- Email: [email protected]
Renal hypouricemia: Prevention of exercise-induced acute renal failure and a review of the literature
Renal Hypouricemia: Prevention of Exercise-Induced Acute Renal Failure and a Review of the Literature Jane Y. Yeun, MD, and James A. Hasbargen,
MD
0 Isolated renal hypouricemia from defective uric acid reabsorption and/or secretion is a well-described entity, with a prevalence of 0.12% to 0.20% in Japan. It is rarely associated with exercise-induced acute renal failure (ARF). The etiology of ARF is debated. Prevention of ARF in renal hypouricemia has not been previously addressed. A 29-year-old Pakistani man had recurrent exercise-induced ARF. He was found to have isolated renal hypouricemia: serum uric acid 0.5 mg/dL, 24-hour urine uric acid 472 t- 25 mg (-t-SD), and fractional excretion of uric acid 55.2% to 69.4%. Both pyrazinamide and probenecid decreased fractional excretion of uric acid and uric acid in our patient, suggesting either a partial presecretory and postsecretory reabsorption excretion rate (UV,,d defect or increased secretion. We investigated renal uric acid excretion during exercise in our patient and four control subjects. All five subjects underwent a physical fitness test (PFI). Our patient developed ARF. Uric acid excretion rate increased in our patient, from 0.46 mg/min at baseline to 1.49 mg/min 4 hours after the PFT, as did the urine uric acid to urine creatinine ratio (U&J,J (0.29 to 1.49). In the controls, UVurate and Uua/lJcr were unchanged after the PFR UVurate was 0.46 2 0.10 mg/min at baseline and 0.59 -f 0.04 mg/min 4 hours after the PFT, while UuA/UCr was 0.30 lr 0.04 at baseline and 0.36 2 0.04 at 4 hours. All five subjects took allopurinol 300 mg daily for 5 days and repeated the PFT. In our patient, allopurinol prevented the ARF as well as the exerciseinduced increases in UVumte (0.28 mg/min to 0.22 mg/min) and Uun/lJcr (0.25 to 0.17). In the controls, the UVurat. and Uun/Ucr responses to exercise were not altered. We conclude that increased renal excretion of uric acid during exercise was responsible for the ARF in our patient with renal hypouricemia and that successful prophylaxis with allopurinol is possible. This is a US government work. There are no restrictions on its use. INDEX
WORDS:
Renal
hypouricemia;
exercise;
acute
R
ENAL HYPOURICEMIA results from an isolated renal tubular defect in reabsorption and/or secretion of uric acid that is genetically determined in an autosomal recessive inheritance pattern.’ It is a rare condition with a reported incidence of 0.12% to 0.20% in Japan.233There are many cases of renal hypouricemia reported in the literature.3-54 However, until 1989, the only adverse effects of renal hypouricemia were thought to be decreased bone density,4 uric acid nephrolithiasis,3*5-13 and possibly calcium nephrolithiasis,4,‘4-20 as documented in case reports. Since then, eight cases of exercise-induced acute renal failure (ARF) have been reported in patients with renal hypouricemia.2’~26 However, only one of these eight patients had recurrent ARFz2 (two episodes). The prevention of exercise-induced ARF has not been addressed. We report an individual with renal hypouricemia who developed recurrent ARF after exercise on at least three occasions. Because of his desire to remain active, we explored potential methods of preventing the ARF. We performed a review of the literature on isolated renal hypouricemia and provide a summary of our results. CASE An otherwise to the emergency American
Journal
REPORT
healthy 29-year-old Pakistani man presented department on March 3, 1993, with nausea, of Kidney
Diseases,
renal
failure;
hypouricemia;
allopurinol;
prophylaxis.
vomiting, and abdominal pain 4 hours after a semiannual physical fitness test (PFT). The PFf consisted of a 2-mile run, sit-ups, and push-ups. He denied any illness, viral prodrome, or nonsteroidal anti-inflammatory drug ingestion prior to exercising. He had been training 3 days a week for the PFT, although at lesser levels of exertion. Of interest, our patient had two prior episodes of similar symptoms occurring shortly after the PFf that were associated with non-oliguric AW. The first episode occurred elsewhere in May 1992; no further evaluation was performed during that admission. The second episode occurred in Denver, CO, in October 1992, with serum creatinine (Sc,) peaking at 4.0 mg/dL. Past medical history was otherwise unremarkable. There is no family history of muscle disorders. However, the patient’s father had end-stage renal disease from nephrolithiasis of unknown composition; a brother has a history of calcium
From the Department of Medicine, Nephrology Service, Fitzsimons Army Medical Center, Aurora, CO; and Indiana University and Veterans Administration Medical Center, Indianapolis, IN. Received September 8, 1994; accepted in revisedform January 20, 1995. The opinions and research contained herein are theprivate ones of the authors and are not to be considered as ofjcial or rejlecting the views of the Department of the Army or the Department of Defense. Address reprint requests to Jane Y. Yeun, MD, Nephrology Service, MCHG-MD& Fitzsimons Army Medical Center, Aurora, CO 80045. This is a US government work. There are no restrictions on its use. 0272-6386/95/2506-0018$0.00/O
Vol 25, No 6 (June), 1995: pp 937-946
937
YEUN
oxalate stones. We were unable to obtain serum uric acid (St,*) levels in any of the relatives. On physical examination, the blood pressure was 132/74 mm Hg without orthostasis and the pulse was 80 beats/min. Examination was entirely unremarkable except for mild abdominal tenderness to palpation, poorly localized, without rebound tenderness. There was no muscle swelling or tenderness. Laboratory evaluation revealed a sodium of 138 mmol/L, potassium 4.1 mmol/L, chloride 108 mmol/L, bicarbonate 18 mmol/L, urea nitrogen 30 mg/dL, creatinine 4.7 mg/dL, calcium 8.8 mg/dL, phosphate 3.6 mg/dL, uric acid 2.1 mg/ dL, creatine kinase 107 U/L, and fractional excretion of sodium 3.3%. Urinalysis revealed a specific gravity of 1.004, 2+ blood, no glucose, pH 6.0, 2 to 4 white blood cells/highpowered field, 0 to 2 red blood cells/high-powered field, rare renal tubular epithelial cells, and rare uric acid crystals. Renal ultrasound was unremarkable, demonstrating normal-sized kidneys without hydronephrosis. The nausea, vomiting, and abdominal pain resolved spontaneously in 24 hours. With conservative therapy, the nonoliguric ARF improved and S, was 1.9 mg/dL at discharge (8 days after initial presentation). During follow-up on April 12, 1993, Scr was 1.1 mg/dL, accompanied by a SuA of 0.5 mgl dL and serum bicarbonate of 26 mmol/L. Subsequent 24hour urine collections revealed 472 ? 25 mg of uric acid (n = 3), uric acid clearance (Cu,) of 57.4 to 65.8 mL/min, fractional excretion of uric acid (F&A) of 55.2% to 69.4%, and normal phosphate (8 14 mg) and calcium (70 to 110 mg; normal range, 42 to 353 mg) excretion. There was no glycosuria or abnormal amino acid excretion. Our patient underwent repeat exercise testing to assess reproducibility of ARF. During the first exercise testing, ARF was reproduced with Seepeaking at 2.5 mg/dL on day 2 after PFT. Magnetic resonance imaging with gadolinium contrast was performed less than 24 hours after the PFT, while a dimercaptosuccinic acid (DMSA) renal scan was done within 48 hours of the PFT to assessrenal cortical perfusion. Subsequent exercise tests were performed to assess the effect of exercise on renal function and uric acid excretion. Four normal male volunteers underwent concomitant exercise testing and served as controls. Informed consent was obtained from all subjects. MATERIALS
AND
Uric acid excretion rate (UVurate) , FaUA, and creatinine clearance (C,) were measured at baseline and after pyrazinamide 3.0 g orally, following the modified method of Steele and Rieselbach.55 After establishing free water diuresis, 30minutes urine collections were obtained, two at baseline and three starting 1 hour after pyrazinamide administration. The effect of probenecid 2.0 g orally on UVurater F&A, and Cc, were measured in an identical fashion 4 days later.
ESfect of Exercise on Renal Function Timed urine collections and blood were obtained at baseline for measurement of Ccr, F&A, S*, U,,/&, and UV,, in our patient and four healthy volunteers from 21 to 41 years
HASBARGEN
of age. Each subject then underwent a standardized PFT, consisting of push-ups and sit-ups to exhaustion over 2 minutes each, and a 2-mile run. Timed urine collections and blood were again obtained at 1 hour, 4 hours, and 24 hours after exercise to allow calculation of the same parameters. All urine samples were spontaneously voided. All subjects ate and drank ad libitum. After each subject had taken allopurinol 300 mg daily for 5 days, the above studies were repeated.
Assays Uric acid was measured using the uricase method,56 with reported accuracy down to 0.2 mg/dL. Creatinine measurements were performed using the Kodak Ektachem system (Rochester, NY).
Literature Review A review of the literature on isolated renal hypouricemia3-54 was performed through use of a MEDLINE search and perusal of bibliographic citations. Any patients who had another potential etiology for uricosuria and resultant hypouricemia (eg, diabetes mellitus,26,39renal tubular damage from renal tuberculosisi or interstitial nephritisI and nephrotic syndrome33) were excluded from this review. The articles were reviewed for the number of individuals or families with isolated renal hypouricemia, gender, age, ethnicity, S“AI F&A, the type of tubular transport defect, and any complications arising directly or indirectly from the renal hypouricemia. Any individual reported as having a similarly affected family member was included in the family category. Turkish Jews, Iraqi Jews, and Libyan Jews were included under the non-Ashkenazi Jew ethnic group. The investigators’ classification of the tubular transport defect after pyrazinamide, probenecid, and/or benzbromarone testing was assumed to be correct. When a classification was not attempted, Sperling’s’ criteria for the classification of type of defect was applied to the data. Complications from renal hypouricemia were summarized as the number of individuals with the complication when there was no family history of renal hypouricemia and as the number of families with the complication when there was a family history of renal hypouricemia, even if only one member of the family was described in sufficient detail.
METHODS
Tubular Function
AND
RESULTS
Tubular Function Administration of pyrazinamide decreased CuA (421 + 38 mL/min to 113 t- 4 mLknin), F&A (360% -+ 24% to 112% + l%), and UVu,,JCc, (3.59 ? 0.23 yg/rnL to 1.12 + 0.01 pg/mL) (Table 1). Pyrazinamide is thought to inhibit secretion of uric acid in the proximal tubule. In our patient, pyrazinamide decreased the excretion of uric acid nearly fourfold. Although probenecid at lower doses can inhibit secretion of uric acid, at the doses used here, it inhibits predominantly postsecretory re-
RENAL
HYPOURICEMIA Table
1. Effect
AND
EXERCISE-INDUCED
of Pyrazinamide
and
939
ARF
Probenecid
on Renal
Tubular
Handling
Pyrazinamide
Time (min)
%A (mg/dL)
C (ml/&)
C (ml.IGin)
of Uric
Acid
in Our
Patient
Probenecid wra&c, WmL)
FEUA (%)
-60 to -30 -30 to 0 Mean 2 SE
0.1 0.1 0.1
459 383 421 238
120 383 114 336 117+-3 360+-24 3 g orally
3.82 3.36 3.59-t0.23
T=O +60 to +90 +90 to +120 +I20 to +150 Mean + SE
0.1 0.1 0.1 0.1
105 115 120 113 i 4
92 104 106 101 ? 4
1.14 1.10 1.12 1.12 e 0.01
114 111 112 112 ?z 1
absorption of uric acid and, to a lesser extent, presecretory reabsorption.‘y57 Therefore, probenecid administration should increase uric acid excretion if reabsorptive function is intact and should have no effect on uric acid excretion if reabsorptive function is defective. In our patient, probenecid was observed to decrease urinary uric acid excretion (Table 1) by nearly half of all calculated parameters. The baseline values for CuA and F&A in the pyrazinamide test are markedly disparate from those in the probenecid test (Table 1) because of the wide variations in measuring our patient’s SuA (0.1 to 0.6 mg/dL) at the lower end of resolution of the assay. However, since UVu,,/Cc, does not include SuA, these data are directly comparable at baseline between the two tests. Renal Cortical Per@sion During Acute Renal Failure
S (mg:L)
C”, (mUmin)
C cr (mUmin)
0.6 0.5 0.55 t 0.05
82.8 91.6 87.2 f 4.4
120 111 116 t 4 2 g orally
69.2 82.2 75.7 i 6.5
4.14 4.13 4.14
0.5 0.5 0.5 0.5
61.2 55.6 51.7 56.2 -c 2.8
102 104 110 105 ? 2
60.3 53.5 47.1 53.6 I 3.8
3.00 2.67 2.35 2.67 ? 0.19
FJJA (%)
wJra&cr WmL)
PFI after allopurinol(75% to 74%, 93% to 94%, 92% to 95%) except for one subject, whose performance improved during the second PIT (59% to 73%). Effect of Exercise on Renal Function
Acute renal failure was reproduced in our patient during PIT, with Ccr decreasing from 151 to 77 mL/min by 4 hours and 46 mL/min by 24 hours (Fig 1). The control subjects retained normal renal function with exercise (138 +- 14 mL/min baseline to 141 + 12 r&/mm at 4 hours and 135 2 22 mL/min at 24 hours; Fig 1). Interestingly, UuA/UCr ratio was markedly elevated in our patient at 4 hours after exercise (0.29 at baseline to 1.49 at 4 hours; Fig 2), associated with a UVUratethat increased from 0.48 mg/min at baseline to 1.49 mg/min at 4 hours (data not shown
Magnetic resonance imaging with gadolinium contrast performed less than 24 hours after an episode of exercise-induced ARF revealed no cortical perfusion defects. A DMSA renal scan performed within 48 hours also revealed no perfusion defects.
1
Extent of Exercise Petiormed
There are age-specific standards set for the PIT, with 100% being a perfect score for the particular age group and 60% a passing score. Compared with other individuals in his age group, our patient performed at 62% for his baseline PFI and 65% for the PFT after allopurinol ingestion. The control subjects’ performances were comparable from the baseline PPT to the
Fig 1. Effect of exercise on Ccr in control subjects and patient with renal hypouricemia at baseline and after allopurinol.
YEUN
Fig 2. Effect of exercise jects and patient with renal and after allopurinol.
on Uun/Ucr hypouricemia
in control subat baseline
in graphic form since the graph is almost identical in appearance to that for UUA/UCrr shown in Fig 2). Such an increase in U&U,, (0.30 2 0.04 at baseline to 0.36 5 0.04 at 4 hours; Fig 2) and uvurate (0.46 + 0.10 mg/min baseline to 0.59 + 0.04 mg/min at 4 hours) was not seen in the control subjects. In fact, in control subjects U,,/ Ucr never exceeded 1, and UUA/UCr and UVurate decreased significantly at 1 hour postexercise (Fig 2). Treatment with allopurinol prevented exercise-induced ARF in our patient (Fig l), prevented the UUA/Ucr ratio from exceeding 1 (0.25 to 0.17; Fig 2), and ameliorated the UVurat, peak after exercise (0.28 to 0.22 mg/min). In the control subjects, treatment with allopurinol had no effect on the responses of UUAAJCr (Fig 2) and UV”ra, to exercise. Literature
Review
The summary of the literature review is presented in Table 2; the data are self-explanatory. DISCUSSION
The true incidence of renal hypouricemia is unclear. Although several studies reported the incidence of hypouricemia of unknown etiology,58-60ranging from 0.16% to 0.18%, only Hisatome et al2 reported specifically the incidence of renal hypouricemia in an outpatient Japanese population (0.12%, or four of 3,258 patients). The incidence of renal hypouricemia in other pa-
AND
HASBARGEN
tient populations is not known, although the majority of case reports appear in patients of Japanese or non-Ashkenazi Jewish descent (Table 2). Uric acid excretion in humans is thought to occur in four steps.‘S57,61The four-component model proposes that uric acid is freely filtered at the glomerulus, nearly completely reabsorbed in the proximal tubule (presecretory reabsorption), subsequently secreted into the proximal tubule, and again reabsorbed (postsecretory reabsorption). Defective presecretory and/or postsecretory reabsorption as well as enhanced secretion can all result in renal hypouricemia. Pyrazinamide inhibits uric acid secretion, while probenecid blocks uric acid reabsorption, mainly at the postsecretory site. However, at lower doses, probenecid can also inhibit uric acid secretion. Since pyrazinamide decreased UV,,,/Cc, substantially (Table l), but not to normal, the mechanism of renal hypouricemia is most likely due to a failure to reabsorb filtered uric acid, although a concomitant postsecretory reabsorption defect or increased secretion cannot be completely excluded. With a presecretory reabsorption defect, probenecid administration will increase UVUrate/CCr. If there is a concomitant postsecretory reabsorption defect, UVu,,t&, should remain unchanged or increase slightly after probenecid administration. The paradoxic decreases in UVu,t&,, F,UA, and CUA in our patient suggest that probenecid is inhibiting secretion rather than presecretory or postsecretory reabsorption, either due to decreased delivery of probenecid into the tubule (through increased uric acid secretion at the expense of probenecid) or to a total/subtotal defect in reabsorption. In both these instances, probenecid has no effect on reabsorption, resulting in unopposed inhibition of uric acid secretion. Our patient’s response to pyrazinamide and probenecid most closely resembles that described by Akaoka et al6 (patients Y.A. and Y.K.), Akaoka et a13’, and Matsuda et a13’. Although a subtotal defect (in a total reabsorptive defect F,UA is >lOO%) in both presecretory and postsecretory reabsorption is the most likely mechanism in these patients, increased secretion of uric acid cannot be completely excluded. Reported complications arising as a result of renal hypouricemia are rare, consisting of case reports of decreased bone density associated with hypercalciuria and hypouricemia,4 uric acid
RENAL Table
HYPOURICEMIA
AND
2. Summary
EXERCISE-INDUCED
of Characteristics
of Patients and Literature
Families Review
with
Individuals
Characteristics No. Age, range Sex Male Female Unknown Ethnicity Japanese
941
ARF
54 W
3-66
Non-Ashkenazi Jew Other Not described Sun range (mg/dL) FEUA range (%) Tubular transport defect Presecretory reabsorption Increased secretion
Postsecretory reabsorption defect Combined reabsorption defect Total/subtotal transport defect Unknown Complications Acute renal failure Hypercalciuria Nephrolithiasis (uric acid) Nephrolithiasis (calcium oxalate) Nephrolithiasis (mixed) Nephrolithiasis (unknown type) Decreased bone density Hematuria (gross and microscopic) * Italian, 1; Turk, 1. T Iraqi, 1; Arab, 1; Gypsy,
Hypouricemia
as Described
(%)
Families
(27 persons (16 persons 0
28 (51.8)
11 (44)
18 (33.3) 6 (11.1)
(%)
or 62.8) or 37.2)
8 (32) 3 um 3 (12) 0.08-2.6 17-181.5 12 (48) 0
11 6 3 10
(20.4) (11.1) (5.6) (18.5)
3 4 3 3
6 8 6 9 2 3 0 3
(11.1) (14.8) (11.1) (16.7) (3.7) (5.6)
2 (8)
(5.6)
in a
25 (43 persons) 2-71
25 (46.3) 25 (46.3) 4 (7.4)
0 2 (3.7) 24 (44.4) 0.1-2.5 18.1-260 defect
Renal
(12) (16) (12) (12)
4 (16) 1 (4) 1 (4)
2 (8) 2 (8) 1 (4) 0
1.
nephrolithiasis,3~5-13 and calcium nephrolithiasis4,14-20 (Table 2). More recently, eight patients with renal hypouricemia were reported to have exercise-induced ARF21-26(Table 3). Erley et al*l described a man who presented with nausea, vomiting, loin pain, and oliguric ARF requiring transient dialysis. The UuA/UCr during ARF was greater than 1.O, and a renal biopsy demonstrated uric acid crystals in tubular lumina with mild to moderate interstitial inflammation. The investigators postulated uric acid nephropathy as the etiology of the ARF. There was no mention of exercise preceding the episode of ARF. Sakurauchi et a12’ presented a man with two episodes of loin pain, fatigue, hypertension, and ARF after a marathon. These investigators did not speculate on the etiology of the ARF. Ishikawa et a123subsequently described three patients with nausea,
vomiting, loin pain, and ARF after exercise. Renal biopsy 2 to 4 weeks later revealed either acute tubular necrosis or normal tissue in all three patients. Two biopsies were preceded by a contrastenhanced computed tomography scan showing patchy contrast uptake with wedge-shaped defects. The investigators suggested that ARF may be part of a spectrum of exercise-induced ischemit ARF in young, previously healthy individuals who have no evidence of myoglobinuria or uric acid nephropathy. Numabe et a124reported an episode of ARF (peak Scr of 8.7 mg/dL) in a man presenting with nausea, vomiting, loin pain, and abdominal pain after playing scuffle. Renal biopsy at 2 weeks revealed acute tubular necrosis. No further comment was offered concerning the etiology of the ARF. Igarashi et a125 described a boy with isolated renal hypouricemia
942
YEUN
Table
3. Summary
of Patients
With
Renal
Hypouricemia
Who
Developed
Exercise-Induced
AND
HASBARGEN
Acute
Renal
Renal Biopsy (no. of days after ARF)
SJA Age 641 Sex
Source Erley et al*’ Sakurauchi lshikawa
et al** et alp3
Ethnicity
(md W
FsUA w
Defect*
Exercise
0.1-0.3
128-260
3
-
1
Yes
NR
Yes
1
Yes
23/M
Turk
21/M
Japanese
0.7
79
17/M
Japanese
0.6
79.3
22/M
Japanese
0.7
52.8-60
Numabe
et alz4
16/M 17/M
Japanese Japanese
1.0 0.6
43.2 52-70
lgarashi
et alz5
12/M
Japanese
0.3
loo-136
46/M 29/M
Japanese Pakistani
0.9 0.5
50 55-69
Hiroshige Present
et alz6
1 1 or4
4 1 4 or2
Yes Yes
Yes Yes
Symptoms
Dialysis
Episodes
N/V, loin pain
Yes
1
Loin pain, malaise, edema Abdominal and loin pain, NN NN, malaise, abdominal and loin pain, fever NN NN, malaise, abdominal and loin pain N, anorexia, back and loin pain -
No
2
Uric acid nephropathy -
No
1
ATN (13)
No
1
ATN (35)
Yes Yes
1 1
NL (18) ATN (14)
No
1
-
No No
1 5
-
N, abdominal back pain
and
Abbreviations: NR, not reported; N, nausea; V, vomiting; ATN, acute tubular necrosis; NL, nomal. l Types of tubular defects in uric acid handling: 1, presecretory reabsorption defect; 2, increased secretion; defect; 4, presecretory and postsecretory reabsorption defect.
who developed ARF associated with nausea, anorexia, and loin pain after exercise. Of interest, this patient’s mother had a history of recurrent uric acid nephrolithiasis. The investigators proposed that exercise-induced ARF be included as a potential complication of renal hypouricemia, but were unable to comment on the pathogenesis. Hiroshige et alz6 described two patients with isolated renal hypouricemia; one had an episode of exercise-induced ARF 4 years ago. No details are available. Interestingly, two other patients had diabetes mellitus associated with renal hypouricemia and one presented with exercise-induced ARF. This patient was not included in this review because of the diabetes. We hypothesize that ARF occurs with exercise in patients with renal hypouricemia because of the increase in uric acid production during exercise. Several studies have documented an increase in SuA after exhaustive exercise62-66due to either decreased renal excretion or increased production.63 With exhaustive exercise, the resultant lactic acidosis can directly interfere with tubular secretion of urate.‘j3 Decreased glomerular filtration rate and a contracted extracellular volume’j3 can further decrease uric acid excretion. However, hyperuricemia also is a marker for cell energy crisis.67 During cellular energy depletion,
Failure
3, postsecretory
(1)
reabsorption
consumption of adenosine triphosphate (ATP) exceeds its synthesis, resulting in an accumulation of adenosine diphosphate (ADP) and adenosine monophosphate (AMP) and their subsequent degradation to inosine, xanthine, hypoxanthine, and, finally, uric acid. That the hyperuricemia seen during exhaustive exercise is due to overproduction of uric acid is supported by the observation that aerobic exercise does not result in hyperuricemia,64~66768whereas anaerobic exercise causes a sequential increase in first hypoxanthine,63 then uric acid levels. 63-66368 In addition, Fry et a169demonstrated that SuA remained elevated at 24 hours after exercise, while lactic acid levels and Scr had normalized by 2 hours, making decreased excretion an unlikely explanation for the persistent hyperuricemia. Finally, the combined studies of Sutton et ak7’ Sahlin et alyl and Hellsten-Westing et a172 demonstrate conclusively that hyperuricemia postexercise is the result of increased uric acid production. Sutton et a17’ demonstrated through muscle biopsies that intracellular ATP levels decreased after exhaustive exercise while ADP and AMP levels increased. Sahlin et a171showed a step-up in arterial to venous hypoxanthine levels after exhaustive exercise of a muscle group, suggesting increased release of hypoxanthine from the involved mus-
RENAL
HYPOURICEMIA
AND
EXERCISE-INDUCED
ARF
cles. Finally, Hellsten-Westing et al” demonstrated not only an arteriovenous increase in hypoxanthine levels in the involved muscle groups, but also an increased uptake of hypoxanthine and inosine by the liver with concomitant increased uric acid release. Taken together, these three studies confirm that during exhaustive exercise, muscles switch to anaerobic metabolism, and ADP and AMP accumulate and are converted to inosine and hypoxanthine, which are then released into the circulation, taken up by the liver, and converted to uric acid. All the uric acid is then promptly filtered and eliminated by the kidney, increasing the urinary uric acid load and, hence, UuA/Ucr and UVurat,. Volume depletion and/or decreased renal blood flow during exercise can further contribute to concentration of urinary uric acid. In addition, lactic acidosis during exercise may lead to increased urinary acidification, favoring uric acid crystallization. There are several theoretic ways of preventing the ARF if the above hypothesis is true. First, administration of allopurinol should decrease basal production of uric acid, ameliorate its increased production during exercise, decrease its subsequent elimination during exercise, and, therefore, ameliorate the ARF. Second, prophylactic alkalinization of the urine prior to exercising should prevent the ARF by increasing the solubility of uric acid. Third, prophylactic administration of pyrazinamide should decrease urinary uric acid and prevent ARF. We elected to test the hypothesis with the administration of allopurinol. The patient we describe here had recurrent exercise-induced ARF. Although a renal biopsy was not performed, there is indirect evidence implicating uric acid nephropathy in the pathogenesis of ARF. First, UuA/Ucr was greater than 1.O in our patient after exercise, associated with ARF. Kelton et a173noted that UuA/UCr greater than 1 .O accurately correlated with the presence of uric acid nephropathy. None of the controls had a Uu,/Uc, greater than 1.0, and none had ARF. Second, our patient had a dramatic increase in UV”rate after exercise, associated with ARF. In contrast, the controls had only a small increase in UVUrate. The observation of uric acid crystals in the urine after exercise and during episodes of ARF lend further support to this theory. Perhaps more importantly, the administration of allopurino1 was effective in preventing exercise-induced
943
ARF in our patient by preventing the increased uric acid excretion after exercise (Fig 2). In a study of patients with hematologic malignancies, Rieselbach et a174 concluded that uric acid excretion and urinary uric acid concentration are more important determinants than hyperuricemia for the development of uric acid nephropathy. Our data directly support this contention, since urinary indices (UuJUc, and UVurate) are elevated in the face of hypouricemia. Our hypothesis of uric acid nephropathy as the cause of exercise-induced ARF in patients with renal hypouricemia concur with the findings of Erley et al.‘l Although Ishikawa et a123and Numabe et al% did not find evidence for uric acid nephropathy in their kidney biopsy specimens, the renal tissue may have been obtained too late in the course of the renal failure. In addition, if the kidney tissue was fixed with formaldehyde, the uric acid crystals may have leached out of the tissue.75 The acute tubular necrosis observed in Ishikawa et al’s study23 also may have been a direct result of the administered contrast. Their observation of patchy contrast uptake by the renal cortex may have been a result of the administered contrast or residual changes from uric acid nephropathy rather than a cause of the renal failure. Our patient demonstrated no renal cortical perfusion defects on magnetic resonance imaging with gadolinium and renal scan performed within 48 hours of ARF in the absence of intravenous contrast administration. Although Loffler et al49concluded that patients with renal hypouricemia may not respond to allopurinol administration because of increased excretion of the active metabolite oxypurinol, this does not clinically appear to be the case. Frank et al’ and Sasaki et al” treated three patients with uric acid nephrolithiasis and renal hypouricemia with allopurinol and achieved stone dissolution as well as prevented further episodes of stone formation. In the present study, our patient clinically responded to allopurinol with prevention of an increase in UuA/UCr and ARF. In conclusion, although renal hypouricemia is a rare condition, it can be associated with significant morbidity to include uric acid nephrolithiasis and exercise-induced ARF. We propose that the ARF is a result of uric acid nephropathy and can be prevented with the administration of allopurinol.
944
YEUN
ACKNOWLEDGMENT The authors thank Frances Matsumoto for her expertise in translating papers from the Japanese literature.
REFERENCES 1. Sperling 0: Renal hypouricemia: Classification, tubular defect and clinical consequences. Co&b Nephrol lOO:l-14, 1992 2. Hisatome I, Ogino K, Kotake H, Ishiko R, Saito M, Hasegawa J, Mashiba H, Nakamoto S: Cause of persistent hypouricemia in outpatients. Nephron 51:13-16, 1989 3. Kotake T, Miura N, Ito H: Renal tubular hypouricemia and calcium urolithiasis. Scanning Microsc 7:417-421, 1993 4. Sperling 0, Weinberger A, Oliver I, Liberman UA, De Vries A: Hypouricemia, hypercalciuria, and decreased bone density: A hereditary syndrome. Ann Intern Med 80:482-487, 1974 5. Kawabe K, Murayama T, Akaoka I: A case of uric acid renal stone with hypouricemia caused by tubular reabsorptive defect of uric acid. J Urol 116:690-692, 1976 6. Akaoka I, Nishizawa T, Yano E, Kamatani N, Nishida Y, Sasaki S: Renal urate excretion in five cases of hypouricemia with an isolated renal defect of urate transport. J Rheumatol 4:86-94, 1977 7. Frank M, Many M, Sperling 0: Familial renal hypouricemia: Two additional cases with uric acid lithiasis. Br J Urol 5188-91, 1979 8. Hedley JM, Phillips PJ: Familial hypouricaemia associated with renal tubular uricosuria and uric acid calculi: Case report. J Clin ,Pathol 33:971-972, 1980 9. Smetana SS, Bar-Khayim Y: Hypouricemia due to renal tubular defect: A study with the probenecid-pyrazinamide test. Arch Intern Med 145:1200-1203, 1985 10. Sasaki M, Takenawa J, Kanamaru H: A case of idiopathic hypouricemia due to augmented renal tubular secretion of uric acid. Nippon Hinyokika Gakkai Zasshi 77: 1349-1352, 1986 11. Gofrit 0, Verstandig AG, Pode D: Bilateral obstructing ureteral uric acid stones in an infant with hereditary renal hypouricemia. J Urol 149:1506-1507, 1993 12. Hisatome I, Tanaka Y, Kotake H, Kosaka H, Hirata N, Fujimoto Y, Yoshida A, Shigemasa C, Mashiba H, Sato R, Takeda A: Renal hypouricemia due to enhanced tubular secretion of urate associated with urolithiasis: Successful treatment of urolithiasis by alkabnization of urine K+, Na+citrate. Nephron 65:578-582, 1993 13. Kaneko K, Fujimori S, Itoh H, Nakayama Y, Oyama H, Kanbayashi T, Miyashita H, Akaoka I: Renal handling of hypoxanthine and xanthine in normal subjects and in four cases of idiopathic renal hypouricemia. J Rheumatol 15:325330, 1988 14. Greene ML, Marcus R, Aurbach GD, Kazam ES, Seegmiller JE: Hypouricemia due to isolated renal tubular defect: Dalmatian dog mutation in man. Am J Med 53:361367, 1972 15. Benjamin D, Sperling 0, Weinberger A, Pinkhas J, de Vries A: Familial hypouricemia due to isolated renal tubular defect: Attenuated response of uric acid clearance to probenecid and pyrazinamide. Nephron 18:220-225, 1977 16. Barrientos A, Perez-Diaz V, Diaz-Gonzalez R, Rodi-
AND
HASBARGEN
cio JL: Hypouricemia by defect in the tubular reabsorption. Arch Intern Med 139:787-789, 1979 17. Tofuku Y, Kuroda M, Takeda R: Hypouricemia due to renal urate wasting: Two types of tubular transport defect. Nephron 30:39-44, 1982 18. Sanz AM, Alonzo-Vega GG, Anton FM, Puig JG: Hypouricemia and renal tubular urate secretion. Arch Intern Med 143:1633-1634, 1983 19. Gaspar GA, Puig JG, Mateos FA, Oria CR, Gomez ME, Gil AA: Hypouricemia due to renal urate wasting: Different types of tubular transport defects. Adv Exp Med Biol 195A:357-363, 1986 20. DeFerrari ME, Colussi G, Benazzi E, Rombola G, Surian M, Malberti F, Brenna S, Minetti L: Calcium nephrolithiasis and renal tubular hypouricemia. Contrib Nephml 58:41-43, 1987 21. Erley CMM, Hirschberg RR, Hoefer W, Schaefer K: Acute renal failure due to uric acid nephropathy in a patient with renal hypouricemia. Klin Wochenschr 67:308-312,1989 22. Sakurauchi Y, Tsuyuki M, Okazaki Y, Sugiyama B, Yamamoto T: Acute renal failure in a patient with renal hypouricemia. Nippon J Gakkai Shi 3 1:1326, 1989 (abstr) 23. Ishikawa I, Sakurai Y, Masuzaki S, Sugishita N, Shinoda A, Shiknra N: Exercise-induced acute renal failure in 3 patients with renal hypouricemia. Nippon J Gakkai Shi 32923-928, 1990 24. Numabe A, Tsukada H, Sugimoto T, Ono H, Hirao S, Abe M, Yagi S: A case of acute renal failure in a patient with idiopathic hypouricemia. Nippon Jinzo Gakkai Shi 34:841-845, 1992 25. Igarashi T, Sekine T, Sugimura H, Hayakawa H, Arayama T: Acute renal failure after exercise in a child with renal hypouricaemia. Pediatr Nephrol 7:292-293, 1993 26. Hiroshige K, Yuu K, Takasugi M, Soejima M, Kuroiwa A: A study on uric acid excretion in patients with hypouricemia. Nippon Jinzo Gakkai Shi 35:829-834, 1993 27. Praetorius E, Kirk JE: Hypouricemia: With evidence for tubular elimination of uric acid. J Lab Clin Med 35:865868, 1950 28. Khachadurian AK, Arslanian MJ: Hypouricemia due to renal uricosuria: A case study. Ann Intern Med 78:547550, 1973 29. Simkin PA, Skeith MD, Healey LA: Suppression of uric acid secretion in a patient with renal hypomicemia. Isr J Med Sci 9: 1113, 1973 (abstr) 30. Healey LA, Skeith MD, Simkin PA: Hypouricemia: An incidental finding indicating xanthinuria or defective reabsorption of uric acid. Arch Intern Med 134:46-47, 1974 3 1. Akaoka I, Nishizawa T, Yano E, Takeuchi A, Nishida Y, Yoshimura T, Horiuchi Y: Familial hyponricemia due to renal tubular defect of mate transport. Ann Clin Res 7:318324, 1975 32. Benjamin D, Sperling 0, Weinberger A, Pinkhas J: Familial hypouricemia due to isolated renal tubular abnormality. Biomedicine 29:54-56, 1978 33. Fujiwara Y, Takamitsu Y, Ueda N, Orita Y, Abe H: Hypouricemia due to an isolated defect in renal tubular urate reabsorption. Clin Nephrol 13:44-48, 1980 34. Sorensen LB, Levinson DJ: Isolated defect in postsecretory reabsorption of uric acid. Ann Rheum Dis 39:180183, 1980
RENAL
HYPOURICEMIA
AND
EXERCISE-INDUCED
ARF
35. Weitz R, Sperling 0: Hereditary renal hypouricemia. Isolated tubular defect of mate reabsorption .I Pediatr 96:850853, 1980 36. Garty BZ, Nitzan M, Sperling 0: Inborn hypouricemia due to isolated defect in renal tubular uric acid transport. Isr J Med Sci 17:295-297, 1981 37. Suzuki T, Kidoguchi K, Hayashi A: Genetic heterogeneity of familial hypouricemia due to isolated renal tubular defect. Jpn J Hum Genet 26:243-248, 1981 38. Matsuda 0, Shiigai T, Ito Y, Aonuma K, Takeuchi J: A case of familial renal hypouricemia associated with increased secretion of para-aminohippurate and idiopathic edema. Nephron 30:178-186, 1982 39. Shichiri M, Matsuda 0, Shiigai T, Takeuchi J, Kanayama M: Hypouricemia due to an increment in renal tubular urate secretion. Arch Intern Med 142:1855-1857, 1982 40. Dumont I, Decaux G: Hypouricemia related to a hypersecretional tubulopathy. Nephron 34:256-259, 1983 41. Vinay P, Gattereau A, Moulin B, Gougoux A, Lemieux G: Normal urate transport into erythrocytes in familial renal hypouricemia and in the Dalmatian dog. Can Med Assoc J 128:545-549, 1983 42. Takeda E, Kuroda Y, Ito M, Toshima K, Watanabe T, Ito M, Naito E, Yokota I, Hwang TJ, Miyao M: Hereditary renal hypouricemia in children. J Pediatr 107:71-74, 1985 43. Colussi G, Rombola G, deFerrari ME, Roland0 P, Surian M, Malberti F, Minetti L: Pharmacological evaluation of urate renal handling in humans: Pyrazinamide test vs combined pyrazinamide and probenecid administration. Nephrol Dial Transplant 2:10-16, 1987 44. Nakajima H, Gomi M, Iida S, Kono N, Moriwaki K, Tarui S: Familial renal hypouricemia with intact reabsorption of uric acid. Nephron 45:40-42, 1987 45. Shichiri M, Iwamoto H, Maeda M, Kanayama M, Shiigai T: Hypouricemia due to subtotal defect in the urate transport. Clin Nephrol 28:300-303, 1987 46. Shichiri M, Iwamoto H, Shiigai T: Hypomicemia due to increased tubular urate secretion. Nephron 45:3 l-34, 1987 47. Hisatome I, Ogino K, Saito M, Miyamoto J, Hasegawa J, Kotake H, Mashiba H, Nakamoto S: Renal hypouricemia due to an isolated renal defect of urate transport. Nephron 49:81-83, 1988 48. Gafter U, Zuta A, Frydman M, Lewinski UH, Levi J: Hypouricemia due to familial isolated renal tubular uricosuria. Miner Electrolyte Metab 15:309-314, 1989 49. Loffler W, Seibke W, Seibke E, Reiter S, Jahn M, Hehlmann R, Zollner N: Non-responsiveness to allopurinol in renal hypouricaemia. Klin Wochenschr 67:47, 1989 50. Shichiri M, Itoh H, Iwamoto H, Hirata Y, Marumo F: Renal tubular hypouricemia: Evidence for defect of both secretion and reabsorption. Nephron 56:421-426, 1990 5 1. Kawachi M, Kono N, Kiyokawa H, Mineo I, Nakajima H, Shimizu T, Yorifuji S, Kuwajima M, Tami S: Decreased renal clearance of xanthine and hypoxanthine in a patient with renal hypouricemia: An new defect in renal handling of purines. Nephron 61:428-431, 1992 52. Barajas de Frutos D, Bravo Mancheno B, Palomino Urda N, Pedrero Vera J: Familial hypouricaemia due to an isolated tubular defect of mate reabsorption. Pediatr Nephrol 7:83-85, 1993 53. Hisatome I, Kato T, Miyakoda H, Takami T, Abe T,
945 Tanaka Y, Kosaka H, Ogino K, Mitani Y, Yoshida A, Kotake H, Shigemasa C, Mashiba H, Sato R, Takeda A: Renal hypouricemia with both drug-insensitive secretion and defective reabsorption of urate: A novel type of renal hypouricemia. Nephron 64:447-45 1, 1993 54. Uribarri J, Oh MS: Renal hypouricemia and absorptive hypercalciuria: A real syndrome. Nephron 63:172-175, 1993 55. Steele TH, Rieselbach RE: The renal mechanism for urate homeostasis in normal man. Am J Med 43:868-875, 1967 56. Kageyama N: A direct calorimetric determination of uric acid in serum and urine with uricase-catalysts system. Clin Chem Acta 31:421-426, 1971 57. Diamond HS: Interpretation of pharmacologic manipulation of urate transport in man. Nephron 5 1: l-5, 1989 58. Ramsdell CM, Kelley WN: The clinical significance of hypouricemia. Ann Intern Med 78:239-242, 1973 59. Van Peenen HJ: Causes of hypouricemia. Ann Intern Med 78:977-978, 1973 60. Yanase M, Nakahama H, Mikami H, Fukuhara Y, Orita Y, Yoshikawa H: Prevalence of hypouricemia in apparently normal population. Nephron 48:80, 1988 61. Puig JG, Anton FM, Sanz AM, Gaspar G, Lesmes A, Ramos T, Vazquez JO: Renal handling of uric acid in normal subjects by means of the pyrazinamide and probenecid tests. Nephron 35:183-186, 1983 62. Schrier RW, Hano J, Keller HI, Finkel RM, Gilliland PF, Cirksena WJ, Teschan PE: Renal, metabolic, and circulatory responses to heat and exercise. Ann Intern Med 73:213223, 1970 63. Knochel JP, Dotin LN, Hamburger RJ: Heat stress, exercise, and muscle injury: Effects on urate metabolism and renal function. Ann Intern Med 81:321-328, 1974 64. Green HJ, Fraser IG: Differential effects of exercise intensity on serum uric acid concentration. Med Sci Sports Exert 20:55-59, 1988 65. Hellsten-Westing Y, Sollevi A, Sjodin B: Plasma accumulation of hypoxanthine, uric acid and creatine kinase following exhausting runs of differing durations in man. Eur J Appl Physiol 62:380-384, 1991 66. Balsom PD, Seger JY, Sjodin B, Ekblom B: Physiological responses to maximal intensity intermittent exercise. Eur J Appl Physiol 65:144-149, 1992 67. Fox IH, Palella TD, Kelley WN: Hypermicemia: A marker for cell energy crisis. N Engl J Med 3 17: 11 l-l 12, 1987 68. Yamanaka H, Kawagoe Y, Taniguchi A, Kaneko N, Kimata S, Hosoda S, Kamatani N, Kashiwazaki S: Accelerated purine nucleotide degradation by anaerobic but not by aerobic ergometer muscle exercise. Metabolism 41:364-369, 1992 69. Fry RW, Morton AR, Garcia-Webb P, Keast D: Monitoring exercise stress by changes in metabolic and hormonal responses over a 24-h period. Eur J Appl Physiol 63:228234, 1991 70. Sutton JR, Toews CJ, Ward GR, Fox IH: Purine metabolism during strenuous muscular exercise in man. Metabolism 29:254-260, 1980 71. Sahlin K, Ekberg K, Cizinsky S: Changes in plasma hypoxanthine and free radical markers during exercise in man. Acta Physiol Stand 142:275-281, 1991
946 72. Hellsten-Westing Y, Kaijser L, Ekblorn B, Sjodin B: Exchange of purines in human liver and skeletal muscle with short-term exhaustive exercise. Am J Physiol266:R81-86, 1994 73. Kelton J, Kelley WN, Holmes EW: A rapid method for the diagnosis of acute uric acid nephropathy. Arch Intern Med 138:612-615, 1978
YEUN
AND
HASBARGEN
74. Rieselbach RE, Bentzel CJ, Cotlove E, Frei E, Freireich EJ: Uric acid excretion and renal function in the acute hyperuricemia of leukemia: Pathogenesis and therapy of uric acid nephropathy. Am J Med 37:872-884, 1964 75. Conger JD: Acute uric acid nephropathy. Med Clin North Am 74:859-871, 1990
MD
0 Isolated renal hypouricemia from defective uric acid reabsorption and/or secretion is a well-described entity, with a prevalence of 0.12% to 0.20% in Japan. It is rarely associated with exercise-induced acute renal failure (ARF). The etiology of ARF is debated. Prevention of ARF in renal hypouricemia has not been previously addressed. A 29-year-old Pakistani man had recurrent exercise-induced ARF. He was found to have isolated renal hypouricemia: serum uric acid 0.5 mg/dL, 24-hour urine uric acid 472 t- 25 mg (-t-SD), and fractional excretion of uric acid 55.2% to 69.4%. Both pyrazinamide and probenecid decreased fractional excretion of uric acid and uric acid in our patient, suggesting either a partial presecretory and postsecretory reabsorption excretion rate (UV,,d defect or increased secretion. We investigated renal uric acid excretion during exercise in our patient and four control subjects. All five subjects underwent a physical fitness test (PFI). Our patient developed ARF. Uric acid excretion rate increased in our patient, from 0.46 mg/min at baseline to 1.49 mg/min 4 hours after the PFT, as did the urine uric acid to urine creatinine ratio (U&J,J (0.29 to 1.49). In the controls, UVurate and Uua/lJcr were unchanged after the PFR UVurate was 0.46 2 0.10 mg/min at baseline and 0.59 -f 0.04 mg/min 4 hours after the PFT, while UuA/UCr was 0.30 lr 0.04 at baseline and 0.36 2 0.04 at 4 hours. All five subjects took allopurinol 300 mg daily for 5 days and repeated the PFT. In our patient, allopurinol prevented the ARF as well as the exerciseinduced increases in UVumte (0.28 mg/min to 0.22 mg/min) and Uun/lJcr (0.25 to 0.17). In the controls, the UVurat. and Uun/Ucr responses to exercise were not altered. We conclude that increased renal excretion of uric acid during exercise was responsible for the ARF in our patient with renal hypouricemia and that successful prophylaxis with allopurinol is possible. This is a US government work. There are no restrictions on its use. INDEX
WORDS:
Renal
hypouricemia;
exercise;
acute
R
ENAL HYPOURICEMIA results from an isolated renal tubular defect in reabsorption and/or secretion of uric acid that is genetically determined in an autosomal recessive inheritance pattern.’ It is a rare condition with a reported incidence of 0.12% to 0.20% in Japan.233There are many cases of renal hypouricemia reported in the literature.3-54 However, until 1989, the only adverse effects of renal hypouricemia were thought to be decreased bone density,4 uric acid nephrolithiasis,3*5-13 and possibly calcium nephrolithiasis,4,‘4-20 as documented in case reports. Since then, eight cases of exercise-induced acute renal failure (ARF) have been reported in patients with renal hypouricemia.2’~26 However, only one of these eight patients had recurrent ARFz2 (two episodes). The prevention of exercise-induced ARF has not been addressed. We report an individual with renal hypouricemia who developed recurrent ARF after exercise on at least three occasions. Because of his desire to remain active, we explored potential methods of preventing the ARF. We performed a review of the literature on isolated renal hypouricemia and provide a summary of our results. CASE An otherwise to the emergency American
Journal
REPORT
healthy 29-year-old Pakistani man presented department on March 3, 1993, with nausea, of Kidney
Diseases,
renal
failure;
hypouricemia;
allopurinol;
prophylaxis.
vomiting, and abdominal pain 4 hours after a semiannual physical fitness test (PFT). The PFf consisted of a 2-mile run, sit-ups, and push-ups. He denied any illness, viral prodrome, or nonsteroidal anti-inflammatory drug ingestion prior to exercising. He had been training 3 days a week for the PFT, although at lesser levels of exertion. Of interest, our patient had two prior episodes of similar symptoms occurring shortly after the PFf that were associated with non-oliguric AW. The first episode occurred elsewhere in May 1992; no further evaluation was performed during that admission. The second episode occurred in Denver, CO, in October 1992, with serum creatinine (Sc,) peaking at 4.0 mg/dL. Past medical history was otherwise unremarkable. There is no family history of muscle disorders. However, the patient’s father had end-stage renal disease from nephrolithiasis of unknown composition; a brother has a history of calcium
From the Department of Medicine, Nephrology Service, Fitzsimons Army Medical Center, Aurora, CO; and Indiana University and Veterans Administration Medical Center, Indianapolis, IN. Received September 8, 1994; accepted in revisedform January 20, 1995. The opinions and research contained herein are theprivate ones of the authors and are not to be considered as ofjcial or rejlecting the views of the Department of the Army or the Department of Defense. Address reprint requests to Jane Y. Yeun, MD, Nephrology Service, MCHG-MD& Fitzsimons Army Medical Center, Aurora, CO 80045. This is a US government work. There are no restrictions on its use. 0272-6386/95/2506-0018$0.00/O
Vol 25, No 6 (June), 1995: pp 937-946
937
YEUN
oxalate stones. We were unable to obtain serum uric acid (St,*) levels in any of the relatives. On physical examination, the blood pressure was 132/74 mm Hg without orthostasis and the pulse was 80 beats/min. Examination was entirely unremarkable except for mild abdominal tenderness to palpation, poorly localized, without rebound tenderness. There was no muscle swelling or tenderness. Laboratory evaluation revealed a sodium of 138 mmol/L, potassium 4.1 mmol/L, chloride 108 mmol/L, bicarbonate 18 mmol/L, urea nitrogen 30 mg/dL, creatinine 4.7 mg/dL, calcium 8.8 mg/dL, phosphate 3.6 mg/dL, uric acid 2.1 mg/ dL, creatine kinase 107 U/L, and fractional excretion of sodium 3.3%. Urinalysis revealed a specific gravity of 1.004, 2+ blood, no glucose, pH 6.0, 2 to 4 white blood cells/highpowered field, 0 to 2 red blood cells/high-powered field, rare renal tubular epithelial cells, and rare uric acid crystals. Renal ultrasound was unremarkable, demonstrating normal-sized kidneys without hydronephrosis. The nausea, vomiting, and abdominal pain resolved spontaneously in 24 hours. With conservative therapy, the nonoliguric ARF improved and S, was 1.9 mg/dL at discharge (8 days after initial presentation). During follow-up on April 12, 1993, Scr was 1.1 mg/dL, accompanied by a SuA of 0.5 mgl dL and serum bicarbonate of 26 mmol/L. Subsequent 24hour urine collections revealed 472 ? 25 mg of uric acid (n = 3), uric acid clearance (Cu,) of 57.4 to 65.8 mL/min, fractional excretion of uric acid (F&A) of 55.2% to 69.4%, and normal phosphate (8 14 mg) and calcium (70 to 110 mg; normal range, 42 to 353 mg) excretion. There was no glycosuria or abnormal amino acid excretion. Our patient underwent repeat exercise testing to assess reproducibility of ARF. During the first exercise testing, ARF was reproduced with Seepeaking at 2.5 mg/dL on day 2 after PFT. Magnetic resonance imaging with gadolinium contrast was performed less than 24 hours after the PFT, while a dimercaptosuccinic acid (DMSA) renal scan was done within 48 hours of the PFT to assessrenal cortical perfusion. Subsequent exercise tests were performed to assess the effect of exercise on renal function and uric acid excretion. Four normal male volunteers underwent concomitant exercise testing and served as controls. Informed consent was obtained from all subjects. MATERIALS
AND
Uric acid excretion rate (UVurate) , FaUA, and creatinine clearance (C,) were measured at baseline and after pyrazinamide 3.0 g orally, following the modified method of Steele and Rieselbach.55 After establishing free water diuresis, 30minutes urine collections were obtained, two at baseline and three starting 1 hour after pyrazinamide administration. The effect of probenecid 2.0 g orally on UVurater F&A, and Cc, were measured in an identical fashion 4 days later.
ESfect of Exercise on Renal Function Timed urine collections and blood were obtained at baseline for measurement of Ccr, F&A, S*, U,,/&, and UV,, in our patient and four healthy volunteers from 21 to 41 years
HASBARGEN
of age. Each subject then underwent a standardized PFT, consisting of push-ups and sit-ups to exhaustion over 2 minutes each, and a 2-mile run. Timed urine collections and blood were again obtained at 1 hour, 4 hours, and 24 hours after exercise to allow calculation of the same parameters. All urine samples were spontaneously voided. All subjects ate and drank ad libitum. After each subject had taken allopurinol 300 mg daily for 5 days, the above studies were repeated.
Assays Uric acid was measured using the uricase method,56 with reported accuracy down to 0.2 mg/dL. Creatinine measurements were performed using the Kodak Ektachem system (Rochester, NY).
Literature Review A review of the literature on isolated renal hypouricemia3-54 was performed through use of a MEDLINE search and perusal of bibliographic citations. Any patients who had another potential etiology for uricosuria and resultant hypouricemia (eg, diabetes mellitus,26,39renal tubular damage from renal tuberculosisi or interstitial nephritisI and nephrotic syndrome33) were excluded from this review. The articles were reviewed for the number of individuals or families with isolated renal hypouricemia, gender, age, ethnicity, S“AI F&A, the type of tubular transport defect, and any complications arising directly or indirectly from the renal hypouricemia. Any individual reported as having a similarly affected family member was included in the family category. Turkish Jews, Iraqi Jews, and Libyan Jews were included under the non-Ashkenazi Jew ethnic group. The investigators’ classification of the tubular transport defect after pyrazinamide, probenecid, and/or benzbromarone testing was assumed to be correct. When a classification was not attempted, Sperling’s’ criteria for the classification of type of defect was applied to the data. Complications from renal hypouricemia were summarized as the number of individuals with the complication when there was no family history of renal hypouricemia and as the number of families with the complication when there was a family history of renal hypouricemia, even if only one member of the family was described in sufficient detail.
METHODS
Tubular Function
AND
RESULTS
Tubular Function Administration of pyrazinamide decreased CuA (421 + 38 mL/min to 113 t- 4 mLknin), F&A (360% -+ 24% to 112% + l%), and UVu,,JCc, (3.59 ? 0.23 yg/rnL to 1.12 + 0.01 pg/mL) (Table 1). Pyrazinamide is thought to inhibit secretion of uric acid in the proximal tubule. In our patient, pyrazinamide decreased the excretion of uric acid nearly fourfold. Although probenecid at lower doses can inhibit secretion of uric acid, at the doses used here, it inhibits predominantly postsecretory re-
RENAL
HYPOURICEMIA Table
1. Effect
AND
EXERCISE-INDUCED
of Pyrazinamide
and
939
ARF
Probenecid
on Renal
Tubular
Handling
Pyrazinamide
Time (min)
%A (mg/dL)
C (ml/&)
C (ml.IGin)
of Uric
Acid
in Our
Patient
Probenecid wra&c, WmL)
FEUA (%)
-60 to -30 -30 to 0 Mean 2 SE
0.1 0.1 0.1
459 383 421 238
120 383 114 336 117+-3 360+-24 3 g orally
3.82 3.36 3.59-t0.23
T=O +60 to +90 +90 to +120 +I20 to +150 Mean + SE
0.1 0.1 0.1 0.1
105 115 120 113 i 4
92 104 106 101 ? 4
1.14 1.10 1.12 1.12 e 0.01
114 111 112 112 ?z 1
absorption of uric acid and, to a lesser extent, presecretory reabsorption.‘y57 Therefore, probenecid administration should increase uric acid excretion if reabsorptive function is intact and should have no effect on uric acid excretion if reabsorptive function is defective. In our patient, probenecid was observed to decrease urinary uric acid excretion (Table 1) by nearly half of all calculated parameters. The baseline values for CuA and F&A in the pyrazinamide test are markedly disparate from those in the probenecid test (Table 1) because of the wide variations in measuring our patient’s SuA (0.1 to 0.6 mg/dL) at the lower end of resolution of the assay. However, since UVu,,/Cc, does not include SuA, these data are directly comparable at baseline between the two tests. Renal Cortical Per@sion During Acute Renal Failure
S (mg:L)
C”, (mUmin)
C cr (mUmin)
0.6 0.5 0.55 t 0.05
82.8 91.6 87.2 f 4.4
120 111 116 t 4 2 g orally
69.2 82.2 75.7 i 6.5
4.14 4.13 4.14
0.5 0.5 0.5 0.5
61.2 55.6 51.7 56.2 -c 2.8
102 104 110 105 ? 2
60.3 53.5 47.1 53.6 I 3.8
3.00 2.67 2.35 2.67 ? 0.19
FJJA (%)
wJra&cr WmL)
PFI after allopurinol(75% to 74%, 93% to 94%, 92% to 95%) except for one subject, whose performance improved during the second PIT (59% to 73%). Effect of Exercise on Renal Function
Acute renal failure was reproduced in our patient during PIT, with Ccr decreasing from 151 to 77 mL/min by 4 hours and 46 mL/min by 24 hours (Fig 1). The control subjects retained normal renal function with exercise (138 +- 14 mL/min baseline to 141 + 12 r&/mm at 4 hours and 135 2 22 mL/min at 24 hours; Fig 1). Interestingly, UuA/UCr ratio was markedly elevated in our patient at 4 hours after exercise (0.29 at baseline to 1.49 at 4 hours; Fig 2), associated with a UVUratethat increased from 0.48 mg/min at baseline to 1.49 mg/min at 4 hours (data not shown
Magnetic resonance imaging with gadolinium contrast performed less than 24 hours after an episode of exercise-induced ARF revealed no cortical perfusion defects. A DMSA renal scan performed within 48 hours also revealed no perfusion defects.
1
Extent of Exercise Petiormed
There are age-specific standards set for the PIT, with 100% being a perfect score for the particular age group and 60% a passing score. Compared with other individuals in his age group, our patient performed at 62% for his baseline PFI and 65% for the PFT after allopurinol ingestion. The control subjects’ performances were comparable from the baseline PPT to the
Fig 1. Effect of exercise on Ccr in control subjects and patient with renal hypouricemia at baseline and after allopurinol.
YEUN
Fig 2. Effect of exercise jects and patient with renal and after allopurinol.
on Uun/Ucr hypouricemia
in control subat baseline
in graphic form since the graph is almost identical in appearance to that for UUA/UCrr shown in Fig 2). Such an increase in U&U,, (0.30 2 0.04 at baseline to 0.36 5 0.04 at 4 hours; Fig 2) and uvurate (0.46 + 0.10 mg/min baseline to 0.59 + 0.04 mg/min at 4 hours) was not seen in the control subjects. In fact, in control subjects U,,/ Ucr never exceeded 1, and UUA/UCr and UVurate decreased significantly at 1 hour postexercise (Fig 2). Treatment with allopurinol prevented exercise-induced ARF in our patient (Fig l), prevented the UUA/Ucr ratio from exceeding 1 (0.25 to 0.17; Fig 2), and ameliorated the UVurat, peak after exercise (0.28 to 0.22 mg/min). In the control subjects, treatment with allopurinol had no effect on the responses of UUAAJCr (Fig 2) and UV”ra, to exercise. Literature
Review
The summary of the literature review is presented in Table 2; the data are self-explanatory. DISCUSSION
The true incidence of renal hypouricemia is unclear. Although several studies reported the incidence of hypouricemia of unknown etiology,58-60ranging from 0.16% to 0.18%, only Hisatome et al2 reported specifically the incidence of renal hypouricemia in an outpatient Japanese population (0.12%, or four of 3,258 patients). The incidence of renal hypouricemia in other pa-
AND
HASBARGEN
tient populations is not known, although the majority of case reports appear in patients of Japanese or non-Ashkenazi Jewish descent (Table 2). Uric acid excretion in humans is thought to occur in four steps.‘S57,61The four-component model proposes that uric acid is freely filtered at the glomerulus, nearly completely reabsorbed in the proximal tubule (presecretory reabsorption), subsequently secreted into the proximal tubule, and again reabsorbed (postsecretory reabsorption). Defective presecretory and/or postsecretory reabsorption as well as enhanced secretion can all result in renal hypouricemia. Pyrazinamide inhibits uric acid secretion, while probenecid blocks uric acid reabsorption, mainly at the postsecretory site. However, at lower doses, probenecid can also inhibit uric acid secretion. Since pyrazinamide decreased UV,,,/Cc, substantially (Table l), but not to normal, the mechanism of renal hypouricemia is most likely due to a failure to reabsorb filtered uric acid, although a concomitant postsecretory reabsorption defect or increased secretion cannot be completely excluded. With a presecretory reabsorption defect, probenecid administration will increase UVUrate/CCr. If there is a concomitant postsecretory reabsorption defect, UVu,,t&, should remain unchanged or increase slightly after probenecid administration. The paradoxic decreases in UVu,t&,, F,UA, and CUA in our patient suggest that probenecid is inhibiting secretion rather than presecretory or postsecretory reabsorption, either due to decreased delivery of probenecid into the tubule (through increased uric acid secretion at the expense of probenecid) or to a total/subtotal defect in reabsorption. In both these instances, probenecid has no effect on reabsorption, resulting in unopposed inhibition of uric acid secretion. Our patient’s response to pyrazinamide and probenecid most closely resembles that described by Akaoka et al6 (patients Y.A. and Y.K.), Akaoka et a13’, and Matsuda et a13’. Although a subtotal defect (in a total reabsorptive defect F,UA is >lOO%) in both presecretory and postsecretory reabsorption is the most likely mechanism in these patients, increased secretion of uric acid cannot be completely excluded. Reported complications arising as a result of renal hypouricemia are rare, consisting of case reports of decreased bone density associated with hypercalciuria and hypouricemia,4 uric acid
RENAL Table
HYPOURICEMIA
AND
2. Summary
EXERCISE-INDUCED
of Characteristics
of Patients and Literature
Families Review
with
Individuals
Characteristics No. Age, range Sex Male Female Unknown Ethnicity Japanese
941
ARF
54 W
3-66
Non-Ashkenazi Jew Other Not described Sun range (mg/dL) FEUA range (%) Tubular transport defect Presecretory reabsorption Increased secretion
Postsecretory reabsorption defect Combined reabsorption defect Total/subtotal transport defect Unknown Complications Acute renal failure Hypercalciuria Nephrolithiasis (uric acid) Nephrolithiasis (calcium oxalate) Nephrolithiasis (mixed) Nephrolithiasis (unknown type) Decreased bone density Hematuria (gross and microscopic) * Italian, 1; Turk, 1. T Iraqi, 1; Arab, 1; Gypsy,
Hypouricemia
as Described
(%)
Families
(27 persons (16 persons 0
28 (51.8)
11 (44)
18 (33.3) 6 (11.1)
(%)
or 62.8) or 37.2)
8 (32) 3 um 3 (12) 0.08-2.6 17-181.5 12 (48) 0
11 6 3 10
(20.4) (11.1) (5.6) (18.5)
3 4 3 3
6 8 6 9 2 3 0 3
(11.1) (14.8) (11.1) (16.7) (3.7) (5.6)
2 (8)
(5.6)
in a
25 (43 persons) 2-71
25 (46.3) 25 (46.3) 4 (7.4)
0 2 (3.7) 24 (44.4) 0.1-2.5 18.1-260 defect
Renal
(12) (16) (12) (12)
4 (16) 1 (4) 1 (4)
2 (8) 2 (8) 1 (4) 0
1.
nephrolithiasis,3~5-13 and calcium nephrolithiasis4,14-20 (Table 2). More recently, eight patients with renal hypouricemia were reported to have exercise-induced ARF21-26(Table 3). Erley et al*l described a man who presented with nausea, vomiting, loin pain, and oliguric ARF requiring transient dialysis. The UuA/UCr during ARF was greater than 1.O, and a renal biopsy demonstrated uric acid crystals in tubular lumina with mild to moderate interstitial inflammation. The investigators postulated uric acid nephropathy as the etiology of the ARF. There was no mention of exercise preceding the episode of ARF. Sakurauchi et a12’ presented a man with two episodes of loin pain, fatigue, hypertension, and ARF after a marathon. These investigators did not speculate on the etiology of the ARF. Ishikawa et a123subsequently described three patients with nausea,
vomiting, loin pain, and ARF after exercise. Renal biopsy 2 to 4 weeks later revealed either acute tubular necrosis or normal tissue in all three patients. Two biopsies were preceded by a contrastenhanced computed tomography scan showing patchy contrast uptake with wedge-shaped defects. The investigators suggested that ARF may be part of a spectrum of exercise-induced ischemit ARF in young, previously healthy individuals who have no evidence of myoglobinuria or uric acid nephropathy. Numabe et a124reported an episode of ARF (peak Scr of 8.7 mg/dL) in a man presenting with nausea, vomiting, loin pain, and abdominal pain after playing scuffle. Renal biopsy at 2 weeks revealed acute tubular necrosis. No further comment was offered concerning the etiology of the ARF. Igarashi et a125 described a boy with isolated renal hypouricemia
942
YEUN
Table
3. Summary
of Patients
With
Renal
Hypouricemia
Who
Developed
Exercise-Induced
AND
HASBARGEN
Acute
Renal
Renal Biopsy (no. of days after ARF)
SJA Age 641 Sex
Source Erley et al*’ Sakurauchi lshikawa
et al** et alp3
Ethnicity
(md W
FsUA w
Defect*
Exercise
0.1-0.3
128-260
3
-
1
Yes
NR
Yes
1
Yes
23/M
Turk
21/M
Japanese
0.7
79
17/M
Japanese
0.6
79.3
22/M
Japanese
0.7
52.8-60
Numabe
et alz4
16/M 17/M
Japanese Japanese
1.0 0.6
43.2 52-70
lgarashi
et alz5
12/M
Japanese
0.3
loo-136
46/M 29/M
Japanese Pakistani
0.9 0.5
50 55-69
Hiroshige Present
et alz6
1 1 or4
4 1 4 or2
Yes Yes
Yes Yes
Symptoms
Dialysis
Episodes
N/V, loin pain
Yes
1
Loin pain, malaise, edema Abdominal and loin pain, NN NN, malaise, abdominal and loin pain, fever NN NN, malaise, abdominal and loin pain N, anorexia, back and loin pain -
No
2
Uric acid nephropathy -
No
1
ATN (13)
No
1
ATN (35)
Yes Yes
1 1
NL (18) ATN (14)
No
1
-
No No
1 5
-
N, abdominal back pain
and
Abbreviations: NR, not reported; N, nausea; V, vomiting; ATN, acute tubular necrosis; NL, nomal. l Types of tubular defects in uric acid handling: 1, presecretory reabsorption defect; 2, increased secretion; defect; 4, presecretory and postsecretory reabsorption defect.
who developed ARF associated with nausea, anorexia, and loin pain after exercise. Of interest, this patient’s mother had a history of recurrent uric acid nephrolithiasis. The investigators proposed that exercise-induced ARF be included as a potential complication of renal hypouricemia, but were unable to comment on the pathogenesis. Hiroshige et alz6 described two patients with isolated renal hypouricemia; one had an episode of exercise-induced ARF 4 years ago. No details are available. Interestingly, two other patients had diabetes mellitus associated with renal hypouricemia and one presented with exercise-induced ARF. This patient was not included in this review because of the diabetes. We hypothesize that ARF occurs with exercise in patients with renal hypouricemia because of the increase in uric acid production during exercise. Several studies have documented an increase in SuA after exhaustive exercise62-66due to either decreased renal excretion or increased production.63 With exhaustive exercise, the resultant lactic acidosis can directly interfere with tubular secretion of urate.‘j3 Decreased glomerular filtration rate and a contracted extracellular volume’j3 can further decrease uric acid excretion. However, hyperuricemia also is a marker for cell energy crisis.67 During cellular energy depletion,
Failure
3, postsecretory
(1)
reabsorption
consumption of adenosine triphosphate (ATP) exceeds its synthesis, resulting in an accumulation of adenosine diphosphate (ADP) and adenosine monophosphate (AMP) and their subsequent degradation to inosine, xanthine, hypoxanthine, and, finally, uric acid. That the hyperuricemia seen during exhaustive exercise is due to overproduction of uric acid is supported by the observation that aerobic exercise does not result in hyperuricemia,64~66768whereas anaerobic exercise causes a sequential increase in first hypoxanthine,63 then uric acid levels. 63-66368 In addition, Fry et a169demonstrated that SuA remained elevated at 24 hours after exercise, while lactic acid levels and Scr had normalized by 2 hours, making decreased excretion an unlikely explanation for the persistent hyperuricemia. Finally, the combined studies of Sutton et ak7’ Sahlin et alyl and Hellsten-Westing et a172 demonstrate conclusively that hyperuricemia postexercise is the result of increased uric acid production. Sutton et a17’ demonstrated through muscle biopsies that intracellular ATP levels decreased after exhaustive exercise while ADP and AMP levels increased. Sahlin et a171showed a step-up in arterial to venous hypoxanthine levels after exhaustive exercise of a muscle group, suggesting increased release of hypoxanthine from the involved mus-
RENAL
HYPOURICEMIA
AND
EXERCISE-INDUCED
ARF
cles. Finally, Hellsten-Westing et al” demonstrated not only an arteriovenous increase in hypoxanthine levels in the involved muscle groups, but also an increased uptake of hypoxanthine and inosine by the liver with concomitant increased uric acid release. Taken together, these three studies confirm that during exhaustive exercise, muscles switch to anaerobic metabolism, and ADP and AMP accumulate and are converted to inosine and hypoxanthine, which are then released into the circulation, taken up by the liver, and converted to uric acid. All the uric acid is then promptly filtered and eliminated by the kidney, increasing the urinary uric acid load and, hence, UuA/Ucr and UVurat,. Volume depletion and/or decreased renal blood flow during exercise can further contribute to concentration of urinary uric acid. In addition, lactic acidosis during exercise may lead to increased urinary acidification, favoring uric acid crystallization. There are several theoretic ways of preventing the ARF if the above hypothesis is true. First, administration of allopurinol should decrease basal production of uric acid, ameliorate its increased production during exercise, decrease its subsequent elimination during exercise, and, therefore, ameliorate the ARF. Second, prophylactic alkalinization of the urine prior to exercising should prevent the ARF by increasing the solubility of uric acid. Third, prophylactic administration of pyrazinamide should decrease urinary uric acid and prevent ARF. We elected to test the hypothesis with the administration of allopurinol. The patient we describe here had recurrent exercise-induced ARF. Although a renal biopsy was not performed, there is indirect evidence implicating uric acid nephropathy in the pathogenesis of ARF. First, UuA/Ucr was greater than 1.O in our patient after exercise, associated with ARF. Kelton et a173noted that UuA/UCr greater than 1 .O accurately correlated with the presence of uric acid nephropathy. None of the controls had a Uu,/Uc, greater than 1.0, and none had ARF. Second, our patient had a dramatic increase in UV”rate after exercise, associated with ARF. In contrast, the controls had only a small increase in UVUrate. The observation of uric acid crystals in the urine after exercise and during episodes of ARF lend further support to this theory. Perhaps more importantly, the administration of allopurino1 was effective in preventing exercise-induced
943
ARF in our patient by preventing the increased uric acid excretion after exercise (Fig 2). In a study of patients with hematologic malignancies, Rieselbach et a174 concluded that uric acid excretion and urinary uric acid concentration are more important determinants than hyperuricemia for the development of uric acid nephropathy. Our data directly support this contention, since urinary indices (UuJUc, and UVurate) are elevated in the face of hypouricemia. Our hypothesis of uric acid nephropathy as the cause of exercise-induced ARF in patients with renal hypouricemia concur with the findings of Erley et al.‘l Although Ishikawa et a123and Numabe et al% did not find evidence for uric acid nephropathy in their kidney biopsy specimens, the renal tissue may have been obtained too late in the course of the renal failure. In addition, if the kidney tissue was fixed with formaldehyde, the uric acid crystals may have leached out of the tissue.75 The acute tubular necrosis observed in Ishikawa et al’s study23 also may have been a direct result of the administered contrast. Their observation of patchy contrast uptake by the renal cortex may have been a result of the administered contrast or residual changes from uric acid nephropathy rather than a cause of the renal failure. Our patient demonstrated no renal cortical perfusion defects on magnetic resonance imaging with gadolinium and renal scan performed within 48 hours of ARF in the absence of intravenous contrast administration. Although Loffler et al49concluded that patients with renal hypouricemia may not respond to allopurinol administration because of increased excretion of the active metabolite oxypurinol, this does not clinically appear to be the case. Frank et al’ and Sasaki et al” treated three patients with uric acid nephrolithiasis and renal hypouricemia with allopurinol and achieved stone dissolution as well as prevented further episodes of stone formation. In the present study, our patient clinically responded to allopurinol with prevention of an increase in UuA/UCr and ARF. In conclusion, although renal hypouricemia is a rare condition, it can be associated with significant morbidity to include uric acid nephrolithiasis and exercise-induced ARF. We propose that the ARF is a result of uric acid nephropathy and can be prevented with the administration of allopurinol.
944
YEUN
ACKNOWLEDGMENT The authors thank Frances Matsumoto for her expertise in translating papers from the Japanese literature.
REFERENCES 1. Sperling 0: Renal hypouricemia: Classification, tubular defect and clinical consequences. Co&b Nephrol lOO:l-14, 1992 2. Hisatome I, Ogino K, Kotake H, Ishiko R, Saito M, Hasegawa J, Mashiba H, Nakamoto S: Cause of persistent hypouricemia in outpatients. Nephron 51:13-16, 1989 3. Kotake T, Miura N, Ito H: Renal tubular hypouricemia and calcium urolithiasis. Scanning Microsc 7:417-421, 1993 4. Sperling 0, Weinberger A, Oliver I, Liberman UA, De Vries A: Hypouricemia, hypercalciuria, and decreased bone density: A hereditary syndrome. Ann Intern Med 80:482-487, 1974 5. Kawabe K, Murayama T, Akaoka I: A case of uric acid renal stone with hypouricemia caused by tubular reabsorptive defect of uric acid. J Urol 116:690-692, 1976 6. Akaoka I, Nishizawa T, Yano E, Kamatani N, Nishida Y, Sasaki S: Renal urate excretion in five cases of hypouricemia with an isolated renal defect of urate transport. J Rheumatol 4:86-94, 1977 7. Frank M, Many M, Sperling 0: Familial renal hypouricemia: Two additional cases with uric acid lithiasis. Br J Urol 5188-91, 1979 8. Hedley JM, Phillips PJ: Familial hypouricaemia associated with renal tubular uricosuria and uric acid calculi: Case report. J Clin ,Pathol 33:971-972, 1980 9. Smetana SS, Bar-Khayim Y: Hypouricemia due to renal tubular defect: A study with the probenecid-pyrazinamide test. Arch Intern Med 145:1200-1203, 1985 10. Sasaki M, Takenawa J, Kanamaru H: A case of idiopathic hypouricemia due to augmented renal tubular secretion of uric acid. Nippon Hinyokika Gakkai Zasshi 77: 1349-1352, 1986 11. Gofrit 0, Verstandig AG, Pode D: Bilateral obstructing ureteral uric acid stones in an infant with hereditary renal hypouricemia. J Urol 149:1506-1507, 1993 12. Hisatome I, Tanaka Y, Kotake H, Kosaka H, Hirata N, Fujimoto Y, Yoshida A, Shigemasa C, Mashiba H, Sato R, Takeda A: Renal hypouricemia due to enhanced tubular secretion of urate associated with urolithiasis: Successful treatment of urolithiasis by alkabnization of urine K+, Na+citrate. Nephron 65:578-582, 1993 13. Kaneko K, Fujimori S, Itoh H, Nakayama Y, Oyama H, Kanbayashi T, Miyashita H, Akaoka I: Renal handling of hypoxanthine and xanthine in normal subjects and in four cases of idiopathic renal hypouricemia. J Rheumatol 15:325330, 1988 14. Greene ML, Marcus R, Aurbach GD, Kazam ES, Seegmiller JE: Hypouricemia due to isolated renal tubular defect: Dalmatian dog mutation in man. Am J Med 53:361367, 1972 15. Benjamin D, Sperling 0, Weinberger A, Pinkhas J, de Vries A: Familial hypouricemia due to isolated renal tubular defect: Attenuated response of uric acid clearance to probenecid and pyrazinamide. Nephron 18:220-225, 1977 16. Barrientos A, Perez-Diaz V, Diaz-Gonzalez R, Rodi-
AND
HASBARGEN
cio JL: Hypouricemia by defect in the tubular reabsorption. Arch Intern Med 139:787-789, 1979 17. Tofuku Y, Kuroda M, Takeda R: Hypouricemia due to renal urate wasting: Two types of tubular transport defect. Nephron 30:39-44, 1982 18. Sanz AM, Alonzo-Vega GG, Anton FM, Puig JG: Hypouricemia and renal tubular urate secretion. Arch Intern Med 143:1633-1634, 1983 19. Gaspar GA, Puig JG, Mateos FA, Oria CR, Gomez ME, Gil AA: Hypouricemia due to renal urate wasting: Different types of tubular transport defects. Adv Exp Med Biol 195A:357-363, 1986 20. DeFerrari ME, Colussi G, Benazzi E, Rombola G, Surian M, Malberti F, Brenna S, Minetti L: Calcium nephrolithiasis and renal tubular hypouricemia. Contrib Nephml 58:41-43, 1987 21. Erley CMM, Hirschberg RR, Hoefer W, Schaefer K: Acute renal failure due to uric acid nephropathy in a patient with renal hypouricemia. Klin Wochenschr 67:308-312,1989 22. Sakurauchi Y, Tsuyuki M, Okazaki Y, Sugiyama B, Yamamoto T: Acute renal failure in a patient with renal hypouricemia. Nippon J Gakkai Shi 3 1:1326, 1989 (abstr) 23. Ishikawa I, Sakurai Y, Masuzaki S, Sugishita N, Shinoda A, Shiknra N: Exercise-induced acute renal failure in 3 patients with renal hypouricemia. Nippon J Gakkai Shi 32923-928, 1990 24. Numabe A, Tsukada H, Sugimoto T, Ono H, Hirao S, Abe M, Yagi S: A case of acute renal failure in a patient with idiopathic hypouricemia. Nippon Jinzo Gakkai Shi 34:841-845, 1992 25. Igarashi T, Sekine T, Sugimura H, Hayakawa H, Arayama T: Acute renal failure after exercise in a child with renal hypouricaemia. Pediatr Nephrol 7:292-293, 1993 26. Hiroshige K, Yuu K, Takasugi M, Soejima M, Kuroiwa A: A study on uric acid excretion in patients with hypouricemia. Nippon Jinzo Gakkai Shi 35:829-834, 1993 27. Praetorius E, Kirk JE: Hypouricemia: With evidence for tubular elimination of uric acid. J Lab Clin Med 35:865868, 1950 28. Khachadurian AK, Arslanian MJ: Hypouricemia due to renal uricosuria: A case study. Ann Intern Med 78:547550, 1973 29. Simkin PA, Skeith MD, Healey LA: Suppression of uric acid secretion in a patient with renal hypomicemia. Isr J Med Sci 9: 1113, 1973 (abstr) 30. Healey LA, Skeith MD, Simkin PA: Hypouricemia: An incidental finding indicating xanthinuria or defective reabsorption of uric acid. Arch Intern Med 134:46-47, 1974 3 1. Akaoka I, Nishizawa T, Yano E, Takeuchi A, Nishida Y, Yoshimura T, Horiuchi Y: Familial hyponricemia due to renal tubular defect of mate transport. Ann Clin Res 7:318324, 1975 32. Benjamin D, Sperling 0, Weinberger A, Pinkhas J: Familial hypouricemia due to isolated renal tubular abnormality. Biomedicine 29:54-56, 1978 33. Fujiwara Y, Takamitsu Y, Ueda N, Orita Y, Abe H: Hypouricemia due to an isolated defect in renal tubular urate reabsorption. Clin Nephrol 13:44-48, 1980 34. Sorensen LB, Levinson DJ: Isolated defect in postsecretory reabsorption of uric acid. Ann Rheum Dis 39:180183, 1980
RENAL
HYPOURICEMIA
AND
EXERCISE-INDUCED
ARF
35. Weitz R, Sperling 0: Hereditary renal hypouricemia. Isolated tubular defect of mate reabsorption .I Pediatr 96:850853, 1980 36. Garty BZ, Nitzan M, Sperling 0: Inborn hypouricemia due to isolated defect in renal tubular uric acid transport. Isr J Med Sci 17:295-297, 1981 37. Suzuki T, Kidoguchi K, Hayashi A: Genetic heterogeneity of familial hypouricemia due to isolated renal tubular defect. Jpn J Hum Genet 26:243-248, 1981 38. Matsuda 0, Shiigai T, Ito Y, Aonuma K, Takeuchi J: A case of familial renal hypouricemia associated with increased secretion of para-aminohippurate and idiopathic edema. Nephron 30:178-186, 1982 39. Shichiri M, Matsuda 0, Shiigai T, Takeuchi J, Kanayama M: Hypouricemia due to an increment in renal tubular urate secretion. Arch Intern Med 142:1855-1857, 1982 40. Dumont I, Decaux G: Hypouricemia related to a hypersecretional tubulopathy. Nephron 34:256-259, 1983 41. Vinay P, Gattereau A, Moulin B, Gougoux A, Lemieux G: Normal urate transport into erythrocytes in familial renal hypouricemia and in the Dalmatian dog. Can Med Assoc J 128:545-549, 1983 42. Takeda E, Kuroda Y, Ito M, Toshima K, Watanabe T, Ito M, Naito E, Yokota I, Hwang TJ, Miyao M: Hereditary renal hypouricemia in children. J Pediatr 107:71-74, 1985 43. Colussi G, Rombola G, deFerrari ME, Roland0 P, Surian M, Malberti F, Minetti L: Pharmacological evaluation of urate renal handling in humans: Pyrazinamide test vs combined pyrazinamide and probenecid administration. Nephrol Dial Transplant 2:10-16, 1987 44. Nakajima H, Gomi M, Iida S, Kono N, Moriwaki K, Tarui S: Familial renal hypouricemia with intact reabsorption of uric acid. Nephron 45:40-42, 1987 45. Shichiri M, Iwamoto H, Maeda M, Kanayama M, Shiigai T: Hypouricemia due to subtotal defect in the urate transport. Clin Nephrol 28:300-303, 1987 46. Shichiri M, Iwamoto H, Shiigai T: Hypomicemia due to increased tubular urate secretion. Nephron 45:3 l-34, 1987 47. Hisatome I, Ogino K, Saito M, Miyamoto J, Hasegawa J, Kotake H, Mashiba H, Nakamoto S: Renal hypouricemia due to an isolated renal defect of urate transport. Nephron 49:81-83, 1988 48. Gafter U, Zuta A, Frydman M, Lewinski UH, Levi J: Hypouricemia due to familial isolated renal tubular uricosuria. Miner Electrolyte Metab 15:309-314, 1989 49. Loffler W, Seibke W, Seibke E, Reiter S, Jahn M, Hehlmann R, Zollner N: Non-responsiveness to allopurinol in renal hypouricaemia. Klin Wochenschr 67:47, 1989 50. Shichiri M, Itoh H, Iwamoto H, Hirata Y, Marumo F: Renal tubular hypouricemia: Evidence for defect of both secretion and reabsorption. Nephron 56:421-426, 1990 5 1. Kawachi M, Kono N, Kiyokawa H, Mineo I, Nakajima H, Shimizu T, Yorifuji S, Kuwajima M, Tami S: Decreased renal clearance of xanthine and hypoxanthine in a patient with renal hypouricemia: An new defect in renal handling of purines. Nephron 61:428-431, 1992 52. Barajas de Frutos D, Bravo Mancheno B, Palomino Urda N, Pedrero Vera J: Familial hypouricaemia due to an isolated tubular defect of mate reabsorption. Pediatr Nephrol 7:83-85, 1993 53. Hisatome I, Kato T, Miyakoda H, Takami T, Abe T,
945 Tanaka Y, Kosaka H, Ogino K, Mitani Y, Yoshida A, Kotake H, Shigemasa C, Mashiba H, Sato R, Takeda A: Renal hypouricemia with both drug-insensitive secretion and defective reabsorption of urate: A novel type of renal hypouricemia. Nephron 64:447-45 1, 1993 54. Uribarri J, Oh MS: Renal hypouricemia and absorptive hypercalciuria: A real syndrome. Nephron 63:172-175, 1993 55. Steele TH, Rieselbach RE: The renal mechanism for urate homeostasis in normal man. Am J Med 43:868-875, 1967 56. Kageyama N: A direct calorimetric determination of uric acid in serum and urine with uricase-catalysts system. Clin Chem Acta 31:421-426, 1971 57. Diamond HS: Interpretation of pharmacologic manipulation of urate transport in man. Nephron 5 1: l-5, 1989 58. Ramsdell CM, Kelley WN: The clinical significance of hypouricemia. Ann Intern Med 78:239-242, 1973 59. Van Peenen HJ: Causes of hypouricemia. Ann Intern Med 78:977-978, 1973 60. Yanase M, Nakahama H, Mikami H, Fukuhara Y, Orita Y, Yoshikawa H: Prevalence of hypouricemia in apparently normal population. Nephron 48:80, 1988 61. Puig JG, Anton FM, Sanz AM, Gaspar G, Lesmes A, Ramos T, Vazquez JO: Renal handling of uric acid in normal subjects by means of the pyrazinamide and probenecid tests. Nephron 35:183-186, 1983 62. Schrier RW, Hano J, Keller HI, Finkel RM, Gilliland PF, Cirksena WJ, Teschan PE: Renal, metabolic, and circulatory responses to heat and exercise. Ann Intern Med 73:213223, 1970 63. Knochel JP, Dotin LN, Hamburger RJ: Heat stress, exercise, and muscle injury: Effects on urate metabolism and renal function. Ann Intern Med 81:321-328, 1974 64. Green HJ, Fraser IG: Differential effects of exercise intensity on serum uric acid concentration. Med Sci Sports Exert 20:55-59, 1988 65. Hellsten-Westing Y, Sollevi A, Sjodin B: Plasma accumulation of hypoxanthine, uric acid and creatine kinase following exhausting runs of differing durations in man. Eur J Appl Physiol 62:380-384, 1991 66. Balsom PD, Seger JY, Sjodin B, Ekblom B: Physiological responses to maximal intensity intermittent exercise. Eur J Appl Physiol 65:144-149, 1992 67. Fox IH, Palella TD, Kelley WN: Hypermicemia: A marker for cell energy crisis. N Engl J Med 3 17: 11 l-l 12, 1987 68. Yamanaka H, Kawagoe Y, Taniguchi A, Kaneko N, Kimata S, Hosoda S, Kamatani N, Kashiwazaki S: Accelerated purine nucleotide degradation by anaerobic but not by aerobic ergometer muscle exercise. Metabolism 41:364-369, 1992 69. Fry RW, Morton AR, Garcia-Webb P, Keast D: Monitoring exercise stress by changes in metabolic and hormonal responses over a 24-h period. Eur J Appl Physiol 63:228234, 1991 70. Sutton JR, Toews CJ, Ward GR, Fox IH: Purine metabolism during strenuous muscular exercise in man. Metabolism 29:254-260, 1980 71. Sahlin K, Ekberg K, Cizinsky S: Changes in plasma hypoxanthine and free radical markers during exercise in man. Acta Physiol Stand 142:275-281, 1991
946 72. Hellsten-Westing Y, Kaijser L, Ekblorn B, Sjodin B: Exchange of purines in human liver and skeletal muscle with short-term exhaustive exercise. Am J Physiol266:R81-86, 1994 73. Kelton J, Kelley WN, Holmes EW: A rapid method for the diagnosis of acute uric acid nephropathy. Arch Intern Med 138:612-615, 1978
YEUN
AND
HASBARGEN
74. Rieselbach RE, Bentzel CJ, Cotlove E, Frei E, Freireich EJ: Uric acid excretion and renal function in the acute hyperuricemia of leukemia: Pathogenesis and therapy of uric acid nephropathy. Am J Med 37:872-884, 1964 75. Conger JD: Acute uric acid nephropathy. Med Clin North Am 74:859-871, 1990