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Krukenberg tumor complicating pregnancy
Krukenberg tumor complicating pregnancy Report of a case with androgenic activity
LEON PARRISH FOX, M.D. WERNER].
STAMM, M.D.*
San Jose, California
T H E K R U K E N B E R G T U M 0 R IS a very rare and interesting ovarian lesion which has occasionally been found associated with pregnancy. In this extremely unusual case the gestate manifested massive virilization during the development and growth of the tumor. This special, solid type of malignant neoplasm is usually secondary from a gastrointestinal tract or other mucinous gland lesion; but occasionally it is a true primary tumor of the ovary. The gross appearance, growth pattern, and the microscopic characteristics, including the identifying signet-ring ce!ls and alteration of the ovarian stroma, arc well-known features. This tumor is generally regarded as hormonally inactive. However, observations in recent years have pointed to functional hormonal properties in several cases. 31 • 35 This is not surprising in the presence of the marked stromal activity noted in these lesions. The incidence of malignant ovarian neoplasms found during gestation has been reported to be .5.5 per cent. 10 Thirty cases of Krukenberg tumor associated with preg-
nancy have been documented, with pertinent data, and of these, 2 have been determined to be of primary origin (Table I). In 2 other previously reported cases there has been associated extensive masculinization, such as found here. 13 • 34 Case report
A 27-year-old gravida iv, para iii was rcff't-red by her family physician during the thirty-second werk of gestation complaining of obstipation, generalized abdominal pain, and extreme pdvic pressure. Antenatal care had been initiated at the 11fteenth week and recorded as uneventful until the twenty-third wePk when intermittent uterine cramps and constipation started a prog-ressive course without apparent cause. One month latrr. rapid virilization and wasting- began, and a mass was palpated in tht· pelvis adjoining the uterus and fixed at the rectal shelf. Proctological biopsy showed inflammatory reaction only. The past and family histori<'S were irrelt·vant. The menarche occurred at age 1:1 and menses had been regular and normal. Thn·e uncomplicated pregnancies, 6, 4, and 2 )'f'ars prrviously had resulted in living normal children. Examination showrd a small. thin 27-ycar-old gravid patient who had apparently lost considerable' weight recently and aged beyond her years. The facies were masculine, gaunt. and anxious with striking- acne and hirsutism extending over the body and exhibiting- a male escutcheon. The breasts were of medium size, flat, and colostrum was present. The abdomen was tPrrn pregnancy size, and then· was edema of the wall. A large, firm, tender mass was palpable in the right flank area contiguous with the uterus and extending into the pelvis. Free fluid signs were inconclusive. Vulvar and vaginal
From the Departments of Obstetrics and Gynecology and Pathology, O'Connor Hospital. *Present address: Dominican Santa Cruz HosPital, Santa Cruz, California. Presented as a part of a Symposium of Interesting and Unusual Cases, at the Thirty-first Annual Meeting of the Pacific Coast Obstetrical and Gynecological Society, Santa Barbara, California, Nov. 4-7, 1964.
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Volume 92 ~umber 5
edema were present but the clitoris was not enlarged. Bimanually, the mass was palpable in the posterior cul-de-sac area and involved the rectum at 7 em., fixed in the sacral curve. Vaginal cytology showed no abnormal cells and exhibited a normal pregnancy pattern. Advised hospitalization for proper evaluation and treatment was refused by the patient until 2 and one-half weeks later when vomiting and discomfort caused admission. She arrived in active labor and promptly was delivered of a 3yt pounds female infant who died in a few hours with respiratory difficulty. There was noticeable enlargement of the clitoris but no other fetal abnormalities were noted. Postdelivery examination showed a seriously ill patient with dehydration and exhaustion. The temperature was 99.6° F., pulse 128, respiration 24, and blood pressure 132/90. Virilization had increased and the abdomen was distended with fluid. The uterus was firm and deflected to the left by a 25 em. hard mass. Above the uterus there was another hard mass about 10 em. in diameter. Laboratory studies were not remarkable. The blood picture and urine were consistent with dehydration. The chest and bone survey x-rays showed no metastatic lesions. Fluid balance was stabilized and laparotomy was done on the fourth postpartum day. The 3,000 c.c. of blood-tinged ascitic fluid was aspirated. The right ovary was completely involved in a hard tumor mass with the tube adherent and was easily delivered and removed. The uterus. left ovary, and tube appeared to be normal. Th<" greater omentum was thick, indurated, and enlarged into a 12 em. mass fixed ben('ath the transverse colon on the left side. The thickened pelvic peritoneum was studded with tumor, while the posterior cul-de-sac and sigmoid were densely infiltrated. The stomach, gallbladder, and small bowel were matted together by soft, irregular adhesions, but no specific neoplasm could be identified. The liver, spleen, and kidneys were not at this time grossly involved. A wedge of the omentum was removed for study and the abdomen was closed. A catheter conduit was fixed in the left lower quadrant for chemotherapy administration. Cytological study of the peritoneal fluid showed malignant cells. A 17-ketosteroid determination shortly after operation was reported as 1.3 mg. per kilogram. The course was stormy but stabilized with
Krukenberg tumor and pregnancy
703
electrolyte balance. During the next 10 days she was given 2 peritoneal infusions of nitrogen mustard 0.2 mg. per kilogram without event ( 200 c.c. of fluid being removed each time). At her insistence, she was dismissed on the nineteenth postoperative day only to be readmitted 4 weeks later after steady deterioration, vomiting, pain, and abdominal distention with fluid. Chest x-ray now showed metastatic pulmonary lesions and she died 2 weeks later on the sixty-seventh day following operation. Surgical pathology. The specimens consisted of a single spherical mass weighing 2,400 grams, measuring 24.0 x 16.0 x 12.0 em. in greatest dimensions, and a piece of indurated omental fat. The tumor surface was smooth and covered by an intact, mottled, grayish red glistening membrane with an attached grossly unremarkable Fallopian tube. The cut surface was tan and roughly lobulated by ill-defined septa, and there were scattered peripheral hemorrhages and cyst formation. Histologically, there were two types of cells supported by edematous connective tissue. One of these represented undifferentiated malignant cells, loosely scattered throughout the stroma and in some areas arranged in small clusters with a pseudogland formation. The cells were charac· terized by a large amount of vacuolated cytoplasm and a small irregularly shaped hyperchromatic nucleus. In some areas the nuclei were compressed and peripherally located, giving· the cells a distinct signet-ring appearance (Fig. 1). Special stains revealed an abundant amount of mucicarmine-positive material within the cytoplasm of these tumor cells (Fig. 2). The second type appeared in groups and clusters of fairly uniform-appearing polyhedral cellular elements. The nucleus was centrally placed, rounded, contained a simple nucleolus, and was surrounded by eosinophilic finely granular cytoplasm. Stains with Sudan IV showed a large amount of sudanophilic material within the cytoplasm (Fig. 3). These cells represent theca I stromal cells having undergone luteinization (Fig. 4). Hemorrhagic necrosis has occurred in several areas. Sections through the Fallopian tube showed clusters of tumor cells within dilated lymphatics. The fatty omental tissue also contained anaplastic tumor cells, many of which had the signet-ring appearance, but in one area the stroma had undergone decidual changes (Fig. 5). Autopsy findings. The postmortem examination
704
Fox and Stamm
July I l!lh'l
Table I. Summary of reported cases of Krukenberg tumor associated with pregnancy·N---------
Author and year
Age
When noted
·-~--
·-
--------
rr _' __ .,. _·
ruutzrn?,
Presenting symptoms
Jlgn.>
1
l.· nilaieral or bilateral
26
5 Months
Pain and abdominal enlargement
l\loJif'
l.lnilateral
Gobiet 17 i909
37
5 Months
Abdominal tumor
:\ow·
Bilateral
Cohn 8
25
3 Months
Vomiting, diarrhea, and abdominal cnlargcmen t
?\iow·
l!nilateral
Hyperemesis
.:\'om·
Bilateral
Burdsinsky"
1908
1910 Schmid 30
t
2-t
1922 Turolt~ 6
1923 Guiroy and Jacobl8
1928 Gauthier-Villarst6
*
8 Months
Abdominal enlargement
*
4y,
Abdominal pain
None
Unilateral
Epigastric pain
None
Bilateral
Months
t
29
1928 Bell and Datnor 4
Bilateral
32
4 Months
Pain, vomiting, and diarrhea
None
C nil a tt·ral
26
712 Months
Chest pain
Yes
Bilateral
t
6Y2 Months
t
None
29
4Y2 Months
t
None
Bilateral
35
6 Months
Pain and vomiting
None
Bilateral
Diarrhea
None
Bilateral
Hyperemesis, abdominal tumor
None
Bilatt'ral
1932 Esau 13
1933 Frankl 14
1933 Frankl14
1933 Puppel2fl
t
1933
37
Wendt"'
16 Weeks
1935 18
von Bud 5
4 Months
1935 Hagstrom~ 0
1938
W atrin, Vermelin, and Chalnot 39
33
23 Weeks
Vomiting
None
Bilateral
28
17 Weeks
Abdominal enlargement
:-.Tone
Bilateral
32
23 Weeks
Abdominal pain
Non<"
Unilateral
32
At term
Tumor found on examination
l\iom·
Bilateral
26
First trimester
Diarrh~a
None
lTnilateral
39
At term
Abdominal pain and tumor
None
Bilateral
1939 Horta Barbosa, Salles, and Pinheiro2 1
1940 de Oliveira
Sarmento~ 8
1942 Garcia Orcoyen 15
and
aseite~
1945 Ameline and co-workers"
1952
*Cases reported by Barata-Ribeiro,a Enzer, 12 Jarcho,2 2 Shaw, 3!! and Vigne-sa 1 and cite-d previously as being ay;;sociated with pre~nancy tinfonnation not given in :report.
Krukenberg tumor and pregnancy
Volume 92 Numbei5
Tumor origin
Obstetric outcome
Treatment of tumor
705
Results Died 3 ~/::! months post partum; metastases
Stomach
Live birth at term
Oophorectomy
Stomach
Intrauterine death
Radical operation and x-ray
Colon
Aborted at 3 months
Oophorectomy
Stomach
Removed
Stomach
Premature live birth
Oophorectomy
Died 3 days after operation; circulatory collapse
Stomach
Delivered at 6Y2 months
None
Died 6 days post partum; perforated stomach
Stomach
Live birth at term
Stomach (pyloris)
Removed
Stomach
Live birth 32 weeks
m
m
utero
utero
Bilateral salpingo-oophorectomy, hysterectomy
t
t Died 3 weeks after operation; torsion and peritonitis
t
t
Bilateral salpingo-oophorectomy, hysterectomy
Died 4Y2 months post partum; carcinomatosis
Bilateral oophorectomy
Died 27 months post partum; intestinal obstruction
t
t
t
Delivered at 6)12 months
Stomach
Delivered at 4Y2 months
Bilateral oophorectomy
Stomach
Cesarean hysterectomy at 6 months
Bilateral salpingo-oophorectomy
Died few days postoperative; ileus
Rectum
Aborted 2 weeks postoperative
Exploratory laparotomy
Died 24 hours postabortal; marasmus
Cesarean section at term live birth
Bilateral oophorectomy
t
Undelivered
Attempted induction of labor
Died during induction; metastases
Hysterectomy at 17 weeks
Hysterectomy, bilateral salpingo-oophorectomy
Died 36 hours after operation
Stomach
Delivered at 26 weeks
None
Died 7 days post partum; torsion and peritonitis
Stomach
Live birth at term
Supravaginal hysterectomy, bilateral salpingooophorectomy
Alive one month after operation
Stomach
Cesarean section, live birth
None
Died aftt'r operation
Stomach
Live birth; pseudohermaphrodite
Hysterectomy, bilateral salpingo-oophorectomy, and gastrectomy
Alive at 4 months
t Stomach
t
could not be verified in the references. 11
t
July I 1%.-,
706 Fox and Stamm
Table
Am.
J.
()b..;t. 8.:
l~vlH'f
I~~Cont'd
Author and year
Age
When noted
Presenting symPtoms
Virilizing signs
Unilnteral or bilateral
Pelvic pressure, vaginal bleeding
None
Bila tr ral
35-36 Weeks
Weight loss, hematemesis
None
Bilateral
32 Weeks
Vomiting
None
Bilateral
Presence of tumor
None
l.' llilatr·ral
Abdominal enlargement; hematemesis
None
Bilateral
Ovarian enlargement
0/une
lJ nilateral
Alter 1 1952
35
3 Months
Alter I 1952
33
Burke 7 1953
22
Moore 26 1954
22
Gustafson, Gardiner, and Stout19 1954
30
t
6 Months
t
13 Weeks
Lawrence, Larson, and Hauge23 1957
20
9 Weeks
Abdominal pain
None
l ' nilateral
Day and Murray 1 0 1958
41
4-5 Months
Abdominal enlargement
:\one
Bilateral
Spadoni 34
20
6
~[onths
En1esis, abdotnina.l pain,
Yes
Unilateral
Yes
Unilateral
Ward 38 1954
and enlargement
1964 Fox and Stamm 1964
27
23 Weeks
Vomiting, constipation, and pain
·---- - --- - ---·--~·----~··-·-- - -.-
Fig. 1. Metastatic tumor cells m ovary. (x430. )
Fig. 2. Mucicarmine positive tumor cells in ovary. (x430.)
was permissively restricted to the abdom en. The extremely emaciated and dehydrated body showed a diffuse growth of black hair over the entire surface. An acneiform rash was present over the face and chest. The entire abdominal and pelvic contents were
fused into a single firm mass by dense fibrous and tumorous adhesions. The stomach measured 12.0 x 6.0 x 6.0 em. in external dimensions and 1 em. in thickness and was lined by a relatively smooth serosal surface. The mucosal surface had a rough, corrugated, and cobblestone appearance
Volume 92 Number 5
Krukenberg tumor and pregnancy
Tumor origin
Obstetric outcome
t
t
Treatment of tumor
707
Results
Removal of tumor after pregnancy
Died 10 months after operation
Stomach
Live birth at 36 weeks
None
Died one week post partum; carcinomatosis
Stomach
Stillborn at 32 weeks
None
Died 2 days post partum; peri toni tis
Apparently aborted
Oophorectomy
Living with possible metastatic symptoms 11 years postoperative; had 2 succeeding pregnancies terminating with live births
Stomach
Cesarean section at 6 months; baby died
Bilateral sal pingo-oophorectomy
Died 6 months after operation; carcinomatosis
Stomach
Live birth at term
Oophorectomy, gastroenterostomy
Died 4 months post partum: carcinomatosis
Primary
Live birth at term
Oophorectomy
Died 3 Y2 months post partum; metastases
Primary
Hysterotomy, 5 months
Hysterectomy, bilateral salpingo-oophorectomy
Died 5 months after operation; carcinomatosis
Breast
Live premature birth at 7 Y2 months
Postpartum hysterectomy, bilateral salpingooophorectomy
Died 6 months after operation; carcinomatosis
Stomach
Live premature birth at 34 weeks; neonatal death
Oophorectomy
Died 7 months post partum: carcinomatosis
t
Fig. 3. Sudan (x430.)
IV~positive
luteinized stromal cells.
(Fig. 6) . The small and large bowel were firmly adherent by hard tumorous and fibrous adhesions, but the mucosal lining appeared uninvolved. The tumor extended retroperitoneally in a haphazard fashion and there was a right hydronephrosis and hydroureter resulting from compression of the
Fig. 4. (x430.)
Luteinization of thecal stromal cells.
lower ureter by tumor. The left ovary could not be identified within the tumor masses. The adrenal glands were not enlarged and grossly not involved by tumor. Microscopic examination revealed a complete replacement and generalized thickening of the
708
Fox and Stamm
Fig. 5. Anaplastic tumor rells and dec idual changes in omentum . ( · 43 0.)
Fig. 6. Postmortem photograph of stomach lesion. Linitis plastica. gastric mucosa by poorly differentiatPd adenocarcinoma. The tumor ct'lls had infiltrated, singly and in small clusters, the underlying submucosa and muscularis layers, producing a fibrous reaction which resulted in marked thickening of the gastric wall, typifying a linitis plastica lesion. Signet-ring cells were scattered throughout the tumor. Retroperitoneal lymph nodes, liver, endometrium, and myometrium, as well as small foci within the submucosa of duodenum and small bowel were seconda rily involved. Comment
The diagnosis of Krukenberg tumor of the ovary before surgical exploration is highly improbable. This is especially true during pregnancy, as shown in this case. Rapidly progressive abdominal pain, tumor enlargement, and encroachment upon the lower bowel associated with sudden dramatic virilization were impressive but gave no clue to the true diagnosis.
july I , 1%5 \m.
J,
Oh:.;t. & Gyncc
More thorough laboratory investigation regarding the extreme masculine chanr.;es would have afforded interesting data. if conditions had been more favorable for the-ir performance. Other cases have documented the presence of high levels of ketosteroid> in these tumors when the luteiniz<·d stroma cells are apparently influenced by such specific types of metastatic neoplasms. Turunen'15 was the first to suggest that the metastatic tumors may be endocrinologically active. He described menstrual irregularities and endometrial hyperplasia in a number of patients , as well as return to normal levels of abnormally elevated estrogen and 17 -ketosteroid \·alues after removal of the involwd ovaries. Scully and Richardson"' also found indirect evidence of hormonal imbala nce in several patients. Most of the hormonally aniw cases previously reported have pointed to the elaboration of estrogenic compounds. Howevt·r , a number of cases with virilization have suggested androgenic activity of the tumor. Histochemical demonstration of steroids in luteinized cells has been tried by a number of methods. These include the Sudan IV stain, phenylhydrazine, and sulfuric acid reactions, as well as evaluation for autofluorescence and birefringence."'· c:. Although a number of functioning tumor~ follow a characteristic staining reaction, the evidence of hormone production by this means is, at best, circumstantial. In some cases of hormonally active tumors, the ex pected histochemical pattern has not been followed." With the recent progress in stProid chemistry, more direct methods of determina tion of abnormal hormonal activity of the diseased ovary have become availabh~. Spadoni, Lindberg, and Herrrnann 3 " were able to isolate a number of hormonal fractions directly from a vi rilizing Krukenberg tumor in a young pregnant woman. They were successful by histochemical techniques in demonstrating probable hormone production by the luteinized stromal cells. In the present case, histochemical studies showed the presence of Sudan IV- positive droplets in the cytoplasm of the luteinized
Volume 92 Number 5
stromal cells. However, application of other known methods for the histologic demonstration of steroids failed to give conclusive results. The marked degree of external virilization of the patient strongly suggests production of androgens by the Krukenberg tumor in the absence of adrenal abnormalities. The low normal postoperative urinary 17 -ketosteroid level is in keeping with normal or low values observed after removal of such tumors. a:>, ":; It is of interest to note that the infant at birth showed a moderate degree of clitoral hypertrophy, indicating excessive androgen production by the mother. The presence of the marked decidual reaction of the omentum also involved by metastatic tumor is somewhat difficult to evaluate. Under circumstances of normal pregnancy, such a reaction would not be surprising. However, Ober and associates~ 7 reported a well-marked decidual reaction of the endometrium in the case of a 46-year-old patient with signs of virilization from a Krukenberg tumor. It appears that the hormone
Krukenberg tumor and pregnancy
709
production by the luteinized stromal cells may be of a rather mixed nature due to elaboration of substances at various levels in the chain of synthesis of steroid hormones." 1 • 3 " Summary
The problem of the Krukenberg tumor complicating pregnancy has been reviewed, and all such case reports have been studied and tabulated with pertinent data abstracted from the 30 known cases. This third known case in which the tumor was involved in extreme androgenic activity and clinical masculinization has been presented with detailed observations and discussion of the clinical and pathological implications.
Grateful appreCiatiOn is expressed to Drs. Arthur T. Hertig, Boston, John I. Brewer, Chicago, and Leslie B. Grams, San Jo>e, for their counsel in reviewing the micropathology in the case presented. Dr. Jorge Franco was very helpful in translating many of the references. The rPferring physician, Dr. Robert J. O'Neill, was most cooperative.
REFERENCE;S
1. Alter, N. M.: Cited by Ovarian Tumor Registry. Personal communication. 2. Ameline, A., LePage, F., Hugier, J., Seneze, J., and Schramm, B.: Arch. mal. app. digest. 41: 565, 1952. 3. Barata Ribeiro, P.: Rev. brasil. cir. 17: 327, 1948. 4. Bell, W. B., and Datnor, M. M.: Am. J. Cancer 16: 439, 1932. 5. von Bud, G.: Orvosi hetil. 79: 146, 1935. 6. Burdsinsky, T. A.: Zentralbl. Gynak. 32: 410, 1908. 7. Burke, S.: J. Obst. & Gynaec. Brit. Emp. 60: 915, 1953. 8. Cohn, F.: Monatsschr. Geburtsh. u. Gynak. 31: 333, 1910. 9. Case Records, Massachusetts General Hospital: New England J. Med. 253: 926, 1955. 10. Day, A., and Murray, D. J.: Canad. M. A. J. 78: 9-4-1, 1958. 11. Diddle, A. W.: Cancer 8: 1026, 1955. 12. Enzer, N.: Ann. Surg. 92: 148, 1930. 13. Esau, P.: Zentralbl. Gynak. 57: 1167, 1933. 14. Frankl, 0.: Zentralbl. Gynak. 57: 788, 1933. 15. Garcia Orcoyen, J.: Rev. espan. cir. 1: 395, 1945. 16. Gauthier-Villars, P.: Ann. d'anat. path. 5: I, 1928.
17. Gobiet, J.: Wien klin. Wcbnschr. 22: 121, 1909. 18. Guiroy, A. J., and Jacob, A.: Bull. Soc. obst. et gynk 17: 535, 1928. 19. Gustafson, G. W., Gardiner, S. H., and Stout, F. E.: AM. J. 0BST. & GYNEC. 67: 1210, 1954. 20. Hagstrom, H. T.: AM. J. 0BST. & GYNEC. 36: 498, 1938. 21. Horta Barbosa, L. A., Salles, N., and Pinheiro, J.: Rev. gynec. et d'obst. 2: 281, 1940. 22. Jarcho, J.: Am. J. Surg. 41: 537, 1938. 23. Lawrence, W. D., Larson, P. N., and Hauge, E. T.: Obst. & Gynec. 10: 84, 1957. 24. McKay, D. J., and Robinson, D.: J. Endocrinol. 41: 378, 1947. 25. McKay, D. J., Robinson, D., and Hertig, A. T.: AM. J. 0BST. & GYNEC. 58: 625, 1949. 26. Moore, J. M.: Cited by Ovarian Tumor Registry. Personal communication. 27. Ober, W. B., Pollak, Ann, Gerstmann, K., and Kupperman, H.: AM. J. 0BsT. & GYNEC. 84: 739, 1962. 28. de Oliveira Sarmento, A.: An. brasil. ginec. 14: 81, 1942. 29. Puppel, E.: Zentralbl. Gynak. 57: 49, 1933. 30. Schmid, H. H.: Arch. Gynak. 117: 418, 1922.
July I. !%')
71 0 Fox and Stamm
31. Scully, R. E., and Richardson, G. S.: Cancer 14: 827, 1961. 32. Shaw, W.: ]. Obst. & Gynaec. Brit. Emp. 33: 256, 1926. 33. Spadoni, L., Lindberg, M., and Herrmann, W. L.: Obst. & Gynec. 23: 630, 1964. 34. Spadoni, L.: Personal communication. 35. Turunen, A.: Acta. endocrinol. 20: 50, 1955. 36. Turolt, Max: Zentralbl. Gynak. 47: 1836, 1923.
Am.
J.
Ob~t.
& Gyncc
37. Vignes, H.: Paris med. 1: 249, 1934. 38. Ward, S. V.: AM. ]. 0BST. & Gv~Ec. 67: 1210, 1954. :l9. Watrin, ].. Vermelin, H .. and Ch:dnot. 1'. · Bull. Soc. gynec. et obst. 28: 37, 1939. +0. Wendt. F.: Svenska lak-tidning 32: 51, J9:Fi. 303 North 15th Street San jose 12, California
LEON PARRISH FOX, M.D. WERNER].
STAMM, M.D.*
San Jose, California
T H E K R U K E N B E R G T U M 0 R IS a very rare and interesting ovarian lesion which has occasionally been found associated with pregnancy. In this extremely unusual case the gestate manifested massive virilization during the development and growth of the tumor. This special, solid type of malignant neoplasm is usually secondary from a gastrointestinal tract or other mucinous gland lesion; but occasionally it is a true primary tumor of the ovary. The gross appearance, growth pattern, and the microscopic characteristics, including the identifying signet-ring ce!ls and alteration of the ovarian stroma, arc well-known features. This tumor is generally regarded as hormonally inactive. However, observations in recent years have pointed to functional hormonal properties in several cases. 31 • 35 This is not surprising in the presence of the marked stromal activity noted in these lesions. The incidence of malignant ovarian neoplasms found during gestation has been reported to be .5.5 per cent. 10 Thirty cases of Krukenberg tumor associated with preg-
nancy have been documented, with pertinent data, and of these, 2 have been determined to be of primary origin (Table I). In 2 other previously reported cases there has been associated extensive masculinization, such as found here. 13 • 34 Case report
A 27-year-old gravida iv, para iii was rcff't-red by her family physician during the thirty-second werk of gestation complaining of obstipation, generalized abdominal pain, and extreme pdvic pressure. Antenatal care had been initiated at the 11fteenth week and recorded as uneventful until the twenty-third wePk when intermittent uterine cramps and constipation started a prog-ressive course without apparent cause. One month latrr. rapid virilization and wasting- began, and a mass was palpated in tht· pelvis adjoining the uterus and fixed at the rectal shelf. Proctological biopsy showed inflammatory reaction only. The past and family histori<'S were irrelt·vant. The menarche occurred at age 1:1 and menses had been regular and normal. Thn·e uncomplicated pregnancies, 6, 4, and 2 )'f'ars prrviously had resulted in living normal children. Examination showrd a small. thin 27-ycar-old gravid patient who had apparently lost considerable' weight recently and aged beyond her years. The facies were masculine, gaunt. and anxious with striking- acne and hirsutism extending over the body and exhibiting- a male escutcheon. The breasts were of medium size, flat, and colostrum was present. The abdomen was tPrrn pregnancy size, and then· was edema of the wall. A large, firm, tender mass was palpable in the right flank area contiguous with the uterus and extending into the pelvis. Free fluid signs were inconclusive. Vulvar and vaginal
From the Departments of Obstetrics and Gynecology and Pathology, O'Connor Hospital. *Present address: Dominican Santa Cruz HosPital, Santa Cruz, California. Presented as a part of a Symposium of Interesting and Unusual Cases, at the Thirty-first Annual Meeting of the Pacific Coast Obstetrical and Gynecological Society, Santa Barbara, California, Nov. 4-7, 1964.
702
Volume 92 ~umber 5
edema were present but the clitoris was not enlarged. Bimanually, the mass was palpable in the posterior cul-de-sac area and involved the rectum at 7 em., fixed in the sacral curve. Vaginal cytology showed no abnormal cells and exhibited a normal pregnancy pattern. Advised hospitalization for proper evaluation and treatment was refused by the patient until 2 and one-half weeks later when vomiting and discomfort caused admission. She arrived in active labor and promptly was delivered of a 3yt pounds female infant who died in a few hours with respiratory difficulty. There was noticeable enlargement of the clitoris but no other fetal abnormalities were noted. Postdelivery examination showed a seriously ill patient with dehydration and exhaustion. The temperature was 99.6° F., pulse 128, respiration 24, and blood pressure 132/90. Virilization had increased and the abdomen was distended with fluid. The uterus was firm and deflected to the left by a 25 em. hard mass. Above the uterus there was another hard mass about 10 em. in diameter. Laboratory studies were not remarkable. The blood picture and urine were consistent with dehydration. The chest and bone survey x-rays showed no metastatic lesions. Fluid balance was stabilized and laparotomy was done on the fourth postpartum day. The 3,000 c.c. of blood-tinged ascitic fluid was aspirated. The right ovary was completely involved in a hard tumor mass with the tube adherent and was easily delivered and removed. The uterus. left ovary, and tube appeared to be normal. Th<" greater omentum was thick, indurated, and enlarged into a 12 em. mass fixed ben('ath the transverse colon on the left side. The thickened pelvic peritoneum was studded with tumor, while the posterior cul-de-sac and sigmoid were densely infiltrated. The stomach, gallbladder, and small bowel were matted together by soft, irregular adhesions, but no specific neoplasm could be identified. The liver, spleen, and kidneys were not at this time grossly involved. A wedge of the omentum was removed for study and the abdomen was closed. A catheter conduit was fixed in the left lower quadrant for chemotherapy administration. Cytological study of the peritoneal fluid showed malignant cells. A 17-ketosteroid determination shortly after operation was reported as 1.3 mg. per kilogram. The course was stormy but stabilized with
Krukenberg tumor and pregnancy
703
electrolyte balance. During the next 10 days she was given 2 peritoneal infusions of nitrogen mustard 0.2 mg. per kilogram without event ( 200 c.c. of fluid being removed each time). At her insistence, she was dismissed on the nineteenth postoperative day only to be readmitted 4 weeks later after steady deterioration, vomiting, pain, and abdominal distention with fluid. Chest x-ray now showed metastatic pulmonary lesions and she died 2 weeks later on the sixty-seventh day following operation. Surgical pathology. The specimens consisted of a single spherical mass weighing 2,400 grams, measuring 24.0 x 16.0 x 12.0 em. in greatest dimensions, and a piece of indurated omental fat. The tumor surface was smooth and covered by an intact, mottled, grayish red glistening membrane with an attached grossly unremarkable Fallopian tube. The cut surface was tan and roughly lobulated by ill-defined septa, and there were scattered peripheral hemorrhages and cyst formation. Histologically, there were two types of cells supported by edematous connective tissue. One of these represented undifferentiated malignant cells, loosely scattered throughout the stroma and in some areas arranged in small clusters with a pseudogland formation. The cells were charac· terized by a large amount of vacuolated cytoplasm and a small irregularly shaped hyperchromatic nucleus. In some areas the nuclei were compressed and peripherally located, giving· the cells a distinct signet-ring appearance (Fig. 1). Special stains revealed an abundant amount of mucicarmine-positive material within the cytoplasm of these tumor cells (Fig. 2). The second type appeared in groups and clusters of fairly uniform-appearing polyhedral cellular elements. The nucleus was centrally placed, rounded, contained a simple nucleolus, and was surrounded by eosinophilic finely granular cytoplasm. Stains with Sudan IV showed a large amount of sudanophilic material within the cytoplasm (Fig. 3). These cells represent theca I stromal cells having undergone luteinization (Fig. 4). Hemorrhagic necrosis has occurred in several areas. Sections through the Fallopian tube showed clusters of tumor cells within dilated lymphatics. The fatty omental tissue also contained anaplastic tumor cells, many of which had the signet-ring appearance, but in one area the stroma had undergone decidual changes (Fig. 5). Autopsy findings. The postmortem examination
704
Fox and Stamm
July I l!lh'l
Table I. Summary of reported cases of Krukenberg tumor associated with pregnancy·N---------
Author and year
Age
When noted
·-~--
·-
--------
rr _' __ .,. _·
ruutzrn?,
Presenting symptoms
Jlgn.>
1
l.· nilaieral or bilateral
26
5 Months
Pain and abdominal enlargement
l\loJif'
l.lnilateral
Gobiet 17 i909
37
5 Months
Abdominal tumor
:\ow·
Bilateral
Cohn 8
25
3 Months
Vomiting, diarrhea, and abdominal cnlargcmen t
?\iow·
l!nilateral
Hyperemesis
.:\'om·
Bilateral
Burdsinsky"
1908
1910 Schmid 30
t
2-t
1922 Turolt~ 6
1923 Guiroy and Jacobl8
1928 Gauthier-Villarst6
*
8 Months
Abdominal enlargement
*
4y,
Abdominal pain
None
Unilateral
Epigastric pain
None
Bilateral
Months
t
29
1928 Bell and Datnor 4
Bilateral
32
4 Months
Pain, vomiting, and diarrhea
None
C nil a tt·ral
26
712 Months
Chest pain
Yes
Bilateral
t
6Y2 Months
t
None
29
4Y2 Months
t
None
Bilateral
35
6 Months
Pain and vomiting
None
Bilateral
Diarrhea
None
Bilateral
Hyperemesis, abdominal tumor
None
Bilatt'ral
1932 Esau 13
1933 Frankl 14
1933 Frankl14
1933 Puppel2fl
t
1933
37
Wendt"'
16 Weeks
1935 18
von Bud 5
4 Months
1935 Hagstrom~ 0
1938
W atrin, Vermelin, and Chalnot 39
33
23 Weeks
Vomiting
None
Bilateral
28
17 Weeks
Abdominal enlargement
:-.Tone
Bilateral
32
23 Weeks
Abdominal pain
Non<"
Unilateral
32
At term
Tumor found on examination
l\iom·
Bilateral
26
First trimester
Diarrh~a
None
lTnilateral
39
At term
Abdominal pain and tumor
None
Bilateral
1939 Horta Barbosa, Salles, and Pinheiro2 1
1940 de Oliveira
Sarmento~ 8
1942 Garcia Orcoyen 15
and
aseite~
1945 Ameline and co-workers"
1952
*Cases reported by Barata-Ribeiro,a Enzer, 12 Jarcho,2 2 Shaw, 3!! and Vigne-sa 1 and cite-d previously as being ay;;sociated with pre~nancy tinfonnation not given in :report.
Krukenberg tumor and pregnancy
Volume 92 Numbei5
Tumor origin
Obstetric outcome
Treatment of tumor
705
Results Died 3 ~/::! months post partum; metastases
Stomach
Live birth at term
Oophorectomy
Stomach
Intrauterine death
Radical operation and x-ray
Colon
Aborted at 3 months
Oophorectomy
Stomach
Removed
Stomach
Premature live birth
Oophorectomy
Died 3 days after operation; circulatory collapse
Stomach
Delivered at 6Y2 months
None
Died 6 days post partum; perforated stomach
Stomach
Live birth at term
Stomach (pyloris)
Removed
Stomach
Live birth 32 weeks
m
m
utero
utero
Bilateral salpingo-oophorectomy, hysterectomy
t
t Died 3 weeks after operation; torsion and peritonitis
t
t
Bilateral salpingo-oophorectomy, hysterectomy
Died 4Y2 months post partum; carcinomatosis
Bilateral oophorectomy
Died 27 months post partum; intestinal obstruction
t
t
t
Delivered at 6)12 months
Stomach
Delivered at 4Y2 months
Bilateral oophorectomy
Stomach
Cesarean hysterectomy at 6 months
Bilateral salpingo-oophorectomy
Died few days postoperative; ileus
Rectum
Aborted 2 weeks postoperative
Exploratory laparotomy
Died 24 hours postabortal; marasmus
Cesarean section at term live birth
Bilateral oophorectomy
t
Undelivered
Attempted induction of labor
Died during induction; metastases
Hysterectomy at 17 weeks
Hysterectomy, bilateral salpingo-oophorectomy
Died 36 hours after operation
Stomach
Delivered at 26 weeks
None
Died 7 days post partum; torsion and peritonitis
Stomach
Live birth at term
Supravaginal hysterectomy, bilateral salpingooophorectomy
Alive one month after operation
Stomach
Cesarean section, live birth
None
Died aftt'r operation
Stomach
Live birth; pseudohermaphrodite
Hysterectomy, bilateral salpingo-oophorectomy, and gastrectomy
Alive at 4 months
t Stomach
t
could not be verified in the references. 11
t
July I 1%.-,
706 Fox and Stamm
Table
Am.
J.
()b..;t. 8.:
l~vlH'f
I~~Cont'd
Author and year
Age
When noted
Presenting symPtoms
Virilizing signs
Unilnteral or bilateral
Pelvic pressure, vaginal bleeding
None
Bila tr ral
35-36 Weeks
Weight loss, hematemesis
None
Bilateral
32 Weeks
Vomiting
None
Bilateral
Presence of tumor
None
l.' llilatr·ral
Abdominal enlargement; hematemesis
None
Bilateral
Ovarian enlargement
0/une
lJ nilateral
Alter 1 1952
35
3 Months
Alter I 1952
33
Burke 7 1953
22
Moore 26 1954
22
Gustafson, Gardiner, and Stout19 1954
30
t
6 Months
t
13 Weeks
Lawrence, Larson, and Hauge23 1957
20
9 Weeks
Abdominal pain
None
l ' nilateral
Day and Murray 1 0 1958
41
4-5 Months
Abdominal enlargement
:\one
Bilateral
Spadoni 34
20
6
~[onths
En1esis, abdotnina.l pain,
Yes
Unilateral
Yes
Unilateral
Ward 38 1954
and enlargement
1964 Fox and Stamm 1964
27
23 Weeks
Vomiting, constipation, and pain
·---- - --- - ---·--~·----~··-·-- - -.-
Fig. 1. Metastatic tumor cells m ovary. (x430. )
Fig. 2. Mucicarmine positive tumor cells in ovary. (x430.)
was permissively restricted to the abdom en. The extremely emaciated and dehydrated body showed a diffuse growth of black hair over the entire surface. An acneiform rash was present over the face and chest. The entire abdominal and pelvic contents were
fused into a single firm mass by dense fibrous and tumorous adhesions. The stomach measured 12.0 x 6.0 x 6.0 em. in external dimensions and 1 em. in thickness and was lined by a relatively smooth serosal surface. The mucosal surface had a rough, corrugated, and cobblestone appearance
Volume 92 Number 5
Krukenberg tumor and pregnancy
Tumor origin
Obstetric outcome
t
t
Treatment of tumor
707
Results
Removal of tumor after pregnancy
Died 10 months after operation
Stomach
Live birth at 36 weeks
None
Died one week post partum; carcinomatosis
Stomach
Stillborn at 32 weeks
None
Died 2 days post partum; peri toni tis
Apparently aborted
Oophorectomy
Living with possible metastatic symptoms 11 years postoperative; had 2 succeeding pregnancies terminating with live births
Stomach
Cesarean section at 6 months; baby died
Bilateral sal pingo-oophorectomy
Died 6 months after operation; carcinomatosis
Stomach
Live birth at term
Oophorectomy, gastroenterostomy
Died 4 months post partum: carcinomatosis
Primary
Live birth at term
Oophorectomy
Died 3 Y2 months post partum; metastases
Primary
Hysterotomy, 5 months
Hysterectomy, bilateral salpingo-oophorectomy
Died 5 months after operation; carcinomatosis
Breast
Live premature birth at 7 Y2 months
Postpartum hysterectomy, bilateral salpingooophorectomy
Died 6 months after operation; carcinomatosis
Stomach
Live premature birth at 34 weeks; neonatal death
Oophorectomy
Died 7 months post partum: carcinomatosis
t
Fig. 3. Sudan (x430.)
IV~positive
luteinized stromal cells.
(Fig. 6) . The small and large bowel were firmly adherent by hard tumorous and fibrous adhesions, but the mucosal lining appeared uninvolved. The tumor extended retroperitoneally in a haphazard fashion and there was a right hydronephrosis and hydroureter resulting from compression of the
Fig. 4. (x430.)
Luteinization of thecal stromal cells.
lower ureter by tumor. The left ovary could not be identified within the tumor masses. The adrenal glands were not enlarged and grossly not involved by tumor. Microscopic examination revealed a complete replacement and generalized thickening of the
708
Fox and Stamm
Fig. 5. Anaplastic tumor rells and dec idual changes in omentum . ( · 43 0.)
Fig. 6. Postmortem photograph of stomach lesion. Linitis plastica. gastric mucosa by poorly differentiatPd adenocarcinoma. The tumor ct'lls had infiltrated, singly and in small clusters, the underlying submucosa and muscularis layers, producing a fibrous reaction which resulted in marked thickening of the gastric wall, typifying a linitis plastica lesion. Signet-ring cells were scattered throughout the tumor. Retroperitoneal lymph nodes, liver, endometrium, and myometrium, as well as small foci within the submucosa of duodenum and small bowel were seconda rily involved. Comment
The diagnosis of Krukenberg tumor of the ovary before surgical exploration is highly improbable. This is especially true during pregnancy, as shown in this case. Rapidly progressive abdominal pain, tumor enlargement, and encroachment upon the lower bowel associated with sudden dramatic virilization were impressive but gave no clue to the true diagnosis.
july I , 1%5 \m.
J,
Oh:.;t. & Gyncc
More thorough laboratory investigation regarding the extreme masculine chanr.;es would have afforded interesting data. if conditions had been more favorable for the-ir performance. Other cases have documented the presence of high levels of ketosteroid> in these tumors when the luteiniz<·d stroma cells are apparently influenced by such specific types of metastatic neoplasms. Turunen'15 was the first to suggest that the metastatic tumors may be endocrinologically active. He described menstrual irregularities and endometrial hyperplasia in a number of patients , as well as return to normal levels of abnormally elevated estrogen and 17 -ketosteroid \·alues after removal of the involwd ovaries. Scully and Richardson"' also found indirect evidence of hormonal imbala nce in several patients. Most of the hormonally aniw cases previously reported have pointed to the elaboration of estrogenic compounds. Howevt·r , a number of cases with virilization have suggested androgenic activity of the tumor. Histochemical demonstration of steroids in luteinized cells has been tried by a number of methods. These include the Sudan IV stain, phenylhydrazine, and sulfuric acid reactions, as well as evaluation for autofluorescence and birefringence."'· c:. Although a number of functioning tumor~ follow a characteristic staining reaction, the evidence of hormone production by this means is, at best, circumstantial. In some cases of hormonally active tumors, the ex pected histochemical pattern has not been followed." With the recent progress in stProid chemistry, more direct methods of determina tion of abnormal hormonal activity of the diseased ovary have become availabh~. Spadoni, Lindberg, and Herrrnann 3 " were able to isolate a number of hormonal fractions directly from a vi rilizing Krukenberg tumor in a young pregnant woman. They were successful by histochemical techniques in demonstrating probable hormone production by the luteinized stromal cells. In the present case, histochemical studies showed the presence of Sudan IV- positive droplets in the cytoplasm of the luteinized
Volume 92 Number 5
stromal cells. However, application of other known methods for the histologic demonstration of steroids failed to give conclusive results. The marked degree of external virilization of the patient strongly suggests production of androgens by the Krukenberg tumor in the absence of adrenal abnormalities. The low normal postoperative urinary 17 -ketosteroid level is in keeping with normal or low values observed after removal of such tumors. a:>, ":; It is of interest to note that the infant at birth showed a moderate degree of clitoral hypertrophy, indicating excessive androgen production by the mother. The presence of the marked decidual reaction of the omentum also involved by metastatic tumor is somewhat difficult to evaluate. Under circumstances of normal pregnancy, such a reaction would not be surprising. However, Ober and associates~ 7 reported a well-marked decidual reaction of the endometrium in the case of a 46-year-old patient with signs of virilization from a Krukenberg tumor. It appears that the hormone
Krukenberg tumor and pregnancy
709
production by the luteinized stromal cells may be of a rather mixed nature due to elaboration of substances at various levels in the chain of synthesis of steroid hormones." 1 • 3 " Summary
The problem of the Krukenberg tumor complicating pregnancy has been reviewed, and all such case reports have been studied and tabulated with pertinent data abstracted from the 30 known cases. This third known case in which the tumor was involved in extreme androgenic activity and clinical masculinization has been presented with detailed observations and discussion of the clinical and pathological implications.
Grateful appreCiatiOn is expressed to Drs. Arthur T. Hertig, Boston, John I. Brewer, Chicago, and Leslie B. Grams, San Jo>e, for their counsel in reviewing the micropathology in the case presented. Dr. Jorge Franco was very helpful in translating many of the references. The rPferring physician, Dr. Robert J. O'Neill, was most cooperative.
REFERENCE;S
1. Alter, N. M.: Cited by Ovarian Tumor Registry. Personal communication. 2. Ameline, A., LePage, F., Hugier, J., Seneze, J., and Schramm, B.: Arch. mal. app. digest. 41: 565, 1952. 3. Barata Ribeiro, P.: Rev. brasil. cir. 17: 327, 1948. 4. Bell, W. B., and Datnor, M. M.: Am. J. Cancer 16: 439, 1932. 5. von Bud, G.: Orvosi hetil. 79: 146, 1935. 6. Burdsinsky, T. A.: Zentralbl. Gynak. 32: 410, 1908. 7. Burke, S.: J. Obst. & Gynaec. Brit. Emp. 60: 915, 1953. 8. Cohn, F.: Monatsschr. Geburtsh. u. Gynak. 31: 333, 1910. 9. Case Records, Massachusetts General Hospital: New England J. Med. 253: 926, 1955. 10. Day, A., and Murray, D. J.: Canad. M. A. J. 78: 9-4-1, 1958. 11. Diddle, A. W.: Cancer 8: 1026, 1955. 12. Enzer, N.: Ann. Surg. 92: 148, 1930. 13. Esau, P.: Zentralbl. Gynak. 57: 1167, 1933. 14. Frankl, 0.: Zentralbl. Gynak. 57: 788, 1933. 15. Garcia Orcoyen, J.: Rev. espan. cir. 1: 395, 1945. 16. Gauthier-Villars, P.: Ann. d'anat. path. 5: I, 1928.
17. Gobiet, J.: Wien klin. Wcbnschr. 22: 121, 1909. 18. Guiroy, A. J., and Jacob, A.: Bull. Soc. obst. et gynk 17: 535, 1928. 19. Gustafson, G. W., Gardiner, S. H., and Stout, F. E.: AM. J. 0BST. & GYNEC. 67: 1210, 1954. 20. Hagstrom, H. T.: AM. J. 0BST. & GYNEC. 36: 498, 1938. 21. Horta Barbosa, L. A., Salles, N., and Pinheiro, J.: Rev. gynec. et d'obst. 2: 281, 1940. 22. Jarcho, J.: Am. J. Surg. 41: 537, 1938. 23. Lawrence, W. D., Larson, P. N., and Hauge, E. T.: Obst. & Gynec. 10: 84, 1957. 24. McKay, D. J., and Robinson, D.: J. Endocrinol. 41: 378, 1947. 25. McKay, D. J., Robinson, D., and Hertig, A. T.: AM. J. 0BST. & GYNEC. 58: 625, 1949. 26. Moore, J. M.: Cited by Ovarian Tumor Registry. Personal communication. 27. Ober, W. B., Pollak, Ann, Gerstmann, K., and Kupperman, H.: AM. J. 0BsT. & GYNEC. 84: 739, 1962. 28. de Oliveira Sarmento, A.: An. brasil. ginec. 14: 81, 1942. 29. Puppel, E.: Zentralbl. Gynak. 57: 49, 1933. 30. Schmid, H. H.: Arch. Gynak. 117: 418, 1922.
July I. !%')
71 0 Fox and Stamm
31. Scully, R. E., and Richardson, G. S.: Cancer 14: 827, 1961. 32. Shaw, W.: ]. Obst. & Gynaec. Brit. Emp. 33: 256, 1926. 33. Spadoni, L., Lindberg, M., and Herrmann, W. L.: Obst. & Gynec. 23: 630, 1964. 34. Spadoni, L.: Personal communication. 35. Turunen, A.: Acta. endocrinol. 20: 50, 1955. 36. Turolt, Max: Zentralbl. Gynak. 47: 1836, 1923.
Am.
J.
Ob~t.
& Gyncc
37. Vignes, H.: Paris med. 1: 249, 1934. 38. Ward, S. V.: AM. ]. 0BST. & Gv~Ec. 67: 1210, 1954. :l9. Watrin, ].. Vermelin, H .. and Ch:dnot. 1'. · Bull. Soc. gynec. et obst. 28: 37, 1939. +0. Wendt. F.: Svenska lak-tidning 32: 51, J9:Fi. 303 North 15th Street San jose 12, California