicocele as related to fertility. Fertil Steril 18:46, 1967 29. Charny CW, Baum S: Varicocele and infertility. JAMA 204:1165, 1968 30. Davidson HA: Testicular temperature and varicocoele. Practitioner 173:703, 1954 31. Hanley HG, Harrison RG: The nature and surgical treatment of varcicoele. Br J Surg 50:64, 1963 32. Tessler AN, Krohn HP: Varicocele and testicular temperature. Fertil Steril 17:201, 1966 33. Stephenson JD, O'Shaughnessy EJ: Hypospermia and its relationship to varicocele and intrascrotal temperatures. Fertil Steril 19:110, 1968 34. Steinberger E: Effect of altered blood flow on the testes. In the Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 313 35. Baumgarten HG, Holstein AF: Catecholaminhaltige Nervenfasern im Hoden des Menschen. Z Zellforsch Mikrosk Anat 79:398, 1967 36. Hodson N: The nerves of the testis, epididymis, and scrotum. In The Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 47 37. Horne HH, Paull DP, Munro D: Fertility studies in the human male with traumatic injuries of the spinal cord and cauda equina. N Engl J Med 239:959, 1948 38. Cooper IS: Metabolic consequences of spinal cord injury. J Clin Endocrinol Metab 10:858, 1950 39. de la BaIze FA, Mancini RE, Arrillage F, Andrada JA, Vilar 0, Gurtman AI, Davidson OW: Histologic study of the undescended human testis during puberty. J Clin Endocrinol Metab 20:286, 1960 40. Engle ET: Atypical cytology in testes biopsies. J Urol 62: 694, 1949 41. Ward B, Hunter WM: The absent testicle: a report on a survey carried out among school boys in Nottingham. Br Med J 1(5179):1110, 1960 42. Giarola A: Protection of reproductive capacity as a factor in therapy for undescended testicle. Fertil Steril 18:375, 1967 43. Klinefelter HF Jr, Reifenstein EC Jr, Albright F: Syndrome characterized by gynecomastia, aspermatogenesis
44.
45.
46. 47.
48.
49.
50.
51.
52.
53.
without A-Leydigism and increased excretion of follicle stimUlating hormone. J Clin Endocrinol Metab 2:615, 1942 Paulsen CA, Gordon DL, Carpenter RW, Gandy HM, Drucker WD: Klinefelter's syndrome and its variants: a hormonal and chromosomal study. Recent Prog Horm Res 24:321, 1968 Ferguson-Smith MA: The prepubertal testicular lesion in chromatin-positive Klinefelter's syndrome (primary microorchidism) as seen in mentally handicapped children. Lancet 1:219, 1959 Bunge RG, Bradbury JT: New concepts of the Klinefelter syndrome. J Urol 76:758, 1956 Steinberger E, Smith KD, Perloff WH: Spermatogenesis in Klinefelter's syndrome. J Clin Endocrinol Metab 25: 1340, 1965 Steinberger E, Smith KD, Tcholakian RK, Chowdhury M, Steinberger A, Ficher M, Paulsen CA: Steroidogenesis in human testes. In Male Fertility and Sterility, Edited by RE Mancini, L Martini. New York, Academic Press, 1974, p 149 Lipsett MB, Davis TE, Wilson H, Canfield CJ: Testosterone production in chromatin-positive Klinefelter's syndrome. J Clin Endocrinol Metab 25:1025, 1965 French FS, Baggett B, Van WykJJ, Talbert LM, Hubbard WR, Johnston FR, Weaver RP: Testicular feminization: clinical, morphological and biochemical studies. J Clin Endocrinol Metab 25:661, 1965 Southren AL, Ross H, Sharma DC, Gordon G, We ingold AB, Dorfman RI: Plasma concentration and biosynthesis of testosterone in the syndrome of feminizing testes. J Clin Endocrinol Metab 25:51, 1965 French FS, Spooner I, Baggett B: Metabolism of 17hydroxyprogesterone in testicular tissue from a patient with the syndrome of testicular feminization. J Clin Endocrinol Metab 27:437, 1967 Leathem JH: Nutritional influences on testicular composition and function in mammals. In Handbook of Physsiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 225
54. Mancini RE, Seiguer AC, Lloret AP: The effect of gonadotropins on the testis of hypophysectomized patients. In Gonadotropins, Edited by E Rosemberg. Los Altos Calif, Geron-X, 1968, p 503 55. Paulsen CA: Effect of human chorionic gonadotropin and human menpausal gonadotropin therapy on testicular function. In Gonadotropins, Edited by E Rosemberg. Los Altos Calif, Geron-X, 1968, p 491 56. Rivarola MA, Podesta EJ, Chemes HE: In vitro testosterone- 14 C metabolism by rat seminiferous tubules at different stages of development: formation of 5a-androstanediol at meiosis. Endocrinology 91:537, 1972 57. Steinberger E, Steinberger A: Testis: basic and clinical aspects. In Reproductive Biology, Edited by H Balin, S Glasser. Amsterdam, Excerpta Medica, 1972, p 144 58. Gillman J: The development ofthe gonads in man, with a consideration of the role of fetal endocrines and the histogenesis of ovarian tumors. Contrib Embryol Carnegie Inst 32:83, 1948 59. Arey LB: Developmental Anatomy, A Textbook and Laboratory Manual of Embryology, Seventh Edition. Philadelphia, WB Saunders Co, 1965
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
60. Roosen-Runge EC, Anderson D: The development of the interstitial cells in the testis of the albino rat. Acta Anat (Basel) 37:125, 1959 61. Clegg EJ: Puberal growth in the Leydig cells and accessory reproductive organs of the rat. J Anat 100:369, 1966 62. Steinberger E, Steinberger A: Hormonal control of testicular function in mammals. In Handbook of Physiology, Edited by E Knobil, WH Sawyer, Sect 7: Endocrinology, Vol 4: The Pituitary Gland and Its Neuroendocrine Control, Part 2. Washington DC, American Physiological Society, 1974, p 325 63. Christensen AK: Leydig cells. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 57 64. Eik-Nes KB: Biosynthesis and secretion of testicular steroids. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 95 65. Goebelsmann U, Horton R, Mestman JH, Arce JJ, Nagata Y, Nakamura RM, Thorneycroft IH, Mishell DR Jr: Male pseudohermaphroditism due to testicular 17f3-hydroxysteroid dehydrogenase deficiency. J Clin Endocrinol Metab 36:867, 1973 66. Steinberger E, Ficher M, Smith KD: An enzymatic defect in androgen biosynthesis in human testis: a case report and response to therapy. Andrologia 6:59, 1974 67. Rodriguez-Rigau LJ, Weiss DB, Smith KD, Steinberger E: Suggestion of abnormal testicular steroidogenesis in some oligospermic men. Acta Endocrinol (Kbh) 87:400, 1978 68. Steinberger E: Hormonal regulation of the seminiferous tubule function. In Hormonal Regulation of Spermatogenesis, Edited by FS French, V Hansson, EM Ritzen, SN Nayfeh. New York, Plenum Press, 1975, p 337 69. Steinberger E: Hormonal control of mammalian spermatogenesis. Physiol Rev 51:1, 1971 70. Dorrington JH, Roller NF, Fritz IB: The effects ofFSH on cell preparations from the rat testis. In Hormone Binding and Target Cell Activation in the Testis, Edited by ML Dufau, AR Means. New York, Plenum Press, 1974, p 237 71. Steinberger A, Elkington JSH, Sanborn BM, Steinberger E, Heindel JJ, Lindsey IN: Culture and FSH responses of Sertoli cells isolated from sexually mature rat testis. In Hormonal Regulation of Spermatogenesis, Edited by FS French, V Hansson, EM Ritzen, SN Nayfeh. New York, Plenum Press, 1975, p 399 72. Heindel JJ, Rothenberg R, Robison GA, Steinberger A: LH and FSH stimulation of cyclic AMP in specific cell types isolated from the testes. J Cyclic Nucleotide Res 1:69,1975 73. Hansson V, Reusch E, Trygstad 0, Torgersen 0, Ritzen EM, French FS: FSH stimulation of testicular androgen binding protein. Nature [New BioI] 246:56, 1973 74. Steinberger E, Steinberger A, Sanborn B: Endocrine control of spermatogenesis. In Physiology and Genetics of Reproduction, Part A, Edited by M Coutinho, F Fuchs. New York, Plenum Press, 1974, p 163 75. Kuehl FA Jr, Patanelli DJ, Tarnoff J, Humes JL: Testicular adenyl cyclase: stimulation by the pituitary gonadotrophins. BioI Reprod 2:154, 1970
491
76. Braun T, Sepsenwol S: Stimulation of 14C-cyclic AMP accumulation by FSH and LH in testis from mature and immature rats. Endocrinology 94:1028, 1974 77. Cooke BA, Rommerts FG, van der Kemp JWCM, van der Molen HJ: Effects ofluteinizing hormone, follicle stimulating hormone, prostaglandin El and other hormones on adenosine-3':5' -cyclic monophosphate and testosterone production in rat testis tissues. Mol Cell Endocrinol 1:99,1974 78. Steinberger A, Steinberger E: The Sertoli cells. In The Testis, Vol 4, Edited by AD Johnson, WR Gomes. New York, Academic Press, 1977, P 371 79. Hansson V, Ritzen EM, French FS, Nayfeh SN: Androgen transport and receptor mechanisms in testis and epididymis. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 173 80. Walsh EL, Cuyler WK, McCullagh DR: Physiologic maintenance of male sex glands; effect of androtin on hypophysectomized rats. Am J Physioll07:508, 1934 81. Elkington JSH, Sanborn BM, Steinberger E: The effect of testosterone propionate on the concentration of testicular and epididymal androgen binding activity in the hypophysectomized rat. Mol Cell EndocrinoI2:157, 1975 82. Hansson V, McLean WS, SmithAA, Tindall DJ, Weddington SC, Nayfeh SN, French FS, Ritzen EM: Androgen receptors in rat testis. Steroids 23:823, 1974 83. Mulder E, Peters MJ, van Beurden WMO, van der Molen HJ: A receptor for testosterone in mature rat testes. FEBS Lett 47:209, 1974 84. Mulder E, Peters MJ, Van Beurden WMO, Galdieri M, Rommerts RRG, Janzen FHA, van der Molen HJ: Androgen receptors in isolated cell preparations obtained from rat testicular tissue. J Endocrinol 70:331, 1976 85. Sanborn BM, Steinberger A, Tcholakian RK, Steinberger E: Direct measurement of androgen receptors in cultured Sertoli cells. Steroids 29:493, 1977 86. Galena HJ, Pillai AK, Terner C: Progesterone and androgen receptors in nonfiagellate germ cells of the rat testis J Endocrinol 63:223, 1974 87. Sanborn BM, Steinberger E: Androgen nuclear exchange activity in rat testis. Endocr Res Commun 2:335, U375 88. Sanborn BM, Steinberger A, Meistrich ML, Steinberger E: Androgen binding sites in t,estis cell fractions as measured by a nuclear exchange assay. J Steroid Biochem 6:1459, 1975 89. Klyzsejko-Stefanowicz L, Chiu JF, Tsai YH, Hnilica L: Acceptor proteins in rat androgenic tissue chromatin. Proc Nat! Acad Sci USA 73:1954, 1976 90. Tsai YH, Sanborn BM, Steinberger A, Steinberger E: Interaction of testicular androgen-receptor complex with rat germ cell and Sertoli cell chromatin. Biochem Biophys Res Commun 25:366, 1977 91. Vigersky RA, Loriaux DL, Howards SS, Hodgen GB, Lipsett MB, Chrambach A: Androgen binding proteins of testis, epididymis, and plasma in man and monkey. J Clin Invest 58:1061, 1976 92. VanDemark NL, Free MJ: Temperature effects. In The Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 233
FERTILITY AND STERILITY Copyright • 1978 The American Fertility Society
THE ETIOLOGY AND PATHOPHYSIOLOGY OF TESTICULAR DYSFUNCTION IN MAN*
EMIL STEINBERGER, M.D.t
Department of Reproductive Medicine and Biology, The University of Texas Medical School at Houston, Houston, Texas 77025
As it will become apparent throughout this review, a peculiar phenomenon is occurring in the area of medicine dealing with the study of testicular disorders. More is being learned about pathophysiologic mechanisms of testicular disease than about its etiology. In other words, we are recognizing and uncovering physiologic mechanisms which, when disturbed, may easily serve as the basis of testicular disease; however, in many ifnot most instances, we'are unable to find the etiologic factors leading to the disturbance. Consequently, we are hampered in establishing specific diagnoses, and as a result therapy is frequently unsuccessful. In this brief review an attempt is made to correlate the available information concerning testicular pathophysiology with the possible etiologic factors involved in testicular dysfunction. The etiologic factors are arbitrarily divided into the following categories: (1) environmental, (2) systemic, (3) intratesticular, and (4) iatrogenic. ENVIRONMENTAL ETIOLOGY OF TESTICULAR DYSFUNCTION
Exposure to Noxious Substances The pathophysiology of testicular disorders resulting from exposure to noxious substances depends entirely on the type of agent causing the disturbance. Workers employed in the manufacture of stilbestrol (a synthetic estrogen capable of suppressing the hypothalami~-pituitary axis)
may inadvertently be exposed to sufficient quantities of this estrogen to develop impotence and testicular atrophy. Thus, the pathophysiology of testicular damage in these cases is hypogonadotropism, resulting in atrophy of both the Leydig cells and seminiferous epithelium. Numerous other· chemical agents-deuterium oxide, cadmium, fiuoroacetamide, various cytotoxic agents (e.g., nitrofurans,. dinitropyrroles, diamines, a-chlorohydrin, various insecticides, and rodenticides) (for review, see references 1 and 2)can produce testicular damage. The pathophysiology of the damage resulting from exposure to these agents varies depending upon the agent employed. Some cause microvascular damage with subsequent ischemia and necrosis of the seminiferous tubule and of the interstitial area (e.g., cadmium), while others produce arrest of spermatogenesis by direct action on the seminiferous tubules (e.g., nitrofurans, dinitropyrroles). Some still unidentified agents discharged into or created in the environment by modern technology may have similarly deleterious effects on the testes. Unfortunately, it is very difficult to establish such a relationship in a patient with testicular dysfunction. In most instances the affected individual may not even be aware of having been exposed to the offending agent. If the damage is due to a chronic low-dose exposure, the morphologic change in the testes subsequent to such a . long-term effect may be nonspecific and easily classified as "adult seminiferous tubule failure."
Received November 17, 1977. cited in this review, the experimental studies by the author were supporteq. by National Insitutes of Health Grants 5 P50 HD 08338 and HD 06316 and by grants from The Ford Foundation and The Clayton Foundation. tReprint requests: Emil Steinberger, M.D.; Department of Reproductive Medicine and Biology, University of Texas Medical School, P.O. Box 20708, Houston, Tex. 77025.
Exposure to Radiation
*As
The deleterious effects of various forms of irradiation on spermatogenesis have been clearly demonstrated both in experimental animals and in man (for review, see reference 3). The pathophysiology of testicular damage following ex-
481
482
STEINBERGER
posure to radiation, however, is still not clearly understood. Damage to chromatin material resulting from ionizations at the target sites may cause a variety of mutations, including "lethal mutation" which results in the death of the affected germ cell. If the "stem cells" of the germ cell line are affected, irreversible destruction of the seminiferous epithelium takes place, and no recovery will occur; At lower rates of radiation the stem cells may not be affected but the more mature cells may, and a maturation depletion of the seminiferous epithelium will occur; followed in time by repopulation of the seminiferous epithelium resulting from mitotic activity of the stem cells. Although the resulting gametes may exhibit normal fertilizing capacity, in some instances the resulting embryo dies and is resorbed in utero. In other instances an apparently normal offspring may result. The possibility that such an offspring may carry mutant genes as an effect of the exposure of the stem cell to radiation is ever-present, as has been demonstrated in experiments in lower species (for review, see reference 4). Emotional Stress Some authors have suggested the possibility that emotional stress may trigger testicular dysfunction. Most of the information in man, particularly as related to the effect of emotional stress on sperm production, is essentially anecdotal in nature. However, several well-documented recent studies have suggested that emotional stress may adversely affect androgen production by the testes. 5·9 It is not known whether the diminution of androgen production in these individuals is also associated with diminished sperm production. Experiments in animals have suggested that "social stress" related to excessive population densities may result in testicular dysfunction and diminished fertility, most likely via the adrenalpituitary-hypothalamic feedback mechanism. 1°-12 Consequently, if emotional factors are indeed involved in causing testicular dysfunction, the pathophysiology of this process most likely involves inadequate gonadotropin stimulation of testicular functions. In general, there is considerable evidence that environmental factors, whether chemical, physical, or emotional, may adversely affect testicular function in men. Unfortunately, in most instances it is extremely difficult to detect and/or to relate a specific environmental factor to the testicular dysfunction in a specific patient. On the other hand, in most patients with testicular disease character-
May 1978
ized by inadequate sperm production, neither can a specific diagnosis be established nor the etiologic factor uncovered. Most of these patients are placed in the diagnostic wastebasket of "adult seminiferous tubule failure." Environmental factors, so difficult to pinpoint, may indeed be the underlying etiologic factors in a segment of a patient population with the diagnosis of "adult seminiferous tubule failure." SYSTEMIC ETIOLOGY OF TESTICULAR DYSFUNCTION
Metabolic No overt and direct relationships have been established between well-defined metabolic-endocrine disorders (e.g., diabetes, hypo- or hyperthyroidism, hypo- or hyperadrenocorticism, disorders of calcium metabolism or lipid metabolism) and testicular dysfunction; however, numerous papers have been written suggesting deleterious effects of metabolic derangements on testicular function in lower species and men (for review, see reference 1). Both hypoglycemia13 and hyperglycemia l4 • 15 have been reported to cause seminiferous epithelium damage in rodents. No definite relationship has been shown between diabetes (whether uncontrolled with the hyperglycemic state prevailing or associated with frequent hypoglycemic episodes) and oligospermia. The possible negative effect of adrenal dysfunction on sperm production has been suggested, but no definite data are available to substantiate this possibility. Considerable attention has been devoted to the possible association of hypothyroidism and diminished sperm production. Although patients with severe hypothyroidism may also show testicular dysfunction, a definite relationship between levels of thyroid hormone and spermatogenesis has been difficult to establish. Again it must be emphasized that in the vast majority of patients with oligo- or azoospermia no serious metabolic disturbance can be detected. Infectious Mumps orchitis is the classic example of testicular dysfunction secondary to a specific infection. During the acute stage, a severe inflammatory response of the gonad associated with increased temperature of the organ, marked swelling, and pain is noted. Subsequently, variable degrees of testicular atrophy may occur,t6 primarily due to .destruction. of a portion or all of theseminiferous epithelium; usually the Leydig cells remain
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
functional. Characteristically the damage to the seminiferous tubules is patchy. Some crosssections of seminiferous tubules show complete spermatogenesis while others show varying degrees of spermatogenic arrest or complete destruction of the seminiferous epithelium. Depending on the severity of damage, the sperm output in these patients will be affected to varying degrees. In most instances, only one testis is severely affected, and sperm production by the other may be sufficient to result in an ejaculate with adequate sperm density. Although this condition is relatively common, the pathophysiology of the damage to the seminiferous epithelium is not clearly understood. There is no evidence that the seminiferous epithelium is directly affected by the virus. Most likely the infectious process is limited to the interstitial area of the testes, and the damage to the seminiferous tubules is due to increased temperature and intratesticular pressure secondary to the edema in the interstitial area. Possibly as a result of the inflammatory process, anatomical and physiologic changes occur in the interstitial tissue, resulting in disruption of normal relationships between the interstitial area and the seminiferous tubules. Although common systemic infections have not been demonstrated to produce clinical manifestations of orchitis or damage to the seminiferous epithelium, evidence in the clinical literature suggests that systemic infections as well as infections in the sex accessories (prostate, seminal vesicles) may be associated with transient (or at times even permanent) diminution of sperm output, possibly associated with subclinical testicular disease. 17-21 It is a distinct possibility that some cases of "adult seminiferous tubule failure" represent the end result of a series of subclinical orchidites secondary to systemic infections.
Vascular Ischemic. Interference with the blood supply to the testis results in severe damage, primarily to the seminiferous epithelium. It should be remembered, however, that the seminiferous epithelium has the potential for adequate recovery even after relatively prolonged periods of ischemia (60 to 90 minutes), but chronic ischemia causes irreversible damage. 22 , 23 Evidence for the possibility that arteriosclerotic changes affecting the intratesticular arterioles may cause seminiferous epithelium damage and gradual diminution of testicular function associated with aging has been reported. 24
483
Vascular Abnormalities. The most common vascular abnormality is the varicocele, sometimes associated with diminution of sperm production and sperm motility. At this time neither the pathophysiology of the spontaneously occurring varicocele nor the mechanism by which it produces testicular damage is clear. The dilatation of the pampiniform plexus of veins is due to the backflow of blood secondary to incompetent valves in the spermatic vein. 25- 29 The mechanism responsible for the valvular incompetence is unclear. The fact that the spermatic vein empties into the renal vein at a right angle has been suggested as a contributing factor, acting in concert with increased orthostatic pressure in the spermatic vein secondary to man's upright position. 28 While these suggestions are plausible, they have not been proved experimentally, and no explanation has been given for the fact that only a small segment of the population develops this problem in spite of the fact that these anatomical and postural relationships exist in most men. The mechanism by which varicocele exerts its postulated effect on the testes is similarly unclear. Originally it was suggested that the dilated veins simply insulate the testis, causing elevation of intratesticular temperature which in turn produces thermal damage to the testes. 30 ,31 This rather plausible suggestion has not been borne out in studies involving direct measurements of intratesticular temperature in patients with varicocele. 32 , 33 It has also been suggested that, since the spermatic vein empties into the renal vein in close proximity to the adrenal vein, the backflow of blood rich in adrenal secretions may expose the testes to high concentrations of adrenal hormones, particularly cortisol, which may be deleterious to testicular function. 27 Measurement of cortisol levels in the blood of the pampiniform plexus resulted in the accumulation of controversial data which at this time are difficult to interpret. 29 Clearly, products of adrenal secretion other than cortisol could also find their way to the testes, and this possibility awaits further study. Finally, the possibility that the pathophysiology of testicular damage in patients with varicocele may be based on physical rather than biochemical phenomena must be considered. Since the testis is surrounded by a relatively inelastic capsule and the testicular parenchyma is under slight pressure, inadequate venous drainage from the testes may induce an increase in intratesticular pressure. There is considerable
484
STEINBERGER
evidence suggesting that increased intratesticular pressure (as, for example, secondary to an inflammatory process) may induce seminiferous epithelium damage. This mechanism conceivably may be involved in the damage produced by a varicocele (for review, see reference 34). Neurologic The role of the nervous system in testicular function (both endocrine and exocrine) is not known. Although anatomical aspects of the nerve supply to the testes have been studied extensively and a relationship of the testes to the autonomic nervous system has been established, there is still controversy over whether the seminiferous epithelium has a nerve supply.35.36 Furthermore, no experimental studies have been conducted to demonstrate whether interruption of the nerve adversely affects the testis. Damage to the seminiferous epithelium and to the Leydig cells has been noted in patients with paraplegia. 37 . 38 Whether the damage is caused by the nerve lesions or other factors is unclear. Suggestions have been made that the anatomical relationships of the lower extremities in these patients cause elevation of temperature and that the lesions in the seminiferous epithelium are secondary to the relative hyperthermia. Developmental Testicular ectopia is the most common type of developmental abnormality affecting the testes. A discussion of the pathophysiology of this condition requires consideration of two factors: the mechanisms responsible for abnormal testicular descent and those responsible for damage to the seminiferous epithelium in the affected testis. Arrest of descent (abdominal, inguinal, or "high riding" testes) and inappropriate descent (crural, suprapubic, or perineal testes) have been considered to be the result of a developmental anatomical abnormality in the path of testicular descent. 39 The damage to the seminiferous epithelium is thought to be secondary to elevated ambient temperature. However, some authors have suggested that both faulty descent and germinal epithelium pathology are due to a congenital testicular abnormality.4°-42 One line of evidence frequently cited in support of this hypothesis is the presence of abnormalities of the seminiferous epithelium in the contralateral scrotal testis in patients with unilateral testicular ectopia. The other evidence to support a congenital etiology is
May 1978
the singularly limited success in preventing the development of abnormalities of the seminiferous epithelium in ectopic testes replaced surgically (orchidopexy) into the scrotums of young (4- to 6year-old) boys. Although thermal damage to the germinal epithelium of abdominal testes must be considered one of the pathophysiologic mechanisms responsible for spermatogenesis, underlying congenital or genetic defects may also be contributory in a least some instances. Genetic
Chromosomal. The classic example of this type of disorder is Klinefelter's syndrome. 43 The abnormality is characterized by the presence of supernumerary sex chromosomes, resulting most commonly in a 47,XXY karyotype. The testicular abnormality in these patients is expressed primarily by defective function of the seminiferous tubules, although a degree of interference with normal androgen production has also been noted. 44 Originally it was thought that the abnormalities in the seminiferous tubules were due to lack of male germ cell development in the embryo because of the "feminizing" effect of an X chromosome. However, studies of testes from prepuberal boys with the diagnosis of Klinefelter's syndrome revealed the presence of gonocytes (stem cells), which gradually diminished in numbers with age. 45 Furthermore, in the testes of adults with Klinefelter's syndrome, patchy areas of spermatogenesis have been noted. 46 . 47 These findings demonstrate that aspermatogenesis in Klinefelter's syndrome is not due to a lack of germ stem cells, but to the inability of most of these cells during testicular development to enter the spermatogenic process and form a mature seminiferous epithelium. Consequently, an abnormality of the spermatogenic process associated with degeneration of the stem cells is the underlying pathophysiology of aspermatogenesis in patients with Klinefelter's syndrome. The possibility that this defect may be related to local insufficiency of testosterone is unlikely: the capacity of testicular tissue from patients with Klinefelter's syndrome to form testosterone in vitro is actually greater than that of normal tissue,48 and the intratesticular concentration of testosterone is higher (although the production rate and ability to respond to gonadotropins is diminished48 . 49). No information is available concerning the biochemical basis for the defective development of the stem cells in testes from patients with Klinefelter's syndrome. Available
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
evidence suggests that in fetal gonads the supporting cells (which, in the male, are the precursors of the Sertoli cells) may play a determinant role in the development of gonadal sex. A possibility thus exists that in patients with an abnormal complement of sex chromosomes a resulting defect in the Sertoli cells may be the underlying pathology of the aspermatogenic state. Testicular pathology associated with other forms of chromosomal abnormalities has been reported. The pathophysiology in these states is understood even less than in Klinefelter's syndrome, and a direct relationship between the chromosomal abnormality and testicular damage has not been firmly established. Biochemical. The testicular feminization syndrome may fall under this category of genetically based systemic biochemical abnormalities associated with dysfunction of the seminiferous tubules. Patients with this syndrome are genetic males and their testes produce testosterone,50, 51 but the target tissues are unable to respond to it because of lack of androgen receptors. 52 These individuals have the physical appearance offemales but have male levels of circulating testosterone. The lack of appropriate development of the seminiferous epithelium may be a reflection of the inability of testosterone to exert its action on testicular tissue and could also be due to the ectopic position of the testes in patients with this syndrome.
Nutritional Testicular damage resulting from specific nutritional deficiencies has been demonstrated experimentally in a variety of mammals. In man there is definite evidence for testicular dysfunction only in cases of chronic starvation and malnutrition. Deleterious effects of vitamin (A and E) deficiency on the seminiferous epithelium have been shown in the rat, but in man no adequate evidence exists to suggest similar relationships.53 Hypothalamic-Pituitary No specific testicular lesions have been described in patients with failure of thyroid-stimulating hormone or adrenocorticotropic hormone. However, inadequate levels of circulating gonadotropins are associated with abnormalities of testicular function in patients with hypothalamic or pituitary disease. Gonadotropins are necessary
485
for both androgen production and formation of spermatozoa. The deficiency syndrome associated with hypogonadotropism is characterized in an adult male by atrophy of Leydig cells with the resulting lack of androgen production and arrest of spermatogenesis. Replacement therapy with both gonadotropins (interstitial cell-stimulating hormone [lCSH] and follicle-stimulating hormone [FSH]) results in stimulation of growth of the Leydig cells, stimulation of androgen production, and stimulation of spermatogenesis in both hypog~nadotropic eunuchs and in patients with hypogonadism secondary to hypophysectomy. 54, 55 Consequently, the pathophysiology of this disorder is simple hormonal (gonadotropin) deficiency. The best available data suggest that ICSH exerts its effect primarily if not exclusively on the Leydig cells. FSH, on the other hand, is apparently responsible for supporting the process of spermiogenesis in the developing immature testis and the process of reinitiation of spermatogenesis in adult testes. Testosterone maintains spermatogenesis in hypophysectomized animals. The administration of testosterone to hypophysectomized men or to hypogonadotropic eunuchs fails to maintain or initiate spermatogenesis. Species differences have been considered as a possible explanation for this phenomenon. However, this may not necessarily be the only explanation, or even a correct one. Maintenance of spermatogenesis in the hypophysectomized rat requires approximately 4 to 8 mg/kg/day of testosterone. Extrapolation to a 70-kg man suggests a dose of 300 to 600 mg/man! day. In no instance has such a high daily dose been administered to a human for a prolonged period of time. Recently it has been shown that the intratesticular levels of testosterone in man are 10- to 100-fold the circulating levels. 48 A similar relationship has been demonstrated in lower species. 56 The minimal intratesticular concentration of testosterone essential for maintaining spermatogenesis is considerably higher than the normal levels in circulation. These findings suggest that a relatively high intratesticular concentration of androgens is required for the spermatogenic process to proceed, and that below a minimal threshold level the spermatogenic process breaks down. Furthermore, the possibility exists that the threshold varies in different individuals. If this turns out to be the case and if methods are developed to determine the threshold, therapeutic approaches are available to increase androgens to the necessary levels (for review, see reference 57).
486
STEINBERGER INTRATESTICULAR ETIOLOGY OF TESTICULAR DYSFUNCTION
Environmental and systemic factors probably play an important etiologic role in only a small percentage of patients with oligo-azoospermia and/or infertility. This leads one to believe that primary intratesticular abnormalities could be responsible for defective spermatogenesis. In the past 5 to 10 years numerous possible sites for biochemically based pathologic processes capable of causing abnormalities of spermatogenesis have been identified in the dual testicular functions of steroidogenesis and spermatogenesis. Steroidogenesis The principal sites of androgen production in the testis are the Leydig cells. The embryonal origin of these cells and the details of their development are not clearly understood, particularly in man. They are probably of mesenchymal origin, 58. 59 and, if one can extrapolate from the lower species, undergo a complicated process of differentiation from both a morphologic60• 61 and a steroidogenic (for review, see reference 62) viewpoint. After attaining maturity they apparently do not divide actively, if at all. Their multiplication, maturation, and steroid biosynthetic activity are under direct control of ICSH, although some evidence has been presented suggesting that FSH may also playa role in this process (for review, see reference 63). Before examining the possible sites where pathophysiology may occur, one must first have a clear understanding of normal Leydig cell function. Although many gaps still exist in our knowledge, considerable advances have been made recently, and a simplified scheme of these processes can be proposed. A great deal of this information has been derived from lower species, although some of the key points have also been observed directly or indirectly to occur in human testes. The first molecular 'event in the chain of events leading to formation of androgens is the interaction of the gonadotropin horinone ICSH with a specific membrane recept-or. on a cell in the interstitial area of the testis, which ultimately will become a mature Leydig cell. The receptor is composed of two parts, .thereceptor site· and a transducer, adenyl cyclase. The message received by the receptor site activates adenyl cyclase to. stimulate production of cyclic adenosine 3':5'-monophosphate(cAMP). The end result of the increased production of this nucl!,!otjde Js
May 1978
to induce multiplication and differentiation of the Leydig cells. Mechanisms involved in this process are unknown, except for the fact that they are probably mediated via a nuclear transcriptional and translation mechanism leading to de novo RNA and protein synthesis. It is doubtful that a substantial proportion of patients with seminiferous tubule abnormalities has a disorder related to inappropriate somatic differentiation of Leydig cells, because in the vast majority of patients the Leydig cell can be seen and no morphologic abnormality in growth and differentiation can be detected. On the other hand, evidence has begun to accumulate that the biochemical events involved in the biogenesis of androgens may indeed be abnormal in some of these patients. Since androgens are essential for both initiation and maintenance of spermatogenesis, an abnormality in this process may be an etiologic factor in some of the cases of "idiopathic adult seminiferous tubule failure." The mechanism ICSH~receptor~cAMP stimulation is also involved in steroidogenesis. ICSH must be bound to the receptor before a steroidogenic effect is induced. Furthermore, a steroidogenic effect can be induced in the absence of ICSH by cAMP, implicating this nucleotide in the mechanism of ICSH action on steroidogenesis. The steps between the formation of cAMP and initiation of steroidogenesis, i.e., conversion of cholesterol to pregnenolone, are still unclear. However, it is fairly well established that the rate-limiting steps in the steroidogenic process under ICSH control involve the conversion of cholesterol to pregnenolone (for review, see reference 64). There are two major steroidogenic pathways leading to formation of androgens, the a4 and the a5 pathways. In some lower species (e.g., the rat) the a4 pathway predominates. In man, the a5 pathway appears to be predoininant. In a number of somatic androgen target tissues (e.g., prostate, seminal vesicles, and skin) a 5a-reduction of testosterone to dihydrotestosterone takes place. The 5a-reduced androgen is the active hormone. Whether the seminiferous epithelium also requires dihydrotestosterone is still unclear. Th~ available information, all of which has been ac~ quired in species other than man, suggests that the seminiferous epithelium may rl:)spond to t~stos terone as well as to 5a-reduced androgens. Nevertheless, Ii possibility exists that 5a-reductase deficiency may .be .responsible, for abnormal· spermatogenesis. A numbet:of enzymes are involved
Vol; 29, No.5·
TESTICULAR DYSFUNCTION IN MAN
in the process of androgen biogenesis. Consequently, deficiency of anyone enzyme can serve as the pathophysiologic basis of seminiferous epithelium abnormality. The maintenance of relatively normal peripheral levels of androgens could conceivably be achieved in the face of diminished androgen concentration in the testes. The range of circulating androgen levels is wide (250 to 1200 ng/100 ml) and depends not only on testicular production rates but also on the rates of peripheral metabolism and renal clearance. It is conceivable that a testis with an enzymic lesion in the steroidogenic pathway may not produce androgens in amounts sufficient to maintain the extremely high intratesticular concentrations, but the peripheral levels could remain within the normal range. Examples of specific enzymic deficiency have been published. Goebelsmann et al. 65 reported patients with 17,a-dehydrogenase deficiency and with deficiency of 17ahydroxylase. The deficiencies of these key enzymes produced an extremely severe deficiency of androgen production and resulted in pseudohermaphroditism. An excess of an enzyme involved in androgen biogenesis may also result·in inadequate androgen production. An excess of5a-reductase activity has been reported resulting in 5a-reduction of early intermediates in the steroidogenic pathway associated with a diminished testosterone production rate. 66 Under normal conditions, testicular tissue is relatively poor in 20a-reductase; 20a-dihydroprogesterone and 20a-dihydropregnenolone are normally only minor metabolites. This situation is in contradistinction to that in the ovaries, which produce great amounts of 20a-dihydroprogesterone. Evidence from in vitro studies suggests that a hydroxyl group in the 20a position interferes with further metabolism of the steroid, particularly with 17a-hydroxylation and with 17-20 lyase activity. Consequently, an excess of 20a-hydrogenase may .interfere .with· the normal progression .of. the androgen biogenetic pathway and thus with·the production of androgens. Recent studies . have demonstrated increased rates· of in vitro formation of 2Oa-hy- . droxylated C 21 steroids, in testicular tissue of some. patients with· severe oligospermia.67
Spermatogenesis Fundamental studies dealing with the phys.iology of Leydig ,cell function and with androgen biosynthesis have already led to palpable clinical
487
benefits. Elucidation of the pathophysiologic principles led to identification of specific pathologic states, thus to· diagnosis, and in some instances to selection of appropriate and successful therapy. Knowledge of the intricacies of the hormonal control of the seminiferous tubule and of the spermatogenic process has been· gained only in the past 5 to 10 years. These studies resulted· in the discovery of a series of basic phenomena dealing with the molecular aspects of hormone action. In analogy with ICSH, it has been demonstrated that FSH also requires specific receptors in the target cell for expression of its action (for review see reference 68). Although FSH has always been considered to be the "germinal cell" hormone, i.e., a hormone that specifically acts on the germinal cells (for review, see reference 69), .the specific receptors for FSH were found in the Sertoli cells. 7G-72 This finding made the Sertoli cell the center of attention 100 years after its discovery and only after numerous . attempts in the course of these years to find a role for FSH in the spermatogenic process. While studies on the binding of· FSH were in progress, several other molecular phenomena were discovered. A specific protein, androgenbinding protein (ABP), was shown to be pro-. duced by the testicular tissue in response to FSH stimulation:73 • 74 An FSH-dependent increase in the formation of cAMP was also demonstrated. 75- 77 . Both events were shown to occur in the Sertoli cell (for review, see reference 78). Androgen-binding protein was shown to be secre- . ted by the Sertoli cells into the lumen of the seminiferous tubules and transported into the epididymis, where it accumulates in concentrations higher than those found in the testes and is thought to be an important factor in providing a high concentration of androgens. locally in the epididymis. 79 This high concentration of androgens . is thought to be essential to the maturation of epididymal spermatozoa. Although no direct evidence has been given for the role of ABP in the testes, a hypothesis for its function there has been proposed and is discussed below. While data have accumulated demonstrating ,a dramatic effect ofFSH on cAMP production, RNA, and general and specific (ABP)·protein.synthesis, no direct evidence has' emerged to link these phenomena with the process of spermatogeBeSis. The ,data suggest that the various.· molecular events under FSH control can be. demonstrated more readily in developing testes or in posthypophysectomy-regressed testes.
488
May 1978
STEINBERGER
The fact that testosterone maintains spermatogenesis in adult animals in the absence of gonadotropins 80 led to the investigation of its effects on the various biochemical parameters discussed above. These studies demonstrated that testosterone, like FSH, will maintain and (under certain conditions) reinitiate ABP production in the testes of hypophysectomized rats. 81 Furthermore,specific testosterone receptors have been demonstrated in cytosol obtained from testicular tissue,82 and evidence has been provided for the translocation of the receptor-steroid complex into the nucleus. 83 It has recently been demonstrated that receptors are present in Sertoli cells in culture. 84 ,85 Furthermore, receptors for testosterone may be present in several types of germinal cells. 86·88 The demonstration of a chromatin acceptor for the receptor-testosterone complex in testicular tissue 89 ,90 added another crucial fragment to the evidence that spermatogenesis is controlled by the hormones through the molecular mechanisms postulated for other systems. It must be emphasized that most of the studies discussed above were conducted in lower species and should be extrapolated to man with caution. The extremely limited information derived from studies on human testicular tissue suggests that the androphilic protein isolated from the human testis may possess physicochemical characteristics identical with those of testosterone-binding globulin,91 a testosterone-transport protein found in blood. Thus, the human testis may not produce a specific testicular androgen-binding protein as does the rat testis. It appears that in the human testis mechanisms at least similar to, if not identical with, those found in lower species will be uncovered. If so, it is quite plausible that a biochemical lesion at any point in the complicated molecular mechanism governing spermatogenesis may result in abnormality of this process. Thus, the pathophysiology of testicular disease resulting in what we now call "adult seminiferous tubule failure" may be the result of fine changes or disturbances in molecular mechanisms governing spermatogenesis. Since some of these mechanisms are now amenable to laboratory scrutiny, appropriate tests will have to be devised to probe these mechanisms under clinical conditions. It is quite likely that as a result of such studies Sertoli cell dysfunction will emerge as a major pathophysiologic mechanism underlying the etiology of "adult seminiferous tubule failure."
The above discussion has centered primarily around the pathophysiology of two testicular components, the Leydig cells and the seminiferous epithelium. Examination of testicular biopsies from patients with disturbed sperm production frequently reveals abnormalities not only in the seminiferous epithelium but also in the limiting membrane of the seminiferous tubules. The two striking changes most easily detected in routine histologic preparations of testicular biopsies are "hyalinization" of the limiting membrane and hyperplasia of the fibroblastic elements, "peritubular fibrosis."
It is not known whether the etiologic factors responsible for the abnormality of the seminiferous epithelium also induce pathologic changes in the limiting membrane or whether the abnormality of the limiting membrane is a primary process which may actually be the cause of damage to the seminiferous epithelium. The available information concerning this question is controversial and confusing. Some investigators have published observations suggesting that treatment with testosterone may induce pathoologic changes in the limiting membrane; however, lack of gonadotropins has also been suggested as a cause for this abnormality, and apparently gonadotropin treatment reverses the lesion. It appears that, since the clinical approach utilized until now to resolve this question may not be adequate, an animal model may have to be developed to study this problem. Unfortunately, the most commonly used experimental animals--rats, mice, and guinea pigs-do not show the characteristic pathologic changes in the limiting membrane under any ofthe experimental conditions studied thus far.
IATROGENIC ETIOLOGY OF TESTICULAR DYSFUNCTION
Surgery Although rare, interference with the blood supply to the testes can occur in the course of hernia repair. Cases of testicular damage secondary to interference with blood vessels in the spermatic cord are occasionally seen. They probably are not as common as might be expected because of the collateral blood supply to the testes. However, if a testicular lesion is produced as a result of blood supply disturbance, it is ischemic in nature and after a period of time irreversible.
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
REFERENCES
Heat The application of heat to the scrotum in patients with various forms of orchidites is still an occasionally practiced form of palliative therapy. Similarly, heavy and tight dressings elevating the scrotum and testes close to the· body are sometimes employed. Such dressings result in elevation of intratesticular temperature and direct injury to the seminiferous epithelium. Although short-term exposure to heat produces reversible changes, chronic exposure will induce irreversible changes, the extent of which will depend on the duration of the exposure and the amount of heat (for review, see reference 92).
Chemotherapy Experimental studies in lower species clearly demonstrated the detrimental effects ofalkylating agents,antimetabolites, and a variety of cytotoxic substances on the seminiferous epithelium. The degree of damage and its reversibility depend greatly on the type of agent used and the dose and duration of treatment. Reports of studies in man are scarce; however, those which are available reveal results similar to those reported in lower species. The damage varies from complete and permanent sterility through subfertility to return of fertility with production of phenotypically normal offspring. The extent of reported data, however, is too limited to allow a definitive evaluation of the relationship between specific agents, dose, and duration of therapy on one hand and the severity and permanence of the damage on the other. Possible genetic abnormalities, not detectable by physical examination of the offspring, have been considered, but no data are available concerning this distinct possibility (for review, see reference 1).
Androgen Therapy The administration of androgens, whether for the purpose of treating impotence or the male climacteric or. for improvement of athletic performance in men. engaged in competitive sports, most likely causes only temporary interference with spermatogenesis. However, therapy with androgens in immature males for the purpose of induction of puberty or stimulation of growth may be detrimental to the normal development ofthe seminiferous epithelium. However, no adequate data are available to permit a definite conclusion about the safety of androgen therapy during puberty.
489
1. Gomes WR: Metabolic and regulatory hormones influenc-
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16. 17.
ing testis function. In The Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 68 Steinberger E: Recent advances in regulation of male fertility. In Regulation of Human Fertility, Edited by KS Moghissi, TN Evans. Detroit, Wayne State University Press, 1976, p 274 Oakberg EF: Effects of radiation on the testis. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 233 Leblond CP, Steinberger E, Roosen-Runge E: Spermatogenesis. In Mechanisms Concerned with Conception, Edited by C Hartman. New York, PergamonPress,1963, pI Rose RM, Bourne PG, Poe RO, Mougey EH, Collins DR, Mason JW: Androgen responses to stress. II. Excretion of testosterone, epitestosterone, androsterone, and etiocholanolone during basic combat training and under threat of attack. PsychosomMed 31:418, 1969 Matsumoto K, Takeyasu K, Mizutani S, Hamanaka Y, Uozumi T: Plasma testosterone levels following surgical stress in male patients. Acta Endocrinol (Kbh) 65:11, 1970 Kreuz LE, Rose RM, Jennings JR: Suppression of plasma testosterone levels and psychologic stress. Arch Gen Psychiatry 26:479, 1972 Monden Y, Koshiyama K, Tanaka H, Mizutani S, Aono T, Hamanaka Y, Uozumi T, Matsumoto K: Influence of major surgical stress on plasma testosterone, plasma LH and urinary steroids. Acta Endocrinol (Kbh) 69:542, 1972 Carstensen H, Amer B, Amer I, Wide L: The post-operative decrease of plasma testosterone in man, after major surgery, in relation to plasma FSH and LH. J Steroid Biochem 4:45, 1973 Christian JJ, Lloyd JA, Davis DE: The role of endocrines in the self regulation of mammalian population. Recent Prog Horm Res 21:501,1965 Lloyd JA: Weights of testes, thymi, and accessory reproductive glands in relation to rank in paired and grouped mice (Mus musculus). Proc Soc Exp BioI Med 137:16, 1971 Lloyd JA: Social structure and reproduction in two freelygrowing populations of house mice (Mus musculus). Anim Behav 23:413, 1975 Mancini RE, Penhos JC, Izquierdo lA, Heinrich JJ: Effects of acute hypoglycemia on rat testis.Proc Soc Exp BioI Med 104:699, 1960 Hunt EL, Bailey DW: The effect of alloxan diabetes on the reproductive system of young male rats. Acta Endocrinol (Kbh) 38:432, 1961 Lidell C, Hellman B: The influence of overeating on the endocrine testis function in mice. Metab Clin Exp 15: 444, 1966 Young DH: The effect of mumps and other factors on male fertility. Stud Fertil 5:27, 1953 Cordes H: Untersuchungen iiber den Einfluss acuter und chronischer Allgemeinerkrankungen auf die Testikel, speziell auf die Spermatogenese, BOwie Beobachtungen iiber das Auftreten von Fett in den Hoden. Arch Pathol Anat Physiol 151:402, 1898
490
May 1978
STEINBERGER
18. Koch K: Zwischenzellen und Hodenatrophie. Arch Pathol Anat Physiol 202:376, 1910 19. Mills RG: The pathological changes in the testes in epidemic pneumonia. J Exp Med 30:505, 1919 20. MacLeod J: Effect of chickenpox and of pneumonia on semen quality. Fertil Steril 2:523, 1951 21. Kar JK: Azoospermia. An analysis of 42 cases. Int J Sexol 7:42, 1953 22. Oettle AG, Harrison RG: Histological changes produced in the rat testis by temporary and permanent occlusion of the testicular artery. J Pathol Bacteriol 64:273, 1952 23. Steinberger E, Tjioe DJ: Spermatogenesis in rat testes after experimental ischemia. Fertil Steril 20:639, 1969 24. Sasano N, Ichijo S: Vascular pattern in the human testis with special reference to its senile changes. Tohoku J Exp Med 99:269, 1969 25. Javert CT, Clark RL: A combined operation for varicocele and inguinal hernia. Surg Gynecol Obstet 79:1,1944 26. EI-Sadr AR, Mina E: Anatomical and surgical aspects in the operative management of varicocele. Urol Cutan Rev 54:257,1950 27. MacLeod J: Seminal cytology in the presence of varicocele. Fertil Steril 16:735, 1965 28. Brown JS, Dubin L, Hotchkiss RS: The varicocele as related to fertility. Fertil Steril 18:46, 1967 29. Charny CW, Baum S: Varicocele and infertility. JAMA 204:1165, 1968 30. Davidson HA: Testicular temperature and varicocoele. Practitioner 173:703, 1954 31. Hanley HG, Harrison RG: The nature and surgical treatment of varcicoele. Br J Surg 50:64, 1963 32. Tessler AN, Krohn HP: Varicocele and testicular temperature. Fertil Steril 17:201, 1966 33. Stephenson JD, O'Shaughnessy EJ: Hypospermia and its relationship to varicocele and intrascrotal temperatures. Fertil Steril 19:110, 1968 34. Steinberger E: Effect of altered blood flow on the testes. In the Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 313 35. Baumgarten HG, Holstein AF: Catecholaminhaltige Nervenfasern im Hoden des Menschen. Z Zellforsch Mikrosk Anat 79:398, 1967 36. Hodson N: The nerves of the testis, epididymis, and scrotum. In The Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 47 37. Horne HH, Paull DP, Munro D: Fertility studies in the human male with traumatic injuries of the spinal cord and cauda equina. N Engl J Med 239:959, 1948 38. Cooper IS: Metabolic consequences of spinal cord injury. J Clin Endocrinol Metab 10:858, 1950 39. de la BaIze FA, Mancini RE, Arrillage F, Andrada JA, Vilar 0, Gurtman AI, Davidson OW: Histologic study of the undescended human testis during puberty. J Clin Endocrinol Metab 20:286, 1960 40. Engle ET: Atypical cytology in testes biopsies. J Urol 62: 694, 1949 41. Ward B, Hunter WM: The absent testicle: a report on a survey carried out among school boys in Nottingham. Br Med J 1(5179):1110, 1960 42. Giarola A: Protection of reproductive capacity as a factor in therapy for undescended testicle. Fertil Steril 18:375, 1967 43. Klinefelter HF Jr, Reifenstein EC Jr, Albright F: Syndrome characterized by gynecomastia, aspermatogenesis
44.
45.
46. 47.
48.
49.
50.
51.
52.
53.
without A-Leydigism and increased excretion of follicle stimUlating hormone. J Clin Endocrinol Metab 2:615, 1942 Paulsen CA, Gordon DL, Carpenter RW, Gandy HM, Drucker WD: Klinefelter's syndrome and its variants: a hormonal and chromosomal study. Recent Prog Horm Res 24:321, 1968 Ferguson-Smith MA: The prepubertal testicular lesion in chromatin-positive Klinefelter's syndrome (primary microorchidism) as seen in mentally handicapped children. Lancet 1:219, 1959 Bunge RG, Bradbury JT: New concepts of the Klinefelter syndrome. J Urol 76:758, 1956 Steinberger E, Smith KD, Perloff WH: Spermatogenesis in Klinefelter's syndrome. J Clin Endocrinol Metab 25: 1340, 1965 Steinberger E, Smith KD, Tcholakian RK, Chowdhury M, Steinberger A, Ficher M, Paulsen CA: Steroidogenesis in human testes. In Male Fertility and Sterility, Edited by RE Mancini, L Martini. New York, Academic Press, 1974, p 149 Lipsett MB, Davis TE, Wilson H, Canfield CJ: Testosterone production in chromatin-positive Klinefelter's syndrome. J Clin Endocrinol Metab 25:1025, 1965 French FS, Baggett B, Van WykJJ, Talbert LM, Hubbard WR, Johnston FR, Weaver RP: Testicular feminization: clinical, morphological and biochemical studies. J Clin Endocrinol Metab 25:661, 1965 Southren AL, Ross H, Sharma DC, Gordon G, We ingold AB, Dorfman RI: Plasma concentration and biosynthesis of testosterone in the syndrome of feminizing testes. J Clin Endocrinol Metab 25:51, 1965 French FS, Spooner I, Baggett B: Metabolism of 17hydroxyprogesterone in testicular tissue from a patient with the syndrome of testicular feminization. J Clin Endocrinol Metab 27:437, 1967 Leathem JH: Nutritional influences on testicular composition and function in mammals. In Handbook of Physsiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 225
54. Mancini RE, Seiguer AC, Lloret AP: The effect of gonadotropins on the testis of hypophysectomized patients. In Gonadotropins, Edited by E Rosemberg. Los Altos Calif, Geron-X, 1968, p 503 55. Paulsen CA: Effect of human chorionic gonadotropin and human menpausal gonadotropin therapy on testicular function. In Gonadotropins, Edited by E Rosemberg. Los Altos Calif, Geron-X, 1968, p 491 56. Rivarola MA, Podesta EJ, Chemes HE: In vitro testosterone- 14 C metabolism by rat seminiferous tubules at different stages of development: formation of 5a-androstanediol at meiosis. Endocrinology 91:537, 1972 57. Steinberger E, Steinberger A: Testis: basic and clinical aspects. In Reproductive Biology, Edited by H Balin, S Glasser. Amsterdam, Excerpta Medica, 1972, p 144 58. Gillman J: The development ofthe gonads in man, with a consideration of the role of fetal endocrines and the histogenesis of ovarian tumors. Contrib Embryol Carnegie Inst 32:83, 1948 59. Arey LB: Developmental Anatomy, A Textbook and Laboratory Manual of Embryology, Seventh Edition. Philadelphia, WB Saunders Co, 1965
Vol. 29, No.5
TESTICULAR DYSFUNCTION IN MAN
60. Roosen-Runge EC, Anderson D: The development of the interstitial cells in the testis of the albino rat. Acta Anat (Basel) 37:125, 1959 61. Clegg EJ: Puberal growth in the Leydig cells and accessory reproductive organs of the rat. J Anat 100:369, 1966 62. Steinberger E, Steinberger A: Hormonal control of testicular function in mammals. In Handbook of Physiology, Edited by E Knobil, WH Sawyer, Sect 7: Endocrinology, Vol 4: The Pituitary Gland and Its Neuroendocrine Control, Part 2. Washington DC, American Physiological Society, 1974, p 325 63. Christensen AK: Leydig cells. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 57 64. Eik-Nes KB: Biosynthesis and secretion of testicular steroids. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 95 65. Goebelsmann U, Horton R, Mestman JH, Arce JJ, Nagata Y, Nakamura RM, Thorneycroft IH, Mishell DR Jr: Male pseudohermaphroditism due to testicular 17f3-hydroxysteroid dehydrogenase deficiency. J Clin Endocrinol Metab 36:867, 1973 66. Steinberger E, Ficher M, Smith KD: An enzymatic defect in androgen biosynthesis in human testis: a case report and response to therapy. Andrologia 6:59, 1974 67. Rodriguez-Rigau LJ, Weiss DB, Smith KD, Steinberger E: Suggestion of abnormal testicular steroidogenesis in some oligospermic men. Acta Endocrinol (Kbh) 87:400, 1978 68. Steinberger E: Hormonal regulation of the seminiferous tubule function. In Hormonal Regulation of Spermatogenesis, Edited by FS French, V Hansson, EM Ritzen, SN Nayfeh. New York, Plenum Press, 1975, p 337 69. Steinberger E: Hormonal control of mammalian spermatogenesis. Physiol Rev 51:1, 1971 70. Dorrington JH, Roller NF, Fritz IB: The effects ofFSH on cell preparations from the rat testis. In Hormone Binding and Target Cell Activation in the Testis, Edited by ML Dufau, AR Means. New York, Plenum Press, 1974, p 237 71. Steinberger A, Elkington JSH, Sanborn BM, Steinberger E, Heindel JJ, Lindsey IN: Culture and FSH responses of Sertoli cells isolated from sexually mature rat testis. In Hormonal Regulation of Spermatogenesis, Edited by FS French, V Hansson, EM Ritzen, SN Nayfeh. New York, Plenum Press, 1975, p 399 72. Heindel JJ, Rothenberg R, Robison GA, Steinberger A: LH and FSH stimulation of cyclic AMP in specific cell types isolated from the testes. J Cyclic Nucleotide Res 1:69,1975 73. Hansson V, Reusch E, Trygstad 0, Torgersen 0, Ritzen EM, French FS: FSH stimulation of testicular androgen binding protein. Nature [New BioI] 246:56, 1973 74. Steinberger E, Steinberger A, Sanborn B: Endocrine control of spermatogenesis. In Physiology and Genetics of Reproduction, Part A, Edited by M Coutinho, F Fuchs. New York, Plenum Press, 1974, p 163 75. Kuehl FA Jr, Patanelli DJ, Tarnoff J, Humes JL: Testicular adenyl cyclase: stimulation by the pituitary gonadotrophins. BioI Reprod 2:154, 1970
491
76. Braun T, Sepsenwol S: Stimulation of 14C-cyclic AMP accumulation by FSH and LH in testis from mature and immature rats. Endocrinology 94:1028, 1974 77. Cooke BA, Rommerts FG, van der Kemp JWCM, van der Molen HJ: Effects ofluteinizing hormone, follicle stimulating hormone, prostaglandin El and other hormones on adenosine-3':5' -cyclic monophosphate and testosterone production in rat testis tissues. Mol Cell Endocrinol 1:99,1974 78. Steinberger A, Steinberger E: The Sertoli cells. In The Testis, Vol 4, Edited by AD Johnson, WR Gomes. New York, Academic Press, 1977, P 371 79. Hansson V, Ritzen EM, French FS, Nayfeh SN: Androgen transport and receptor mechanisms in testis and epididymis. In Handbook of Physiology, Edited by DW Hamilton, RO Greep, Sect 7: Endocrinology, Vol 5: Male Reproductive System. Washington DC, American Physiological Society, 1975, p 173 80. Walsh EL, Cuyler WK, McCullagh DR: Physiologic maintenance of male sex glands; effect of androtin on hypophysectomized rats. Am J Physioll07:508, 1934 81. Elkington JSH, Sanborn BM, Steinberger E: The effect of testosterone propionate on the concentration of testicular and epididymal androgen binding activity in the hypophysectomized rat. Mol Cell EndocrinoI2:157, 1975 82. Hansson V, McLean WS, SmithAA, Tindall DJ, Weddington SC, Nayfeh SN, French FS, Ritzen EM: Androgen receptors in rat testis. Steroids 23:823, 1974 83. Mulder E, Peters MJ, van Beurden WMO, van der Molen HJ: A receptor for testosterone in mature rat testes. FEBS Lett 47:209, 1974 84. Mulder E, Peters MJ, Van Beurden WMO, Galdieri M, Rommerts RRG, Janzen FHA, van der Molen HJ: Androgen receptors in isolated cell preparations obtained from rat testicular tissue. J Endocrinol 70:331, 1976 85. Sanborn BM, Steinberger A, Tcholakian RK, Steinberger E: Direct measurement of androgen receptors in cultured Sertoli cells. Steroids 29:493, 1977 86. Galena HJ, Pillai AK, Terner C: Progesterone and androgen receptors in nonfiagellate germ cells of the rat testis J Endocrinol 63:223, 1974 87. Sanborn BM, Steinberger E: Androgen nuclear exchange activity in rat testis. Endocr Res Commun 2:335, U375 88. Sanborn BM, Steinberger A, Meistrich ML, Steinberger E: Androgen binding sites in t,estis cell fractions as measured by a nuclear exchange assay. J Steroid Biochem 6:1459, 1975 89. Klyzsejko-Stefanowicz L, Chiu JF, Tsai YH, Hnilica L: Acceptor proteins in rat androgenic tissue chromatin. Proc Nat! Acad Sci USA 73:1954, 1976 90. Tsai YH, Sanborn BM, Steinberger A, Steinberger E: Interaction of testicular androgen-receptor complex with rat germ cell and Sertoli cell chromatin. Biochem Biophys Res Commun 25:366, 1977 91. Vigersky RA, Loriaux DL, Howards SS, Hodgen GB, Lipsett MB, Chrambach A: Androgen binding proteins of testis, epididymis, and plasma in man and monkey. J Clin Invest 58:1061, 1976 92. VanDemark NL, Free MJ: Temperature effects. In The Testis, Vol 3, Edited by AD Johnson, WR Gomes, NL VanDemark. New York, Academic Press, 1970, p 233