Your search keyword '"Sulfates urine"' showing total 740 results

201. Urinary excretion of cicletanine in the rat. Stereochemical aspects.

Author

Vistelle R, Lamiable D, Morin E, Trenque T, and Kaltenbach M

Subjects

Animals, Chromatography, High Pressure Liquid, Glucuronates urine, Male, Rats, Rats, Wistar, Spectrophotometry, Ultraviolet, Stereoisomerism, Sulfates urine, Antihypertensive Agents urine, Pyridines urine

Abstract

The metabolism of (+)-cicletanine and (-)-cicletanine (10 mg kg-1) was studied in healthy male Wistar rats 24 hr after a single dose and following daily oral administration for 25 days. Urine, collected in 24-hr intervals on days 1, 5, 10, 15, 20, and 25, was analyzed by an HPLC method for parent drug and its sulfate/glucuronide conjugates. In urine, the sulfate and glucuronide conjugates of cicletanine were the only two major components quantitated; parent drug was a minor component. Within 24 hr after the first dose of (+)-cicletanine, the sulfate conjugate was the major urinary component; the ratio of sulfate to glucuronide conjugate was 3. After oral administration of (-)-cicletanine, the glucuronide and sulfate conjugates were present in similar amounts. For each enantiomer, the ratio of sulfate/glucuronide did not change upon multiple dosing, and inversion of the enantiomers did not occur. Although sulfate and glucuronide conjugates of each enantiomer are formed, the relative amounts of each conjugate depends on the enantiomer, indicating that there is stereospecificity in the disposition of cicletanine.

Published

1995

202. High levels of inorganic sulfate cause diarrhea in neonatal piglets.

Author

Gomez GG, Sandler RS, and Seal E Jr

Subjects

Animals, Diarrhea, Infantile urine, Dose-Response Relationship, Drug, Eating drug effects, Eating physiology, Feces chemistry, Female, Humans, Infant, Newborn, Kidney anatomy & histology, Kidney drug effects, Organ Size drug effects, Random Allocation, Sulfates pharmacology, Sulfates urine, Weight Gain drug effects, Weight Gain physiology, Animals, Newborn, Diarrhea, Infantile chemically induced, Disease Models, Animal, Sulfates adverse effects, Swine

Abstract

Artificially reared neonatal piglets were used to study the effect of inorganic sulfate on bowel function in human infants. Two experiments were conducted to evaluate the effect of high levels of inorganic sulfate on the growth, feed intake and feces consistency of artificially reared piglets, and to determine the dose at which at least 50% of piglets develop nonpathogenic diarrhea. The effect of sulfate level on kidney weight and concentration of inorganic sulfate in urine was also assessed. In each experiment, 40 pigs with an average initial age of 5 d were individually caged and reared with an automatic feeding device. Ten pigs per dietary treatment were fed one of four diets containing the following levels of added inorganic sulfate (mg/L of diet), as anhydrous sodium sulfate (USP): 0, 1200, 1600 and 2000 for Experiment 1 (18-d study), and 0, 1800, 2000 and 2200 for Experiment 2 (16-d study). The levels of added sulfate did not affect (P > 0.05) the growth of piglets, or their feed intake. Whereas 1200 mg added sulfate/L had essentially no effect on feces consistency, levels > 1800 mg/L of diet resulted in a persistent, nonpathogenic diarrhea in neonatal piglets. Added sulfate did not affect (P > 0.05) relative kidney weight. Inorganic sulfate in urine reached maximum concentration (P < 0.05) in pigs fed diets with 1600 and 1800 mg added sulfate/L in Experiments 1 and 2, respectively, but declined at higher levels. The results suggest that the level of added dietary inorganic sulfate at which 50% of piglets develop nonpathogenic diarrhea is between 1600 and 1800 mg/L.

Published

1995

203. Different biliary excretion systems for glucuronide and sulfate of a model compound; study using Eisai hyperbilirubinemic rats.

Author

Takenaka O, Horie T, Suzuki H, and Sugiyama Y

Subjects

Animals, Benzothiazoles, Glucuronates urine, Hepatectomy, Hyperbilirubinemia, Hereditary blood, Hyperbilirubinemia, Hereditary urine, Liver metabolism, Liver physiopathology, Male, Pyridines blood, Rats, Rats, Mutant Strains, Rats, Sprague-Dawley, Species Specificity, Sulfates urine, Thiazoles blood, Biliary Tract metabolism, Glucuronates metabolism, Hyperbilirubinemia, Hereditary metabolism, Lipoxygenase Inhibitors blood, Lipoxygenase Inhibitors metabolism, Pyridines metabolism, Sulfates metabolism, Thiazoles metabolism, Thromboxane-A Synthase antagonists & inhibitors

Abstract

The disposition of conjugated metabolites (sulfate and glucuronide) was investigated in Eisai hyperbilirubinemic rats (EHBR) and normal Sprague-Dawley (SD) rats by in vivo and liver perfusion methods. EHBR are mutant rats that have conjugated hyperbilirubinemia as an autosomal recessive trait inheritance, and they show impaired excretion of organic anions into the bile. 6-Hydroxy-5,7-dimethyl-2-methylamino-4-(3-pyridylmethyl) benzothiazole (E3040), a novel dual inhibitor of 5-lipoxygenase and thromboxane A2 synthetase, was used as a model compound, because the major metabolites of E3040 are glucuronide and sulfate. After the i.v. injection of [14C]E3040 to EHBR and SD rats, the plasma AUC for glucuronide was greater in EHBR than in SD rats. The cumulative biliary excretion of the glucuronide was impaired to a great extent in EHBR, and the urinary excretion was enhanced. There was no significant difference in the cumulative biliary and urinary excretion of sulfate between EHBR and SD rats. The influx, efflux and sequestration rates of E3040, measured by a multiple indicator dilution method in the perfused rat liver, were similar in EHBR and SD rats. The biliary excretion of the glucuronide formed in the liver, measured by the liver perfusion method, was also severely impaired in EHBR, so the recovery of the glucuronide in the outflow specimens was markedly enhanced. The disposition of the sulfate did not change in either type of rat.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1995

204. Micronutrient antioxidant status in black South Africans with chronic pancreatitis: opportunity for prophylaxis.

Author

Segal I, Gut A, Schofield D, Shiel N, and Braganza JM

Subjects

Adult, Ascorbic Acid blood, Carotenoids blood, Chronic Disease, Female, Humans, Male, Middle Aged, Reference Values, Selenium blood, South Africa, Sulfates urine, Vitamin E blood, beta Carotene, Antioxidants metabolism, Black People, Micronutrients metabolism, Pancreatitis blood, Pancreatitis prevention & control

Abstract

Biochemical assessments of micronutrient antioxidant status were done in 14 consecutive black patients with calcific chronic pancreatitis and 15 controls at Soweto, near Johannesburg in southern Africa. The patients showed subnormal levels of vitamin C in plasma; selenium, beta-carotene and alpha-tocopherol in serum; and inorganic sulphate (as an index of long-term sulphur amino acid intake) in urine (P < 0.001 for each): furthermore, among the patients ascorbate constituted a lower fraction of vitamin C (P < 0.002), indicating heightened oxidation of the bioactive form. By comparing the results in Sowetan controls with reference ranges from Manchester, UK, the markedly lower vitamin C and, hence, ascorbate levels in the Sowetans was underlined (P < 0.001) and their selenium levels were also lower (P < 0.001), but beta-carotene, alpha-tocopherol and inorganic sulphate levels were comparable. The very low bioavailability of ascorbate among Sowetan controls is reminiscent of our previous finding in outwardly healthy people at Madras in southern India: in both these areas chronic pancreatitis is currently endemic, has a propensity to pancreatic calculi and runs a virulent course towards premature death from diabetes, malnutrition or pancreatic cancer. Considering that low ascorbate levels are a feature in patients with chronic pancreatitis who develop pancreatic calculi at Manchester and that antioxidant supplements ameliorate painful symptoms, we suggest that poor antioxidant intake may predispose underprivileged tropical communities to the disease. If so, there could be an opportunity for prophylaxis through a daily tablet containing vitamin C, perhaps along with selenium at Soweto and beta-carotene at Madras.

Published

1995

205. Effects of the submarine environment on renal-stone risk factors and vitamin D metabolism.

Author

Dlugos DJ, Perrotta PL, and Horn WG

Subjects

Adult, Creatinine urine, Humans, Kidney Calculi blood, Male, Parathyroid Hormone blood, Phosphorus urine, Risk Factors, Sodium urine, Sulfates urine, Vitamin D blood, Diving adverse effects, Kidney Calculi urine

Abstract

The effects of total sunlight deprivation on urinary risk factors for nephrolithiasis and vitamin D metabolism were studied in 20 healthy male subjects. Blood and 24-h urine samples were collected before submarine deployment and 68 days later while still at sea. No subject received sunlight exposure during the test interval. Significant decreases in daily urinary excretion of calcium, uric acid, sodium, sulfate, and phosphorus were found. The relative supersaturation ratio of monosodium urate also fell. There was no change in urinary citrate or urine volume. Mean serum levels of 25-hydroxyvitamin D [25(OH)D] declined from 31 to 19 pg/ml (P < 0.0001), parathyroid hormone increased from 22 to 30 pg/ml (P < 0.0001), and osteocalcin (GLA) increased from 2.7 to 3.3 ng/ml (P = 0.005). Mean serum levels of 1,25 dihydroxy-vitamin D were unchanged. Four subjects had 25(OH)D levels below 10 ng/ml by the end of the submarine patrol. These findings suggest that exposure to the submarine environment produces physiologic changes that decrease the risk for renal stone formation. The data are consistent with the role of vitamin D metabolism in sunlight deprivation and demonstrate that compensatory mechanisms are well established within 68 days.

Published

1995

206. Renal adaptation to altered dietary sulfate in rats.

Author

Benincosa LJ, Sagawa K, and Morris ME

Subjects

Animals, Diet, Female, Fluorescence Polarization, In Vitro Techniques, Membrane Fluidity, Membrane Lipids physiology, Methionine metabolism, Rats, Rats, Inbred Lew, Sulfates urine, Kidney Tubules, Proximal metabolism, Sulfates metabolism

Abstract

Proximal tubular reabsorption is of primary importance in the regulation of the homeostasis of inorganic sulfate, an electrolyte that is necessary for biosynthetic and detoxification reactions. The objective of the present investigation was to determine the effect of dietary sulfate deprivation, produced by a diet low in methionine, on the renal transport of sulfate. Female Lewis rats were fed a diet containing negligible amounts of sulfate and cystine and low in methionine (0.37%) or a control diet (methionine 1.12%, cystine 0.07%) for 8 days to examine the urinary excretion rate and renal clearance of sulfate. The sulfate excretion rate was decreased by day 4 of the low methionine diet and remained low. Both the urinary excretion rates and renal clearance values were significantly decreased on day 8 (144 +/- 71 vs. 517 +/- 264 mumol/12 hr in controls, mean +/- S.D., n = 7, P < .005 and 0.38 +/- 0.19 vs. 1.07 +/- 0.61 ml min-1 kg-1 in controls, n = 5-6, P < .05, respectively), although the serum sulfate concentrations were unchanged. In vitro transport studies were performed in kidney cortex brush border membrane (BBM) and basolateral membrane vesicles isolated from rats fed either the low methionine or control diet for 7 to 9 days. The Vmax for BBM sodium/sulfate cotransport was increased in kidneys from animals that received the low methionine diet (1.1 +/- 0.10 vs. 0.75 +/- 0.08 nmol mg of protein-1 10 sec-1 in controls, n = 5, P < .001); there were no significant differences in the Km.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1995

207. Increased excretion of taurine, hypotaurine and sulfate after hypotaurine loading and capacity of hypotaurine metabolism in rats.

Author

Fujiwara M, Ubuka T, Abe T, Yukihiro K, and Tomozawa M

Subjects

Animals, Kinetics, Male, Rats, Rats, Wistar, Taurine metabolism, Taurine pharmacokinetics, Time Factors, Sulfates urine, Taurine analogs & derivatives, Taurine urine

Abstract

Hypotaurine was intraperitoneally injected into rats and urinary taurine, hypotaurine and sulfate were determined. Taurine excretion increased dose-dependently when 1 to 7 mmol of hypotaurine per kg of body weight was administered. The total excretion and the increased excretion (difference of those before and after the loading) were 2328 +/- 219 and 1948 +/- 153 mumol per kg of body weight per day, respectively, at 7 mmol of hypotaurine loading. Hypotaurine excretion was negligible in the normal rat urine. However, it increased when hypotaurine was loaded. Hypotaurine excretion at 7 mmol of hypotaurine loading was 2282 +/- 258 mumol per kg per day. These results indicate that the capacity of hypotaurine oxidation to taurine in rats is more than 2 mmol per kg per day under the present experimental conditions. Sulfate excretion increased significantly when more than 3 mmol of hypotaurine per kg of body weight was injected. When 5 and 7 mmol of hypotaurine was loaded, the increased excretion of sulfate was 619 +/- 205 and 632 +/- 118 mumol per kg per day, respectively. It was confirmed that in vitro incubation of hypotaurine and 2-oxoglutarate with rat liver homogenate results in the formation of L-glutamate and sulfate. Present findings indicate that hypotaurine in vivo was mainly oxidized to taurine and that it was partly metabolized to sulfate via transamination reaction.

Published

1995

208. 5-Hydroxytryptophol conjugation in man: influence of alcohol consumption and altered serotonin turnover.

Author

Helander A, Beck O, and Boysen L

Subjects

Adult, Drug Stability, Female, Gas Chromatography-Mass Spectrometry, Glucuronates urine, Humans, Hydrolysis, Male, Middle Aged, Sensitivity and Specificity, Sulfates urine, Alcohol Drinking urine, Hydroxytryptophol urine, Serotonin metabolism

Abstract

The distribution of free and conjugated forms of the serotonin (5-hydroxytryptamine) metabolite 5-hydroxytryptophol (5HTOL) in human urine was determined. 5HTOL was analyzed using a sensitive and specific gas chromatographic-mass spectrometric method. The sulfate and glucuronide conjugated forms were measured indirectly following enzymatic hydrolysis. Total 5HTOL levels in control samples ranged between 98-301 nM, in samples collected following ingestion of bananas, a food rich in serotonin, between 450-3292 nM, following alcohol consumption between 863-13326 nM, and in samples obtained from patients with serotonin producing carcinoid tumors between 1695-3793 nM. Free 5HTOL accounted for less than 4% of total 5HTOL in all samples. Sulfate conjugated 5HTOL was calculated to comprise about 17% of total 5HTOL in the control samples and 15% in the alcohol samples, whereas the mean proportion was significantly increased to 33% and 27% in the samples collected after ingestion of bananas and from patients with carcinoid tumors, respectively. The results show that conjugation with glucuronic acid followed by urinary excretion is normally the predominant route for elimination of 5HTOL in man. However, in situations of elevated levels of total 5-hydroxyindoles originating from dietary sources or serotonin producing tumors in the gut, sulfate conjugation becomes more important.

Published

1995

209. Fate in humans of dietary intake of cyanogenic glycosides from roots of sweet cassava consumed in Cuba.

Author

Hernández T, Lundquist P, Oliveira L, Pérez Cristiá R, Rodriguez E, and Rosling H

Subjects

Adult, Creatinine urine, Cuba, Cyanides toxicity, Cyanides urine, Eating, Female, Glycosides pharmacokinetics, Humans, Hydrolysis, Intestines enzymology, Male, Middle Aged, Nitriles pharmacokinetics, Nitriles toxicity, Plant Extracts pharmacokinetics, Plant Extracts toxicity, Smoking urine, Sulfates urine, Thiocyanates urine, beta-Glucosidase metabolism, Cyanides pharmacokinetics, Glycosides toxicity, Manihot, Nitriles urine, Plant Roots metabolism

Abstract

We studied if consumption of boiled fresh roots from sweet cassava varieties grown in Cuba resulted in exposure to cyanogenic glycosides and their final breakdown product, cyanide. When adult, nonsmoking subjects consumed 1-4 kg cassava over 2 days, their urinary levels of the main cyanide metabolite, thiocyanate, only increased from a mean +/- SEM of 12 +/- 2 to 22 +/- 2 mumol/l, indicating a negligible cyanide exposure. Their mean urinary linamarin, the main cyanogenic glucoside in cassava, increased from 2 +/- 1 to 68 +/- 16 mumol/l. In a second experiment 5 subjects consumed one meal of 0.5 kg boiled cassava that contained 105 mumol linamarin and 8 mumol hydrogen cyanide (HCN). Quantitative urine collections prior to and after intake showed that 28% of linamarin was excreted during the following 24 hours, whereas a modest increase of urinary thiocyanate (SCN) only corresponded to the small amount of free HCN ingested. These results indicate that the dominant cyanogen in boiled cassava is glycosides that pass through the human body without causing cyanide exposure. It remains to be studied whether humans occasionally possess intestinal or tissue beta-glucosidases that can hydrolyse cyanogenic glycosides from cassava.

Published

1995

210. Pharmacokinetic profile of conjugated verrucarol urinary metabolites in dogs.

Author

Barel S, Yagen B, and Bialer M

Subjects

Animals, Dogs, Female, Gas Chromatography-Mass Spectrometry, Glucuronates urine, Half-Life, Hydrolysis, Male, Sulfates urine, Trichothecenes administration & dosage, Trichothecenes urine, Trichothecenes pharmacokinetics

Abstract

The pharmacokinetics and renal excretion of a trichothecene mycotoxin, verrucarol, were studied in six mongrel dogs following IV administration (0.4 mg kg-1). The fraction of verrucarol excreted intact in the urine ranged from 0.9% to 2.7% of the administered dose. The fraction of verrucarol metabolites excreted in the urine was 32-60% for verrucaryl glucuronides and 32-47% for verrucaryl sulphates. These urinary conjugated metabolites were analysed quantitatively following their enzymatic hydrolysis. The half-life of verrucarol calculated from the urinary data of its conjugated metabolites was not significantly different from the half-life calculated from the plasma data of the parent compound.

Published

1994

211. Low bone mass in idiopathic renal stone formers: magnitude and significance.

Author

Jaeger P, Lippuner K, Casez JP, Hess B, Ackermann D, and Hug C

Subjects

Absorptiometry, Photon, Adult, Aged, Aged, 80 and over, Amino Acids urine, Analysis of Variance, Biomarkers blood, Biomarkers urine, Calcium urine, Creatinine urine, Femur physiology, Humans, Hydrogen-Ion Concentration, Lumbar Vertebrae physiology, Male, Middle Aged, Reference Values, Sodium urine, Sulfates urine, Tibia physiology, Uric Acid blood, Uric Acid urine, Bone Density physiology, Kidney Calculi pathology

Abstract

To assess bone mineral density (BMD) in idiopathic calcium nephrolithiasis, dual-energy x-ray absorptiometry was performed at lumbar spine, upper femur (femoral neck, Ward's triangle, and total area), distal tibial diaphysis, and distal tibial epiphysis in 110 male idiopathic calcium stone formers (ICSF); 49 with and 61 without hypercalciuria on free-choice diet). Results were compared with those obtained in 234 healthy male controls, using (1) noncorrected BMD, (2) BMD corrected for age, height, and BMI, and (3) a skeletal score based on a tercile distribution of BMD values at following four sites: lumbar spine, Ward's triangle, tibial diaphysis, and tibial epiphysis. After correction, BMD--and therefore also skeletal score--tended to be lower in the stone formers than in controls at five of the six measurement sites, that is, lumbar spine, upper femur, Ward's triangle, tibial diaphysis, and tibial epiphysis, limit of significance being reached for the last two sites without difference between hypercalciuric (HCSF) and normocalciuric stone formers (NCSF). Estimated current daily calcium intake was significantly lower in patients (616 +/- 499 mg/24 h, mean +/- SEM) than in controls (773 +/- 532, p = 0.02). Of 17 patients who in the past had received a low-calcium diet for at least 1 year, 10 had a low skeletal score (4-6) whereas only 1 had a high score (10-12; p = 0.037). Of the 12 stone formers in the study with skeletal score 4 (i.e., the lowest), 8 had experienced in the past one or more fractures of any kind versus only 19 of the remaining 77 patients with skeletal score 5-12 (p = 0.01).(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1994

212. Use of proton nmr spectroscopy to measure propofol metabolites in the urine of the female Caucasian patient.

Author

Sneyd JR, Simons PJ, and Wright B

Subjects

Adult, Female, Glucuronates urine, Humans, Middle Aged, Propofol administration & dosage, Sulfates urine, Anesthesia, Magnetic Resonance Spectroscopy, Propofol urine

Abstract

1. Six female Caucasian patients received i.v. doses of propofol (2.7 +/- 0.3 (SE) mg/kg) for induction of anaesthesia. Anaesthesia was maintained with nitrous oxide, oxygen and enflurane for periods up to 3 h. A total urine collection was made from each subject for 24 h after administration of propofol; samples were concentrated and analysed for propofol metabolites by nmr spectroscopy. 2. By 24 h, 50.9 +/- 4.0% of the dose of propofol was recovered as metabolites. The proportions of propofol metabolites, 1-quinol glucuronide (1-QG), 4-quinol glucuronide (4-QG), propofol glucuronide (PG) and 4-quinol sulphate (4-QS) recovered in urine (0-24 h) of the patients were 12 +/- 1, 8 +/- 2, 76 +/- 4 and 4 +/- 1% respectively. However, one patient showed a metabolite profile in which PG comprised 93% and 1-QG 7% of the total metabolites. 3. Nmr spectroscopy has been shown to be a satisfactory method for the quantification of propofol metabolites in urine without the necessity for reference samples.

Published

1994

213. Urinary excretion of thyroid hormones in rainbow trout, Oncorhynchus mykiss.

Author

Parry JE, Zhang C, and Eales JG

Subjects

Animals, Chromatography, High Pressure Liquid, Female, Glomerular Filtration Rate, Glucuronates urine, Iodine Radioisotopes, Male, Sulfates urine, Thyroxine urine, Triiodothyronine urine, Oncorhynchus mykiss metabolism, Thyroid Hormones urine

Abstract

Urinary excretion of the thyroid hormones (TH) L-thyroxine (T4), and 3,5,3'-triiodo-L-thyronine (T3) and their derivatives was studied in urinary-catheterized rainbow trout (mean wt. 227 g) fasted for 2 days under a 12-hr L:12-hr D photocycle in running water (12 degrees). Catheterized trout were intracardiac-injected with [125I]T4 (*T4) or [125I]T3 (*T3) and urine was collected as 2-hr fractions over 48 hr. The 125I corresponding to I-, TH conjugates (sulfates and glucuronides), or TH was separated by LH-20 column chromatography and HPLC. Urine production (daily mean, 72.5 ml/kg/day) was lowest during the scotophase and doubled at the start of photophase, causing acute fluctuations in excretion of 125I-labeled materials, and implying dependence on glomerular filtration rate. During the first 48 hr, 8.2% of *T4 (I-, 3.6%: TH conjugates, 1.7%; TH, 2.9%) and 6.7% of injected *T3 (I-, 1.8%; TH conjugates, 2.5%; TH, 2.4%) was excreted in urine; 32.6% (*T4) and 26.4% (*T3) was in the gall bladder; 45.5% (*T4) and 45.7% (*T3) were in the remaining carcass; and 13.7% (*T4) and 23.7% (*T3) were lost via other routes. We extrapolate that about 15% of *T4-injected and 12% of *T3-injected total radioactivity would be excreted ultimately in urine, with 8.4% (*T4) and 9.0% (*T3) as TH or their conjugates. Neither a T4 nor a T3 challenge (20 ng/g) influenced the amount of radioactive loss in urine over 48 hr. We conclude that the urine is a significant route for excretion of TH and their conjugates, and that urinary TH loss depends to a large extent on the rate of urine production.

Published

1994

214. Effect of malaria infection on the pharmacokinetics of paracetamol in rat.

Author

Ismail S, Kokwaro GO, Back DJ, and Edwards G

Subjects

Acetaminophen blood, Acetaminophen urine, Animals, Glucuronates urine, Male, Rats, Rats, Wistar, Sulfates urine, Acetaminophen pharmacokinetics, Malaria metabolism, Plasmodium berghei

Abstract

1. Paracetamol (P; 50 and 300 mg/kg i.v.) was administered to the control and malaria-infected (MI) male Wistar rat in order to assess the effect of MI on the metabolism of paracetamol to its glucuronide (PG) and sulphate (PS) conjugates and their excretion in urine. 2. At a dose of 50 mg/kg, neither total clearance (ClT) (controls, 20.3 +/- 0.5; MI, 19.9 +/- 0.9, ml/min/kg; mean +/- SD, p > 0.05) nor the renal clearance of P (ClR) were affected by MI. Although the formation clearance of PG (Clf PG) was decreased by about 40% (controls, 6.6 +/- 1.1; MI, 3.9 +/- 0.9, ml/min/kg, p < 0.05), the formation clearance of PS (Clf PS) was increased by 30% in the MI rat (controls, 8.8 +/- 0.9; MI, 11.2 +/- 1.7, ml/min/kg, p < 0.05), and therefore Clm (controls, 19.7 +/- 0.5; MI, 19.2 +/- 0.8, ml/min/kg, p > 0.05) was unchanged by MI. 3. At a dose of 300 mg/kg, MI produced a significant decrease in the total clearance of P (ClT) (controls, 16.9 +/- 1.0; MI, 11.9 +/- 0.9, ml/min/kg, p < 0.05), metabolic clearance (Clm) (controls, 15.9 +/- 1.4; MI, 11.3 +/- 0.9, ml/min/kg, p < 0.05) and the formation clearance of PG (Clf PG) (controls, 7.9 +/- 1.3; MI, 4.7 +/- 1.5, ml/min/kg, p < 0.05) without affecting Clf PS and ClR of P. 4. These findings indicate that MI impairs the glucuronidation of paracetamol in rat in vivo at both the low and high doses of P. Increased sulphate formation appeared to compensate for decreased glucuronidation at the lower dose.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1994

215. Metabolism of [3H] 17 beta-dihydroequilin and [3H] 17 beta-dihydroequilin sulfate in normal postmenopausal women.

Author

Bhavnani BR, Cecutti A, and Wallace D

Subjects

Equilin administration & dosage, Equilin metabolism, Equilin urine, Estrogens, Conjugated (USP) urine, Female, Glucuronates urine, Humans, Middle Aged, Oxygen Radioisotopes, Sulfates urine, Equilin analogs & derivatives, Postmenopause metabolism

Abstract

The metabolism of 17 beta-dihydroequilin and 17 beta-dihydroequilin sulfate was investigated after intravenous administration of [3H] 17 beta-dihydroequilin and [3H] 17 beta-dihydroequilin sulfate to postmenopausal women. Urine was collected for 3 days and 46.2 +/- 10.5% and 54.5 +/- 8.7% of the injected dose of [3H] 17 beta-dihydroequilin and [17 beta-3H]dihydroequilin sulfate was excreted in the urine respectively. The estrogens present in urine were extracted and fractionated into unconjugated, sulfate, and glucuronide conjugated forms. With both precursors, the major amount (63-64%) of metabolites were excreted in the urine conjugated with glucuronic acid. From the unconjugated, sulfate, and glucuronide fraction, 17 beta-dihydroequilenin, 17 beta-dihydroequilin, equilenin, and equilin were isolated. The conversions with both precursors were similar and 17 beta-dihydroequilenin was the major metabolite isolated from all three fractions; however, the highest levels of all four metabolites were present in the glucuronide fraction. Along with these identifiable metabolites, a large amount (51-81%) of radioactivity was present in the form of metabolites which are more polar than any of the known ring-B unsaturated estrogens. These appear to be polyhydroxy 17 beta-reduced ring-B unsaturated estrogens which remain to be identified. The in-vivo formation of equilenin and 17 beta-dihydroequilenin indicates the presence of the enzyme 6.8(9) steroid dehydrogenase in humans.

Published

1994

216. Design of in vivo cadmium-mobilizing agents: synthesis and properties of monobenzyl meso-2,3-dimercaptosuccinate.

Author

Jones MM, Singh PK, Basinger MA, Gale GR, Smith AB, and Harris WR

Subjects

Administration, Oral, Animals, Bile metabolism, Cadmium urine, Chelating Agents administration & dosage, Chelating Agents pharmacology, Drug Design, Female, Injections, Intraperitoneal, Injections, Intravenous, Male, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Rats, Rats, Sprague-Dawley, Succimer administration & dosage, Succimer chemical synthesis, Succimer pharmacology, Succinates metabolism, Succinates urine, Sulfates metabolism, Sulfates urine, p-Aminohippuric Acid metabolism, p-Aminohippuric Acid urine, Cadmium metabolism, Chelating Agents chemical synthesis, Succimer analogs & derivatives

Abstract

A novel method for the synthesis of monoesters of meso-2,3-dimercaptosuccinic acid (DMSA) is presented which utilizes the reaction of the vicinal sulfhydryl-protected anhydride with the corresponding alcohol in the presence of a base. The product is then treated successively with mercuric chloride to remove the protecting group and form the mercuric complex, and hydrogen sulfide to regenerate thiol groups by removal of mercury as HgS. This strategy was exploited to synthesize monobenzyl meso-2,3-dimercaptosuccinate (MBzDMS), C6H5CH2O(O)CCH(SH)CH(SH)C(O)OH, and demonstrates a feasible synthesis of monoesters difficult to obtain by direct esterification, via the use of the reactive anhydride. The resultant compound was found to be an effective cadminum-mobilizing agent when used with cadmium-exposed rats or mice and when administered by any one of several routes (ip, iv, po). This monobenzyl ester (MBzDMS) of DMSA was found to be somewhat less effective than the corresponding monoisoamyl ester (Mi-ADMS) in mobilizing cadmium from such cadmium deposits. The ability of MBzDMS to mobilize cadmium into the urine is significantly decreased by the coadministration of p-aminobenzoic acid, in support of the hypothesis that MBzDMS enters renal cells via an anion transport system. An analysis of the structural features of vicinal dithiols examined as antagonists for chronic cadmium intoxication allows a hypothesis to be formulated indicating essential features required for the design of effective new cadmium antagonists of this type.

Published

1994

217. The urinary bile acid excretion in healthy premature and full-term infants during the neonatal period.

Author

Strandvik B, Wahlén E, and Wikström SA

Subjects

Cholic Acid, Cholic Acids urine, Gas Chromatography-Mass Spectrometry, Glucuronates urine, Glycine urine, Humans, Hydroxylation, Ketones urine, Prospective Studies, Reference Values, Sulfates urine, Taurine urine, Bile Acids and Salts urine, Infant, Newborn urine, Infant, Premature urine

Abstract

The 24h urinary bile acid excretion was prospectively studied during the neonatal period in healthy, fully breastfed, premature and full-term infants. The urinary bile acids were identified by gas-liquid chromatography (GLC)-mass spectrometry and quantified by GLC. The excretion of bile acids in urine increased after birth, reaching maximum levels by the 3-4th day. Taurine conjugates predominated and the excretion of bile acid sulphates was remarkably low. Cholic acid and atypical bile acids were the main bile acids in urine during the first week. Tetrahydroxylated bile acids carrying hydroxyl groups at C-1, C-2 and C-6 were common, and also other 1- and 6-hydroxylated bile acids, including hyocholic and hyodeoxycholic acids. Three tentatively identified 4-hydroxylated bile acids, including one ketonic bile acid, were also found. Ketonic bile acids constituted an average of 16% of total urinary bile acids during the first week. Unsaturated bile acids were scantily found only during the first days. The excretion of atypical bile acids decreased to 1 month of age, parallel with the total bile acid excretion. The data support earlier hypothesis of a physiological cholestasis in the newborn. Atypical hydroxylated and ketonic bile acids, as well as cholic acid, constituted the major part of the urinary bile acids. The persistent atypical pattern of bile acids in urine during the first month of life indicates a longer period of immaturity of bile acid metabolism in healthy infants than previously described.

Published

1994

218. Polymorphic paracetamol conjugation: phenotyping in a Hungarian population.

Author

Róna K, Ary K, Szüts I, Kovács L, and Gachályi B

Subjects

Administration, Oral, Adult, Age Factors, Chromatography, Liquid, Female, Humans, Hungary, Male, Phenotype, Acetaminophen pharmacokinetics, Glucuronates urine, Sulfates urine

Abstract

The authors studied the distribution of the paracetamol conjugation in a Hungarian population (53 adult Caucasian persons). The data indicated that the excretion of paracetamol glucuronide and sulphate were not normally distributed. Bimodality were apparent in both conjugation pathways: 15.1% of subjects was relatively extensive glucuronidators, and the 24.5% of subjects was extensive sulphatators. Monitoring the ratios of various urinary paracetamol conjugates/paracetamol may be useful as a tool for determining the glucuronide and sulphate conjugation capacity in humans.

Published

1994

219. Death by tanning--a case of fatal basic chromium sulphate poisoning.

Author

van Heerden PV, Jenkins IR, Woods WP, Rossi E, and Cameron PD

Subjects

Adult, Chromium Compounds blood, Chromium Compounds chemistry, Chromium Compounds urine, Fatal Outcome, Female, Humans, Poisoning complications, Prognosis, Renal Dialysis, Sulfates blood, Sulfates chemistry, Sulfates urine, Tanning, Chromium Compounds poisoning, Sulfates poisoning

Abstract

A woman ingested 400 ml of leather tanning solution containing 48 g of basic chromium sulphate (CrOHSO4). This substance forms hydrogen ions and trivalent chromium when it reacts with tissue proteins. The patient died of cardiogenic shock, complicated by pancreatitis and gut mucosal necrosis and haemorrhage. There are no reported cases of toxicity due to oral ingestion of trivalent chromium. Toxicity of hexavalent and trivalent chromium is discussed and suggestions made for management of future cases.

Published

1994

220. Pharmacokinetic interaction between benzene metabolites, phenol and hydroquinone, in B6C3F1 mice.

Author

Legathe A, Hoener BA, and Tozer TN

Subjects

Animals, Benzene metabolism, Drug Interactions, Glucuronates urine, Hydroquinones blood, Hydroquinones pharmacology, Hydroquinones urine, Male, Mice, Mice, Inbred Strains, Models, Biological, Phenol, Phenols blood, Phenols pharmacology, Phenols urine, Sulfates urine, Benzene toxicity, Hydroquinones pharmacokinetics, Phenols pharmacokinetics

Abstract

There is strong evidence that metabolites are responsible for adverse effects of benzene. Benzene myelotoxicity, reproduced by coadministering phenol (PH) and hydroquinone (HQ) but not when these benzene metabolites were administered alone, has been postulated to be induced by PH stimulating the myeloperoxidase-mediated oxidation of HQ to the toxic 1,4-benzoquinone in bone marrow. A pharmacokinetic interaction between PH and HQ is also hypothesized to contribute to the observation. Both metabolites are sulfoconjugated and glucuronoconjugated. Sulfoconjugation of phenolic substrates has been shown to approach saturation at high concentrations in rats. Thus, more PH may be converted to HQ and HQ conjugation may be diminished. These effects would increase the amounts of PH and HQ present and result (by further oxidation) in the formation of more 1,4-benzoquinone. To test this hypothesis, we investigated the pharmacokinetics in blood and the recovery of hydroquinone and phenol in urine when the metabolites were administered intraperitoneally alone or in combination at 75 mg/kg each to B6C3F1 mice. The combination resulted in a 2.6-fold increase in the area under the blood concentration-time curve (AUC) of HQ compared to the sum of AUC values observed after administration of each compound alone. The half-life of HQ was also increased from 9 +/- 2 to 15 +/- 3 min. The AUC of PH was increased by a factor of 1.4. The clearance of phenol decreased from 89 +/- 13 ml/min per kilogram when injected alone to 62 +/- 7 ml/min per kilogram after coadministration. A decreased clearance of formation of each conjugate demonstrated that both conjugation pathways were diminished. This interaction may contribute to the observed production of myelotoxicity when these metabolites are coadministered.

Published

1994

221. The detection of molybdenum cofactor deficiency: clinical symptomatology and urinary metabolite profile.

Author

van Gennip AH, Abeling NG, Stroomer AE, Overmars H, and Bakker HD

Subjects

Amino Acids urine, Child, Preschool, Chromatography, High Pressure Liquid, Humans, Infant, Newborn, Molybdenum Cofactors, Purines urine, Sulfates urine, Coenzymes, Metal Metabolism, Inborn Errors urine, Metalloproteins metabolism, Pteridines metabolism

Published

1994

222. Measurement of urinary androgen sulfates without previous hydrolysis: a tool to investigate adrenarche. Determination of total 17-ketosteroid sulfates.

Author

Remer T, Hintelmann A, and Manz F

Subjects

Adolescent, Adrenal Glands growth & development, Adult, Child, Child, Preschool, Colorimetry statistics & numerical data, Dehydroepiandrosterone analogs & derivatives, Dehydroepiandrosterone urine, Dehydroepiandrosterone Sulfate, Female, Humans, Hydrolysis, Male, Reference Values, Regression Analysis, Sensitivity and Specificity, 17-Ketosteroids urine, Adrenal Glands metabolism, Androgens metabolism, Sulfates urine

Abstract

According to published data the group of urinary total 17-ketosteroid sulfates appears to represent an index of overall adrenal androgen production, at least before the onset of puberty. To quantify total 17-ketosteroid sulfates a modified colorimetric assay based on the Zimmermann reaction was validated. 17-ketosteroid sulfates were measured without previous hydrolysis (as conjugated Zimmermann chromogens against authentic dehydroepiandrosterone sulfate (DHEAS) as assay standard) after C18 reversed-phase extraction and LH-20 chromatography. Intra- and inter-assay coefficients of variation were 8.4% (15.0%) and 5.9% (17.6%), respectively, at urinary 17-ketosteroid sulfate concentrations of 10.8 (1.9) nmol/ml. Recoveries observed in spiking and parallelism experiments varied between 88 and 102%. In a group of 4-year-old children showing a renal DHEAS output of less than 0.1 mumol/d/1.73 m2 (measured by radioimmunoassay) a relatively high median 17-ketosteroid sulfate excretion of 1.29 mumol/d/1.73 m2 was found. Older children aged 8 years as well as a group aged 12-14 years demonstrated only moderately higher urinary 17-ketosteroid sulfates whereas excretion of DHEAS/d/1.73 m2 more than tripled from age group to age group. For children from 8 years onwards, adolescents, and adults, linear regression analysis indicated that urinary DHEAS elevations seem to contribute with a constant proportion of approximately 70% to the increments of total urinary 17-ketosteroid sulfates. These findings suggest that the attainment of such a constant relationship (between the total 17-ketosteroid sulfates and their major component) from about 8 years of age onwards could represent the hormonal correlate of the completion of the continuous zona reticularis in the adrenal gland (developing around this age from a focal reticularis zone).

Published

1994

223. A study of the effect of oral zinc supplementation during pregnancy on pregnancy outcome.

Author

Garg HK, Singhal KC, and Arshad Z

Subjects

Administration, Oral, Apgar Score, Birth Weight drug effects, Female, Fetal Blood, Fetal Growth Retardation prevention & control, Gestational Age, Humans, Infant, Newborn, Infant, Small for Gestational Age, Obstetric Labor, Premature, Pregnancy, Sulfates blood, Sulfates urine, Zinc Compounds blood, Zinc Compounds urine, Zinc Sulfate, Pregnancy Outcome, Sulfates administration & dosage, Zinc Compounds administration & dosage

Abstract

Women in different trimesters of pregnancy (Group B; n = 106) were administered 200 mg zinc sulphate (elemental Zn 45 mg) orally/day from the day of reporting till delivery. Untreated group of 62 served as control. Levels of zinc in maternal serum, umbilical cord blood serum, and urine were estimated. Pregnancy outcome was assessed in terms of incidence of prematurity, IUGR, birth weight; apgar score and gestational age. Serum zinc levels in Gp. A declined significantly from 113.00 +/- 2.80 ug/dl in I trimester to 83.78 +/- 2.20 ug/dl in III (P < 0.001). Following zinc supplementation (Gp. B) serum zinc levels increased significantly from 109.70 + 3.23 micrograms/dl to 205.40 +/- 4.47 micrograms/dl (P < 0.001). Urinary excretion of zinc in Gp. A declined significantly with increase in the period of gestation. However in Gp. B, elimination of Zn increased significantly in proportion with the serum levels (P < 0.001) cord blood serum zinc level was normal irrespective of maternal serum Zn levels. Following oral Zn supplementation, levels increased significantly from below 127.0 micrograms/dl to above 158.0 micrograms/dl in Gp. B (P < 0.001). Maternal serum and cord blood serum zinc ratios were fairly constant in Gp. A as well as in Gp. B. Birth weight of babies born with Zn supplementation was significantly higher than control and was related to duration of oral zinc supplementation (P < 0.001). Gestational age of babies in Gp. B was significantly higher than respective controls when Zn supplementation was given for more than 3 months (P < 0.01), and was related to duration of zinc therapy (P < 0.05).(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

224. Identification of major urinary metabolites of the catechol-O-methyltransferase inhibitor entacapone in the dog.

Author

Wikberg T, Ottoila P, and Taskinen J

Subjects

Animals, Biotransformation, Catechols chemistry, Catechols pharmacokinetics, Chromatography, High Pressure Liquid, Dogs, Female, Glucuronates urine, Hydrolysis, Isomerism, Male, Mass Spectrometry, Nitriles, Spectrophotometry, Infrared, Spectrophotometry, Ultraviolet, Sulfates urine, Catechol O-Methyltransferase Inhibitors, Catechols urine

Abstract

Metabolites of entacapone, (E)-2-cyano-N,N-diethyl-3-(3,4-dihydroxy-5-nitrophenyl) propenamide, a potent inhibitor of catechol-O-methyltransferase, were isolated from dog urine. After hydrolysis of glucuronides and sulfates, 5 metabolites were identified in addition to unchanged entacapone by HPLC with diode-array UV detection, electron ionization mass spectrometry and IR spectroscopy. The (Z)-isomer of entacapone was the most abundant phase I metabolite while less abundant metabolites were formed through cleavage or reduction of the side chain carbon-carbon double bond, hydrolysis of the amide bond or through hydration of the nitrile group. The most abundant urinary metabolites were glucuronides. The glucuronidation site of these ortho-nitrocatechols was shown to be the hydroxyl meta to the nitro group.

Published

1993

225. Induction of 5-oxoprolinuria in the rat following chronic feeding with N-acetyl 4-aminophenol (paracetamol).

Author

Ghauri FY, McLean AE, Beales D, Wilson ID, and Nicholson JK

Subjects

Acetaminophen administration & dosage, Acetaminophen urine, Acetylcysteine urine, Animals, Glucuronates urine, Magnetic Resonance Spectroscopy methods, Male, Rats, Rats, Wistar, Sulfates urine, Acetaminophen metabolism, Pyrrolidonecarboxylic Acid urine

Abstract

The urine of rats fed on 1% paracetamol in the diet for up to 10 weeks was analysed using 500 MHz 1H NMR spectroscopy. After 3 weeks, paracetamol-dosed rats were found to excrete massive quantities of an unknown metabolite in the urine. Using a range of 1 and 2 dimensional 1H NMR spectroscopic techniques, solid phase extraction and mass spectrometry, the metabolite was identified at 5-oxoproline (5OXP, pyroglutamic acid). Rats fed paracetamol plus methionine, which prevents the depletion of sulphur-containing amino acids, did not develop 5OXP-uria during the study period. Quantitative 1H NMR spectroscopy of whole urine showed that no 5OXP appeared in the urine in the first 2 weeks of feeding paracetamol to the animals, but urinary concentrations then rose rapidly up to 1 M in some animals. This unusually high concentration of 5OXP in the urine and its prevention by methionine indicates that chronic high level paracetamol dosing leads to severe depletion of sulphur-containing amino acids including cysteine with consequent disruption of the glutathione cycle.

Published

1993

226. Tiaprofenic acid inhibits the renal reabsorption of sulfate in rats.

Author

Benincosa LJ and Morris ME

Subjects

Animals, Biological Transport, Active, Creatinine metabolism, Female, Glomerular Filtration Rate drug effects, Infusions, Intravenous, Injections, Intravenous, Kidney drug effects, Propionates administration & dosage, Rats, Sulfates blood, Sulfates urine, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Dinoprostone pharmacology, Kidney metabolism, Propionates pharmacology, Sulfates metabolism

Abstract

The objectives of the current investigation were: (1) to examine the effects of the nonsteroidal anti-inflammatory drug, tiaprofenic acid (TA), on sulfate renal reabsorption, and (2) to determine if concomitant prostaglandin E2 (PGE2) could reverse these effects. In crossover studies, female Lewis rats (n = 9) received either TA (as an intravenous (i.v.) bolus injection of 15 mg/kg and constant infusion of 0.02 mg/min) or its vehicle for 6 h. A blood sample was obtained at 5 h and urine was collected between 4 and 6 h. At a steady-state TA serum concentration of approximately 190 micrograms/ml, the PGE2 urinary excretion rate was inhibited by > 90% with no change in glomerular filtration rate (GFR), as measured by creatinine clearance. TA administration resulted in a significant decrease in serum sulfate concentrations (0.65 +/- 0.22 vs 1.1 +/- 0.15 mM, mean +/- SD, p < 0.01) and increase in sulfate clearance ratio (0.32 +/- 0.14 vs 0.13 +/- 0.06, p < 0.01) when compared to the vehicle-treated period. There was also a significant decrease in the fraction of sulfate reabsorbed by the kidneys (0.68 +/- 0.14 vs 0.87 +/- 0.06 in the vehicle-treated period, p < 0.01). In a second crossover study, rats received either TA or TA plus PGE2. PGE2 was administered as an infusion (0.1 micrograms/min) beginning 210 min after the start of the TA infusion. An additional group of rats served as controls and received both vehicles.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1993

227. Studies on the renal excretion of the acyl glucuronide, phenolic glucuronide and sulphate conjugates of diflunisal.

Author

Dickinson RG, King AR, McKinnon GE, Hooper WD, Eadie MJ, and Herkes GK

Subjects

Adult, Blood Proteins metabolism, Diflunisal blood, Diflunisal pharmacology, Diuresis drug effects, Drinking, Drug Interactions, Glucuronates urine, Humans, Kidney Glomerulus metabolism, Kidney Tubules metabolism, Male, Middle Aged, Phenols urine, Probenecid pharmacology, Protein Binding, Sulfates urine, Diflunisal urine

Abstract

1. In five healthy male volunteers given multiple doses of diflunisal (DF), renal clearances (CLR) of the acyl glucuronide (DAG), phenolic glucuronide (DPG) and sulphate (DS) conjugates were about 42, 25 and 13 ml min-1, respectively. 2. These relatively low CLR values are probably due largely to the very high plasma protein binding of the conjugates, found in vitro to be 99.0%, 97.8% and 99.45%, respectively. 3. Thus glomerular filtration plays the minor and active tubular secretion the major role in renal excretion of the three conjugates. 4. This conclusion was supported by the effect of probenecid co-administration, which decreased CLR of DAG and DPG by about 70%. CLR for DS could not be calculated when probenecid was co-administered (because of interference by probenecid metabolites in the analysis of DS in urine). 5. Water-induced diuresis had no effect on CLR of the DF conjugates, consistent with tubular reabsorption being negligible.

Published

1993

228. Metabolism of N-[4-chloro-2-fluoro-5-[(1-methyl-2- propynl)oxy]phenyl]-3,4,5,6-tetrahydrophthalimide (S-23121) in the rat: I. Identification of a new, sulphonic acid type of conjugate.

Author

Yoshino H, Matsunaga H, Kaneko H, Yoshitake A, Nakatsuka I, and Yamada H

Subjects

Animals, Chromatography, High Pressure Liquid, Chromatography, Thin Layer, Cysteine metabolism, Feces, Female, Glucuronates urine, Glutathione metabolism, Herbicides urine, Male, Phthalimides urine, Rats, Rats, Sprague-Dawley, Sulfates metabolism, Sulfates urine, Sulfonic Acids metabolism, Sulfur Radioisotopes, Herbicides metabolism, Phthalimides metabolism

Abstract

1. Several metabolites of 14C-labelled N-[4-chloro-2-fluoro-5-[(1-methyl- 2-propynyl)oxy]phenyl]-3,4,5,6-tetra-hydrophthalimide (S-23121) were identified. 2. The major urinary metabolites were found to be 4-chloro-2-fluoro-5-hydroxyaniline, its sulphate and glucuronide by t.l.c. cochromatography with authentic standards. 3. The major faecal metabolites in addition to the parent compound were six sulphonic acid conjugates having a sulphonic acid group incorporated into the double bond of the 3,4,5,6-tetrahydrophthalimide moiety. These sulphonic acid conjugates have never been reported previously for this type of compound. 4. To confirm the mechanism of biosynthesis of the sulphonic acid conjugates, sodium sulphate, cysteine and glutathione labelled with 35S were administered to the male rat together with unlabelled S-23121. The same faecal metabolites as those detected in faeces of the rat dosed with 14C-labelled S-23121 were similarly found after dosing with any of the 35S-labelled chemicals. Their biosynthesis was most pronounced with 35S-labelled sodium sulphate, implying that the sulphonic acid is incorporated into the double bond after reduction of sulphate to sulphite.

Published

1993

229. Metabolism of 1-(4-hydroxy-3-methoxyphenyl)-2-propanone, a smoke flavour ketone, in rat.

Author

Jodynis-Liebert J

Subjects

Acetone urine, Animals, Chromatography, Gas, Chromatography, Thin Layer, Glucuronates urine, Guaiacol urine, Hydrolysis, Male, Mass Spectrometry, Rats, Rats, Wistar, Sulfates urine, Acetone analogs & derivatives, Flavoring Agents, Guaiacol analogs & derivatives

Abstract

1. Metabolites of 1-(4-hydroxy-3-methoxyphenyl)-2-propanone (HMP-one), a smoke flavour compound, were isolated from rat urine using hydrolysis, ether extraction, t.l.c. and g.l.c. 2. Three metabolites were identified by mass spectrometry and independent synthesis, namely: 1-(3, 4-dihydroxyphenyl)-2-propanone (Met I), 1-(3, 4-dihydroxyphenyl)-2-propanol (Met II), and 1-(4-hydroxy-3-methoxyphenyl)-2-propanol (Met III). 3. A g.l.c. method for the quantitative determination of the parent compound and metabolites in urine was devised. Unchanged HMP-one accounted for about 74% dose, with Met I 11%, Met II 5%, and Met III 9%. All compounds were excreted both as sulphate and glucuronide conjugates.

Published

1993

230. Increased fractional excretion of sulphate in stone formers.

Author

Puche RC, Vaccaro D, Sánchez A, González A, and Sarano HD

Subjects

Adult, Female, Humans, Kidney Calculi blood, Male, Middle Aged, Sulfates blood, Kidney Calculi urine, Sulfates urine

Abstract

This study was performed to determine urinary sulphate excretion in patients with renal stone disease. Stone formers showed a significantly higher fractional excretion of sulphate than control subjects; 80% of stone formers had fractional excretions > 0.26. No significant relationship was established between increased urinary sulphate excretion and any identifiable metabolic disorder, or the recurrence rate of stone episodes. The increase in fractional excretion of sulphate appears to be a more prevalent tubular defect among stone formers than has hitherto been reported.

Published

1993

231. Age-related changes in homeostasis of inorganic sulfate in male F-344 rats.

Author

Bakhtian S, Kimura RE, and Galinsky RE

Subjects

Animals, Glomerular Filtration Rate, Homeostasis, Kidney Tubules metabolism, Kinetics, Male, Rats, Rats, Inbred F344, Renal Circulation, Sulfates blood, Sulfates urine, Aging metabolism, Kidney metabolism, Sulfates metabolism

Abstract

Advanced age is associated with a decline in renal function including decreased glomerular filtration rate, renal blood flow and renal tubular secretion. Endogenous inorganic sulfate homeostasis is maintained by concentration-dependent active renal reabsorption in the proximal tubule. The purpose of this study was to determine the effects of advanced age on: (1) the renal mechanisms for conserving endogenous inorganic sulfate and (2) the turnover of inorganic sulfate. Awake, male Fischer 344 rats age 4-5 months and 22-23 months received i.v. acetaminophen, 300 mg/kg, followed 2 h later by i.v. sodium sulfate, 2 mmol/kg, to lower and raise, respectively, plasma inorganic sulfate in order to measure the renal clearance of this anion from plasma at sub- and supraphysiologic concentration ranges. Another group of old and young male F-344 rats received a tracer injection of [35S]sodium sulfate to determine the effect of aging on the turnover of the endogenous inorganic sulfate pool. There was no statistically significant effect of advanced age on baseline plasma sulfate concentration or on the renal clearance of inorganic sulfate from plasma. The baseline excretion rate of inorganic sulfate in the senescent animals (0.38 +/- 0.25 mumol/min/kg, mean +/- S.D., n = 7) was significantly (P < 0.05) lower than that observed in the young animals (0.64 +/- 0.19 mumol/min/kg, n = 8). There was no difference in the turnover rate constant, as measured by the change in specific activity of urinary [35S]sodium sulfate, for the endogenous sulfate pool in old and young animals. Following acetaminophen administration, plasma sulfate concentrations declined similarly in young and old animals. Under the conditions of relative inorganic sulfate depletion, the renal excretion rate of inorganic sulfate decreased to zero in 7 of 8 young rats, whereas the old animals continued to excrete sulfate anion at an average rate of 23% of the baseline value. Aged animals have a defect in active tubular renal reabsorption of sulfate under conditions of sulfate depletion. Age-related changes in the total sulfate excretion rate may reflect changes in the metabolic fate of endogenous sulfate rather than changes in the endogenous production rate of this anion.

Published

1993

232. Urinary chemistry of the normal Sprague-Dawley rat.

Author

Shevock PN, Khan SR, and Hackett RL

Subjects

Ammonia urine, Animals, Creatinine urine, Electrolytes urine, Enzymes urine, Male, Phosphates urine, Proteinuria urine, Rats, Reference Values, Sulfates urine, Rats, Sprague-Dawley urine, Urine chemistry

Published

1993

233. Identification of major metabolites of the catechol-O-methyltransferase inhibitor entacapone in rats and humans.

Author

Wikberg T, Vuorela A, Ottoila P, and Taskinen J

Subjects

Adult, Animals, Carbon Radioisotopes, Catechols blood, Catechols urine, Chromatography, High Pressure Liquid, Erythrocytes metabolism, Female, Glycosides urine, Humans, Hydrolysis, Male, Mass Spectrometry, Nitriles, Rats, Rats, Wistar, Sulfates urine, Catechol O-Methyltransferase Inhibitors, Catechols metabolism

Abstract

Metabolites of entacapone [(E)-2-cyano-N,N-diethyl-3-(3,4-dihydroxy-5-nitrophenyl)propenamide++ +], a potent inhibitor of catechol-O-methyltransferase, were isolated from human and rat urine. After hydrolysis of glycosides and sulfates, four human and eight rat metabolites were identified, in addition to unchanged entacapone by HPLC with diode-array UV detection, electron ionization mass spectrometry, and IR spectroscopy. In man 10% of an oral dose was excreted in urine during 8 hr. The glucuronides of entacapone and its (Z)-isomer represented about 70 and 25% of the urinary metabolites, respectively. The (Z)-isomer of entacapone and two less abundant urinary metabolites, formed through cleavage or reduction of the side chain carbon-carbon double bond, were also formed in an erythrocyte incubation. The (Z)-isomer was the only phase I metabolite found in addition to entacapone in human plasma. The nitro group of entacapone seems to hinder methylation of the catechol hydroxyls in man, because no methylation products were detected. Twenty-four hr after iv administration of 14C-labeled entacapone to rats, over 50% was excreted in the feces and approximately 35% extensively metabolized in the urine. Entacapone and its phase I metabolites were excreted mainly as glucuronides and sulfates in rat urine. The most abundant urinary metabolite was the glucuronide of entacapone. Unchanged, N-dealkylated, and O-methylated entacapone, the (Z)-isomer of entacapone, and 3,4-dihydroxy-5-nitrobenzaldehyde were found in both plasma and urine from rats. Two minor urinary metabolites were formed through reduction of the side chain carbon-carbon double bond and through acetylation of the amino group resulting from nitro reduction.

Published

1993

234. Reduced vertebral bone density in hypercalciuric nephrolithiasis.

Author

Pietschmann F, Breslau NA, and Pak CY

Subjects

Absorptiometry, Photon, Adult, Fasting, Female, Humans, Male, Middle Aged, Sodium urine, Spine physiopathology, Sulfates urine, Uric Acid urine, Bone Density, Calcium urine, Kidney Calculi physiopathology

Abstract

Dual-energy x-ray absorptiometry and single-photon absorptiometry were used to determine bone density at the lumbar spine and radial shaft in 62 patients with absorptive hypercalciuria, 27 patients with fasting hypercalciuria, and 31 nonhypercalciuric stone formers. Lumbar bone density was significantly lower in patients with absorptive (-10%) as well as in those with fasting hypercalciuria (-12%), with 74 and 92% of patients displaying values below the normal mean, whereas only 48% of the nonhypercalciuric stone formers had bone density values below the normal mean. In contrast, radial bone density was similar in all three groups of renal stone formers investigated. The comparison of urinary chemistry in patients with absorptive hypercalciuria and low normal bone density compared to those with high normal bone density showed a significantly increased 24 h urinary calcium excretion on random diet and a trend toward a higher 24 h urinary uric acid excretion and a higher body mass index in patients with low normal bone density. Moreover, among the patients with absorptive hypercalciuria we found a statistically significant correlation between the spinal bone density and the 24 h sodium and sulfate excretion and the urinary pH. These results gave evidence for an additional role of environmental factors (sodium and animal proteins) in the pathogenesis of bone loss in absorptive hypercalciuria. In conclusion, our data suggest an osteopenia of trabecular-rich bone tissues in patients with fasting and absorptive hypercalciurias.

Published

1992

235. Is the tyramine test for depressive illness useful in elderly patients?

Author

Arnold E, Fineberg N, Hannah P, Glover V, Pitt B, and Sandler M

Subjects

Aged, Aged, 80 and over, Alzheimer Disease diagnosis, Alzheimer Disease psychology, Alzheimer Disease urine, Dementia psychology, Dementia urine, Dementia, Multi-Infarct diagnosis, Dementia, Multi-Infarct psychology, Dementia, Multi-Infarct urine, Depressive Disorder psychology, Depressive Disorder urine, Diagnosis, Differential, Female, Humans, Male, Mental Status Schedule, Personality Inventory, Sulfates urine, Dementia diagnosis, Depressive Disorder diagnosis, Tyramine urine

Abstract

There were no significant differences in tyramine sulphate excretion following tyramine ingestion between elderly depressed, demented or control patient groups, in contrast with younger subjects where this test is a trait marker for unipolar endogenous depression. There are inherent problems in urine collection studies in the elderly and the results may have been influenced by the medication that elderly patients have to take for other disorders. This study suggests that the tyramine test is unlikely to be of clinical usefulness in the over 65 age group.

Published

1992

236. Homeostasis of sulfate and 3'-phosphoadenosine 5'-phosphosulfate in rats with deficient dietary intake of sulfur.

Author

Rozman P, Kim HJ, Madhu C, Gregus Z, and Klaassen CD

Subjects

Amino Acids administration & dosage, Amino Acids pharmacology, Analysis of Variance, Animals, Body Weight drug effects, Chromatography, High Pressure Liquid, Glutathione analysis, Male, Methionine administration & dosage, Rats, Rats, Inbred Strains, Sulfates blood, Sulfates urine, Sulfur administration & dosage, Sulfur deficiency, Kidney metabolism, Liver metabolism, Phosphoadenosine Phosphosulfate metabolism, Sulfates metabolism, Sulfur pharmacology

Abstract

This study was designed to determine the role of dietary organic and inorganic sulfur on 3'-phosphoadenosine 5'-phosphosulfate (PAPS) homeostasis. Organic sulfur was altered by adding various amounts of methionine (0.15, 0.3, 0.6, or 1.2%) to a sulfhydryl-deficient diet. Inorganic sulfur was altered by providing rats with no sulfate or sulfate in their diets (0.12%) and distilled or tap water. Rats received these diets for 5 days. The two lowest methionine-containing diets produced a 60% reduction in liver glutathione concentrations, and the addition of sulfate to the diets did not restore hepatic glutathione levels. Urinary sulfate excretion was reduced by 95% in rats fed the three low-methionine diets. Addition of sulfate to these diets increased the urinary excretion of sulfate, but did not return sulfate levels to control values. The three low-methionine-containing diets decreased serum and liver sulfate concentrations about 50% and addition of sulfate to these diets largely restored them to control levels. Hepatic PAPS concentration was decreased (10%) only in the group receiving the lowest methionine content in their diet, and addition of sulfate had no effect on hepatic PAPS. In summary, dietary alterations of sulfur lowered the glutathione concentration in the liver as well as decreased sulfate levels in serum, liver, and urine, but had minimal effect on hepatic PAPS concentrations. Therefore, it appears that hepatic steady-state PAPS levels are not highly dependent on the sulfur content of the diet.

Published

1992

237. Cassava cyanogens and konzo, an upper motoneuron disease found in Africa.

Author

Tylleskär T, Banea M, Bikangi N, Cooke RD, Poulter NH, and Rosling H

Subjects

Adolescent, Adult, Child, Child, Preschool, Cyanides blood, Cyanides urine, Democratic Republic of the Congo epidemiology, Female, Flour analysis, Flour poisoning, Food Handling methods, Humans, Male, Motor Neuron Disease blood, Motor Neuron Disease epidemiology, Motor Neuron Disease urine, Rural Health, Sampling Studies, Sulfates blood, Sulfates urine, Thiocyanates blood, Thiocyanates urine, Cyanides poisoning, Manihot poisoning, Motor Neuron Disease etiology

Abstract

Konzo is a distinct form of tropical myelopathy characterised by abrupt onset of spastic paraparesis. Epidemics in East Africa have been attributed to dietary cyanide exposure from insufficiently processed cassava but a study done in Zaire disputed such an aetiology. We investigated a konzo-affected population in rural Zaire and measured the cyanogen content of cassava flour, determined urinary thiocyanate as an indicator of cyanide intake, and compared blood cyanide concentrations in cases and controls. The affected population consumed flour made from short-soaked (one day) cassava roots and thus had high dietary cyanide exposure (urinary thiocyanate in 31 children = 757 mumol/l) compared with the unaffected population (urinary thiocyanate in 46 children = 50 mumol/l) that ate cassava that had been soaked for three days before consumption. 3 konzo patients, but only 2 of 23 controls, had blood cyanide concentrations above 4 mumol/l (p less than 0.01), although serum thiocyanate concentrations were similar. Our findings indicate a causal role in konzo of sustained high blood cyanide concentrations maintained by a deficient sulphur intake impairing cyanide to thiocyanate conversion. The underlying causes of konzo are poverty and food shortage, but a minor improvement of food processing may, as in beri-beri, be preventive.

Published

1992

238. Relative importance of urinary sulfate and net acid excretion as determinants of calciuria in normal subjects.

Author

Puche RC and Feldman S

Subjects

Adult, Ammonium Chloride urine, Calcium, Dietary pharmacokinetics, Diet, Vegetarian, Dietary Proteins administration & dosage, Eating, Fasting, Female, Humans, Male, Methionine urine, Middle Aged, Reference Values, Acids urine, Calcium urine, Diet, Sulfates urine

Abstract

In normal subjects fed western-mixed diets, in the fasting state, 39.6% of the variance of calciuria is accounted for by net acid excretion and 4% by sulfaturia. In the postprandial period, net acid accounts for 6.9% and sulfaturia for 11.8% of the variance of calciuria. As expected, after a load of ammonium chloride, net acid excretion exceeded the importance of sulfaturia (36.2% vs. 8.4%) and the opposite was observed after DL-methionine load (1.5% and 46.2%). A group of normal subjects fed vegetarian diets was also investigated. The excretion of the three variables measured were significantly reduced in this group when compared with that of the former group. In the fasting state the variance of calciuria was accounted mainly by net acid excretion (85.7%). In the postprandial state net acid (4.9%) and sulfate (2.2%) had much less importance as determinants of calciuria. It is concluded that in spite of their metabolic relationship, net acid and sulfate excretions are independent determinants of calciuria. The relative importance of each variable changes as a function of metabolic circumstances.

Published

1992

239. Developmental changes in the renal capacity for sulfate reabsorption in the guinea pig.

Author

Neiberger RE

Subjects

Absorption, Age Factors, Animals, Diet, Glomerular Filtration Rate, Guinea Pigs, Kidney growth & development, Kidney Tubules growth & development, Kidney Tubules metabolism, Sulfates blood, Sulfates urine, Kidney metabolism, Sulfates pharmacokinetics

Abstract

During growth, immature guinea pigs maintain a positive inorganic sulfate balance. In the present study, renal clearance techniques were used to determine the maximum renal capacity for sulfate reabsorption [TmRsi/glomerular filtration rate (GFR)] in three groups of guinea pigs at different stages of development (10-34 days, 35-80 days and greater than 120 days of age). These ages are comparable to infant, adolescent, and adult guinea pigs. The guinea pigs were weaned at 10 days and then maintained on normal guinea pig chow (0.13% sulfate). The TmRsi/GFR was determined by infusions of increasing concentrations of sulfate (0-16.8 mumol/min). TmRsi/GFR was significantly greater in young (infant and adolescent) than in older (adult) guinea pigs (2.20 +/- 0.26 mumol/ml and 1.80 +/- 0.27 mumol/ml vs 0.942 +/- 0.08 mumol/ml, P less than 0.05). These results demonstrate that the tubular capacity for inorganic sulfate reabsorption per milliliter of glomerular filtrate is enhanced in immature guinea pigs and decreases with age.

Published

1992

240. Bile acids and conjugates identified in metabolic disorders by fast atom bombardment and tandem mass spectrometry.

Author

Libert R, Hermans D, Draye JP, Van Hoof F, Sokal E, and de Hoffmann E

Subjects

Adrenoleukodystrophy metabolism, Bile Acids and Salts blood, Bile Acids and Salts urine, Glycine analysis, Glycine blood, Glycine urine, Humans, Hydroxylation, Microbodies physiology, Refsum Disease metabolism, Sulfates blood, Sulfates metabolism, Sulfates urine, Taurine analysis, Taurine blood, Taurine urine, Zellweger Syndrome metabolism, Bile Acids and Salts analysis, Mass Spectrometry, Metabolic Diseases metabolism, Spectrometry, Mass, Fast Atom Bombardment

Abstract

From a study of the collision-activated fragmentation of bile acids, a qualitative analytical method based on negative ion fast atom bombardment tandem mass spectrometry has been developed. The times for sample preparation and analyses are short. Both free and conjugated bile acids are detected as they occur in biological fluids, without derivatization. For identifying bile acids and conjugates, the method offers better specificity and sensitivity than does the fast atom bombardment mass spectrometric technique alone. Specific scan modes have been developed for the selective detection of taurine conjugates, delta 4-unsaturated taurine conjugates, delta 4-3-keto free acids and their glycine conjugates, free acids and glycine conjugates bearing a hydroxyl group at the C-12 position, sulfates of glycine and taurine conjugates, and a C29 dicarboxylic bile acid, specific for generalized peroxisomal disorders. Applications of this technique demonstrate its potential usefulness, principally in the diagnosis of several peroxisomal disorders.

Published

1991

241. Paracetamol metabolism after general anaesthesia.

Author

Lewis RP, Dunphy JA, and Reilly CS

Subjects

Acetaminophen blood, Acetaminophen pharmacokinetics, Acetaminophen urine, Acetylcysteine blood, Acetylcysteine urine, Adult, Anesthesia, Inhalation, Anesthesia, Intravenous, Female, Humans, Male, Middle Aged, Postoperative Period, Sulfates blood, Sulfates urine, Time Factors, Acetaminophen metabolism, Anesthesia, General

Abstract

Paracetamol metabolism was compared between nine patients after general anaesthesia and nine healthy volunteers. Each subject received 1.5 g of paracetamol orally, and paracetamol concentrations in venous blood were measured by HPLC at intervals over 12 h. Urine samples collected over 24 h were analysed by HPLC for cysteine, mercapturic acid, sulphate and glucuronide metabolites. There were no significant differences in the area under the concentration-time curve for paracetamol, or plasma half-life. Statistically significant differences were observed in the median percentages of unchanged paracetamol (volunteers 2.9%, patients 2.0%) and mercapturic acid (volunteers 4.5%, patients 6.5%) excreted in 24 h. The percentage of sulphate excreted was significantly lower in the 8-24-h period, although there was no difference over the total 24 h.

Published

1991

242. Effects of protein and carbohydrate content of diet on drug conjugation.

Author

Pantuck EJ, Pantuck CB, Kappas A, Conney AH, and Anderson KE

Subjects

Acetaminophen pharmacokinetics, Adult, Diet, Dietary Carbohydrates administration & dosage, Dietary Proteins administration & dosage, Glucuronates metabolism, Glucuronates urine, Half-Life, Humans, Male, Metabolic Clearance Rate, Oxazepam pharmacokinetics, Sulfates metabolism, Sulfates urine, Dietary Carbohydrates pharmacology, Dietary Proteins pharmacology

Abstract

Eight healthy subjects were fed a high-protein-low-carbohydrate diet and, after a 3-day washout period, an isocaloric low-protein-high-carbohydrate diet. They received acetaminophen and oxazepam, drugs metabolized primarily by conjugation, on days 11 and 13, respectively, of each diet. Changing the diets of subjects from the high-protein-low-carbohydrate diet to the low-protein-high-carbohydrate diet resulted in a 14% increase in urinary recovery of acetaminophen glucuronide and a 32% increase in urinary recovery of oxazepam glucuronide (p less than 0.05). The increases in glucuronidation were at the expense of other pathways of metabolism, and there were no significant changes in the metabolic clearance rates of acetaminophen and oxazepam. Mean renal clearances of acetaminophen glucuronide, acetaminophen sulfate, and oxazepam glucuronide decreased 45%, 32%, and 54%, respectively (p less than 0.05), when the subjects were switched to the low-protein-high-carbohydrate diet.

Published

1991

243. Protein intake and urinary excretion of protein-derived metabolites in aging female vegetarians and nonvegetarians.

Author

Kunkel ME and Beauchene RE

Subjects

Adult, Aged, Aged, 80 and over, Aging urine, Creatinine urine, Diet Records, Dietary Proteins metabolism, Energy Intake, Female, Humans, Hydroxyproline urine, Middle Aged, Nitrogen urine, Plant Proteins, Dietary administration & dosage, Plant Proteins, Dietary metabolism, Regression Analysis, Sulfates urine, Urea urine, Aging metabolism, Diet, Vegetarian, Dietary Proteins administration & dosage

Abstract

Relationships among age, protein intake, and urinary excretion of protein-derived metabolites were studied in 125 vegetarian and nonvegetarian women ages 40-92. There were 63 women in the vegetarian (AV) group and 62 women in the nonvegetarian (NV) group. Average daily intakes of energy and total animal and vegetable protein were calculated from 7-day dietary records. Twenty-four-hour urine samples were analyzed for total nitrogen, urea, creatinine, hydroxyproline, and inorganic sulfate. Energy intakes for the two groups were similar. AVs consumed less total and animal protein and more vegetable protein than NVs, even though both groups consumed more than the RDA for protein. No significant differences existed between the groups in the urinary excretion of total nitrogen, urea nitrogen, hydroxyproline, or inorganic sulfate. Energy and protein intakes and total nitrogen excretion were lower in older AVs than in younger AVs, while those of NVs increased between 40 and 55 years of age, and decreased among the older NV women. The relationship between these variables and age in NVs was more accurately described by polynomial rather than linear regression models.

Published

1991

244. Metabolism of dietary sulphate: absorption and excretion in humans.

Author

Florin T, Neale G, Gibson GR, Christl SU, and Cummings JH

Subjects

Aged, Bacteria isolation & purification, Feces chemistry, Feces microbiology, Female, Humans, Ileostomy, Male, Middle Aged, Sulfates administration & dosage, Sulfates urine, Diet, Intestinal Absorption, Sulfates metabolism

Abstract

Dietary sulphate may affect colonic pathophysiology because sulphate availability determines in part the activity of sulphate reducing bacteria in the bowel. The main product of sulphate reducing bacterial oxidative metabolism, hydrogen sulphide, is potentially toxic. Although it is generally believed that the sulphate ion is poorly absorbed, there are no available data on how much sulphate reaches the colon nor on the relative contributions from diet and endogenous sources. To resolve these questions, balance studies were performed on six healthy ileostomists and three normal subjects chosen because they did not have detectable sulphate reducing bacteria in their faeces. The subjects were fed diets which varied in sulphate content from 1.6-16.6 mmol/day. Sulphate was measured in diets, faeces (ileal effluent in ileostomists), and urine by anion exchange chromatography with conductivity detection. Overall there was net absorption of dietary sulphate, with the absorptive capacity of the gastrointestinal tract plateauing at 5 mmol/day in the ileostomists and exceeding 16 mmol/day in the normal subjects. Endogenous secretion of sulphate in the upper gastrointestinal tract was from 0.96-2.6 mmol/day. The dietary contribution to the colonic sulphate pool ranged up to 9 mmol/day, there being linear identity between diet and upper gastrointestinal losses for intakes above 7 mmol/day. Faecal losses of sulphate were trivial (less than 0.5 mmol/day) in the normal subjects at all doses. It is concluded that diet and intestinal absorption are the principal factors affecting the amounts of sulphate reaching the colon. Endogenous secretion of sulphate by colonic mucosa may also be important in determining amounts of sulphate in the colon.

Published

1991

245. Analysis of anion constituents of urine by inorganic capillary electrophoresis.

Author

Wildman BJ, Jackson PE, Jones WR, and Alden PG

Subjects

Arsenates urine, Arsenic urine, Carbonates urine, Chlorides urine, Citrates urine, Electrophoresis instrumentation, Humans, Nitrates urine, Oxalates urine, Phosphates urine, Sulfates urine, Anions urine, Arsenites, Electrophoresis methods

Abstract

Inorganic capillary electrophoresis (ICE) is a new separations technology which melds the technique of classical electrophoresis with the separations approach of ion chromatography. Matrices which have been difficult to deal with using ion chromatography have proven amenable to analysis by ICE. The simultaneous analysis of weak acid anions, oxalate and citrate and inorganic anions, chloride, sulfate, nitrate, phosphate and carbonate in diluted urine was achieved using ICE. The determination of the oxyanions of arsenic (i.e. arsenite and arsenate) in urine was also performed.

Published

1991

246. Modulation of the secretion of potassium by accompanying anions in humans.

Author

Carlisle EJ, Donnelly SM, Ethier JH, Quaggin SE, Kaiser UB, Vasuvattakul S, Kamel KS, and Halperin ML

Subjects

Acetazolamide pharmacology, Bicarbonates pharmacology, Bicarbonates urine, Chlorides urine, Extracellular Space metabolism, Fludrocortisone pharmacology, Humans, Osmolar Concentration, Reference Values, Sulfates pharmacology, Sulfates urine, Time Factors, Anions pharmacology, Potassium metabolism

Abstract

In animals, secretion of potassium (K) in the cortical collecting duct (CCD) is modulated by the properties of the accompanying anion. In humans, results are inconclusive as previous studies have not differentiated between a kaliuresis due to a rise in the concentration of K from one due to an increase in the volume of urine. Our purpose was to study the effects of chloride (Cl) and bicarbonate on the secretion of K in the CCD in humans using the transtubular K concentration gradient (TTKG), a semi-quantitative index of secretion of K in the terminal CCD. After control blood and urine samples were obtained, all subjects ingested 0.2 mg fludrocortisone to ensure that mineralocorticoids were not limiting the secretion of K. The anionic composition of the urine was varied using three protocols: Normal subjects (N = 11) ingested cystine and methionine to induce sulfaturia; nine subjects with a contracted ECF volume (to lower the concentration of Cl in the urine) were also studied during sulfaturia following the ingestion of cystine and methionine; 13 normovolemic subjects were studied during bicarbonaturia following the ingestion of acetazolamide. When the concentration of Cl in the urine was greater than 15 mmol/liter, sulfate had no effect on the TTKG. With lower concentrations of Cl in the urine, the TTKG rose 1.5-fold. The TTKG rose 1.8-fold in the presence of bicarbonaturia despite concentrations of Cl in the urine that were greater than 15 mmol/liter, suggesting that bicarbonate has additional effects on this K secretory process. At comparable concentrations of sulfate and bicarbonate in the urine, the TTKG was increased only with bicarbonaturia.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1991

247. The effects of high dietary concentrations of sodium saccharin on in vivo metabolism of xenobiotics in rats.

Author

Heaton GD and Renwick AG

Subjects

3-Hydroxyanthranilic Acid metabolism, Administration, Oral, Animals, Arylsulfotransferase metabolism, Cysteine pharmacology, Diet, Female, Glucuronosyltransferase metabolism, Glycosaminoglycans metabolism, Male, Phenol, Rats, Rats, Inbred Strains, Saccharin administration & dosage, Sulfates urine, Urinary Bladder drug effects, Urinary Bladder metabolism, Phenols metabolism, Saccharin pharmacology, Sulfates pharmacokinetics

Abstract

The effect of feeding a diet containing 7.5% sodium saccharin on the conjugation of [14C]phenol has been studied during neonatal development in male and female rats using a two-generation protocol. Decreased formation of phenol sulphate was observed in the F1 saccharin-treated rats from 4 wk of age and this was compensated for by an increase in the formation of quinol glucuronide. This shift in the conjugation pattern of [14C]phenol, with an increase in oxidation, was not sex specific. The daily excretion of indican was significantly increased from 5 wk of age. Feeding a diet containing 7.5% sodium saccharin did not affect in vitro activities of the enzymes involved in the conjugation reactions, that is, aryl sulphotransferase and uridine-5'-diphosphate glucuronyltransferase. The incorporation of 5% cysteine into the diet of saccharin-treated rats for 1 wk prevented the change in conjugation of [14C]phenol observed in the saccharin-treated animals. Absorption of sodium [35S]sulphate from the gastro-intestinal tract was not appreciably affected by a high dietary concentration of sodium saccharin. A high dietary concentration of saccharin affected the conjugation of 3-hydroxyanthranilic acid during neonatal development, possibly as a result of sulphate depletion.

Published

1991

248. The effect of therapeutic doses of paracetamol on sulphur metabolism in man.

Author

Blackledge HM, O'Farrell J, Minton NA, and McLean AE

Subjects

Acetaminophen administration & dosage, Acetaminophen metabolism, Administration, Oral, Adult, Aged, Aged, 80 and over, Dose-Response Relationship, Drug, Female, Humans, Male, Methionine pharmacology, Middle Aged, Sulfates urine, Sulfur urine, Acetaminophen pharmacology, Sulfur metabolism

Abstract

1. This study was designed to investigate the effect of prolonged paracetamol intake on sulphur metabolism in patients. Six patients, taking paracetamol in doses of 2-4 g d-1 and one taking 12 g d-1 took part in the study. Daily (24-h) collections of urine, and also plasma samples from these patients were analysed and in one case a study with additional methionine was performed. 2. The patients showed variable decrease in urinary output of inorganic sulphate but moderately raised plasma levels of inorganic sulphate. 3. Paracetamol metabolism was characterized by dominance of the glucuronidation pathway with the increase of the administered dose of paracetamol. Methionine added to the diet did not change this metabolic pattern. None of the subjects produced more than 0.6 mmol h-1 paracetamol sulphate while total sulphur excretion was 7.5-26.7 mmol d-1. 4. Volunteers taking 3 g d-1 paracetamol were also studied. 5. In persons taking a normal western diet containing over 20 mmol d-1 sulphur amino-acids paracetamol metabolism will not lead to sulphur amino-acid depletion even if high daily doses are used.

Published

1991

249. Simple method for the determination of inorganic sulfate in human serum and urine using single-column ion chromatography.

Author

Hoffman DA, Wallace SM, and Verbeeck RK

Subjects

Acetaminophen administration & dosage, Acetaminophen pharmacology, Humans, Male, Sulfates urine, Chromatography, Ion Exchange methods, Sulfates blood

Abstract

A single-column ion chromatographic assay with conductivity detection was developed to determine inorganic sulfate concentrations in human plasma and urine samples. Plasma samples were ultrafiltered to remove proteins. Plasma ultrafiltrate and urine samples were diluted prior to injection onto the anion-exchange column. The described method is simple, fast, sensitive and reproducible and was used to study the effect of subchronic administration of acetaminophen on the plasma concentrations and urinary excretion of inorganic sulfate in healthy volunteers.

Published

1991

250. Urinary excretion of CGS 5,649 and its conjugated glucuronide and sulfate in man.

Author

Nilsson E, Schneider T, Hoffmann E, and Schmidt EK

Subjects

Chromatography, High Pressure Liquid, Dansyl Compounds analysis, Glucuronates urine, Half-Life, Humans, Male, Psychotropic Drugs pharmacokinetics, Pyridines pharmacokinetics, Spectrometry, Fluorescence, Spectrophotometry, Ultraviolet, Sulfates urine, Psychotropic Drugs urine, Pyridines urine

Abstract

Experiments in animals have indicated that CGS 5,649 B [6-(2-isopropylaminopropyl)-3-pyridinol fumarate] might enhance memory and learning processes and might be a valuable drug for treatment of impairment of vigilance and mental performance in the elderly. CGS 5,649 (I) is extensively metabolized. Therefore, we investigated the excretion of the drug and its conjugates (I-SULF,I-GLUC) into urine after oral administration of 1200 mg of the fumarate salt of I to one healthy male volunteer. Three HPLC methods were developed to analyze the three compounds in urine: a. Solid-phase extraction and UV-measurement at 280 nm; b. Dansylation followed by fluorometric detection (lambda ex 340, lambda em 525 nm); c. Direct injection of diluted urine, gradient system with ion-pair reagent and UV-detection at 280 nm. The conjugates were measured after enzymatic hydrolysis with glucuronidase/sulfatase and sulfatase. I-GLUC was also measured directly since a synthetic sample had become available. Results from the different analytical methods showed agreement: about 100% of the administered dose was excreted within 24 h; the relative amounts of I, I-SULF and I-GLUC were about 1:2:2; after oral administration, CGS 5,649 B is rapidly and completely absorbed; it is eliminated from plasma by conjugation and direct excretion into urine.

Published

1991