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489 results on '"J. Gustafsson"'

451. Specificity of neonatal, androgen-induced imprinting of hepatic steroid metabolism in rats.

Author

Gustafsson J and Stenberg A

Subjects
Animals, DDT pharmacology, Dihydrotestosterone pharmacology, Epitestosterone pharmacology, Etiocholanolone pharmacology, Liver drug effects, Liver enzymology, Male, Rats, Sex Differentiation drug effects, Testosterone pharmacology, Androgens pharmacology, Androstane-3,17-diol metabolism, Androstanes metabolism, Androstenedione metabolism, Animals, Newborn metabolism, Estradiol pharmacology, Liver metabolism
Abstract

The specificity of the neonatal, andreogen-induced, irreversible programming of hepatic steroid metabolism in the rat was investigated. 5-alpha-Dihydrotestosterone propionate and estradiol benzoate were as efficient as testosterone propionate in inducing a male type of liver metabolism in the adult animal, whereas epitestosterone propionate, etiocholanolone propionate, and o,p'-DDT were practically inactive in this respect. These findings indicate that different mechanisms are involved in neonatal imprinting of hepatic steroid metabolism and in the well-known neonatal androgenic and estrogenic induction of persistent estrus and acyclic gonadotropin secreqion.

Published
1976
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453. Metabolism of mono-(2-ethylhexyl)phthalate in fetal, neonatal and adult rat liver.

Author

Sjöberg P, Bondesson U, and Gustafsson J

Subjects
Animals, Cytochrome P-450 CYP4A, Diethylhexyl Phthalate analogs & derivatives, Diethylhexyl Phthalate pharmacokinetics, Female, Gas Chromatography-Mass Spectrometry, Inactivation, Metabolic, Male, Mixed Function Oxygenases metabolism, Pregnancy, Rats, Rats, Inbred Strains, Aging metabolism, Animals, Newborn metabolism, Diethylhexyl Phthalate metabolism, Fetus enzymology, Microsomes, Liver enzymology, Phthalic Acids metabolism
Abstract

The aim of the investigation was to study to what extent maturity influences the metabolism of mono-(2-ethylhexyl)phthalate (MEHP), the primary metabolite of the plasticizer di-(2-ethylhexyl)phthalate. The conversion of MEHP to its (omega-1)-hydroxylated product was determined in liver microsomes from fetal, neonatal (1- and 5-day-old) and adult rats. Product formation was determined by gas chromatography-mass spectrometry. The results show that fetal and neonatal as well as adult rat livers are capable of metabolizing MEHP by (omega-1)-hydroxylation. Preparations from 1- and 5-day-old rats were much more efficient than those from fetal rats. The transition into adult life gave no further increase in hydroxylase activity as compared to that in 5-day-old rats. The work shows that there is a rapid postnatal development of MEHP (omega-1)-hydroxylase activity in the rat.

Published
1988
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454. Biosynthesis of bile acids in man. An in vivo evaluation of the conversion of R and S 3 alpha, 7 alpha, 12 alpha-trihydroxy-5 beta-cholestanoic and 3 alpha, 7 alpha, 12 alpha-24 xi-tetrahydroxy-5 beta-cholestanoic acids to cholic acid.

Author

Swell L, Gustafsson J, Danielsson H, Schwartz CC, and Vlahcevic ZR

Subjects
Bile metabolism, Carbon Radioisotopes, Humans, Kinetics, Radioisotope Dilution Technique, Tritium, Bile Acids and Salts biosynthesis, Cholestanols metabolism, Cholic Acids biosynthesis, Cholic Acids metabolism
Abstract

In vivo studies were carried out on three bile fistula patients to further elucidate the side chain oxidation pathways from C-27 bile acids to cholic acid in man. Two patients each received (25-R)- and (25-S)-3 alpha, 7 alpha,-12 alpha-trihydroxy-5 beta-[7 beta-3H]cholestanoic acid (THCA) on consecutive days and three patients wee administered 3 alpha, 7 alpha, 12 alhpa, 24 xi-tetrahydroxy-5 beta-[7 beta-3H]cholestanoic acid (varanic acid). The varanic acid was biosynthetically prepared with rat liver microsomes and was probably the 24 alpha isomer. The patients efficiently (84 to 97%) converted both (R)- and (S)-THCA to cholic acid. There was no apparent significant difference in the ability of either (R)- or (S)-THCA to form cholic acid. Varanic acid was poorly converted (20 to 27%) to cholic acid in all three patients. From 49 to 75% of the administered 3H activity was recovered in the bile as other labeled products. The bulk (30 to 35%) of this 3H activity was identified by thin layer chromatography as varanic acid. The rate of conversion of (R)-THCA, (S)-THCA, and varanic acid was extremely rapid in all three patients with a t 1/2 of 35 to 74 min. The findings suggest that (a) the stereospecific configuration at C-25 of THCA has no significant effect on the efficiency of side chain oxidation to cholic acid; and (b) side chain cleavage pathways may exist which do not pass through varanic acid, or the oxidation of varanic acid in man is highly stereospecific with respect to the hydroxyl group at C-24. To prove the latter, it will be necessary to compare the metabolism of the 24 alpha and 24 beta isomers of varanic acid.

Published
1981

455. Dispositions of di- and mono-(2-ethylhexyl) phthalate in newborn infants subjected to exchange transfusions.

Author

Sjöberg P, Bondesson U, Sedin G, and Gustafsson J

Subjects
Diethylhexyl Phthalate adverse effects, Diethylhexyl Phthalate analogs & derivatives, Half-Life, Humans, Infant, Newborn, Infant, Premature, Plasticizers adverse effects, Plasticizers metabolism, Diethylhexyl Phthalate blood, Exchange Transfusion, Whole Blood adverse effects, Phthalic Acids blood
Abstract

The dispositions of the plasticizer di-(2-ethylhexyl) phthalate (DEHP) and its primary metabolite mono-(2-ethylhexyl) phthalate (MEHP) were studied in newborn infants subjected to exchange transfusions. During a single exchange transfusion the amounts of DEHP and MEHP infused ranged from 0.8-3.3 and 0.05-0.20 mg kg-1 body weight, respectively. There were indications that about 30% of the infused DEHP originated from parts of the transfusion set other than the blood bag. Approximately 30% of the infused amount of DEHP was withdrawn during the course of each transfusion. Immediately after the transfusions the plasma levels of DEHP ranged between 5.8 and 19.6 micrograms ml-1, and subsequently they declined rapidly. This decline, probably reflecting distribution of DEHP within the body, was followed by a slower elimination phase. The half-life of this phase was approximately 10 h. The maximal plasma levels of MEHP were about 5 micrograms ml-1. In one pre-term infant the elimination of MEHP was slower than its formation, whereas in one full-term newborn the formation appeared to be rate-limiting for the elimination.

Published
1985
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456. Pituitary involvement in the control of hepatic steroid metabolism in the rat.

Author

Skett P, Gustafsson J, Stenberg A, and Larsson A

Subjects
Androstenedione pharmacology, Animals, Cell Line, Female, Follicle Stimulating Hormone isolation & purification, Follicle Stimulating Hormone pharmacology, Kinetics, Liver drug effects, Oxidoreductases metabolism, Rats, Tissue Extracts, Liver metabolism, Pituitary Gland physiology, Steroids metabolism
Published
1976
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458. [Diagnosis and treatment of fetal congenital adrenal cortex hyperplasia].

Author

Gustavson KH, Larsson A, Nillius SJ, Gustafsson J, Tuvemo T, Ritzén M, Haglund-Stengler B, and Luthman H

Subjects
Adrenal Hyperplasia, Congenital drug therapy, Adrenal Hyperplasia, Congenital genetics, Adult, Dexamethasone administration & dosage, Female, Fetal Diseases diagnosis, Fetal Diseases drug therapy, Humans, Infant, Newborn, Male, Prednisolone administration & dosage, Pregnancy, Adrenal Hyperplasia, Congenital diagnosis, Prenatal Diagnosis
Published
1986

460. [Autoimmune polyendocrinopathies in children].

Author

Gustafsson J and Tuvemo T

Subjects
Adolescent, Adult, Age Factors, Child, Endocrine System Diseases classification, Endocrine System Diseases diagnosis, Female, Humans, Male, Autoimmune Diseases, Endocrine System Diseases immunology
Published
1986

461. DiGeorge syndrome in a child with partial monosomy of chromosome 22.

Author

Annerén G, Gustafsson J, and Sunnegårdh J

Subjects
Cytogenetics, DiGeorge Syndrome diagnosis, Female, Humans, Infant, Chromosome Deletion, Chromosomes, Human, Pair 22, DiGeorge Syndrome genetics, Immunologic Deficiency Syndromes genetics
Abstract

A girl with severe neonatal hypocalcaemia, thymic hypoplasia, congenital heart disease and mental retardation in combination with a partial monosomy of chromosome 22, del(22)(pter-q11.3), is reported. Nine other patients with an association between partial monosomy 22 and a DiGeorge syndrome have been reported earlier, and this combination probably constitutes a deletion syndrome similar to the Prader-Willi and the aniridia-Wilms' tumour syndromes. However, the deletion of chromosome 22 is mostly due to a translocation, with trisomy for another chromosomal segment. Such a mechanism may explain the different clinical features seen in patients with partial monosomy 22. In the present case there was an unbalanced translocation with a probable trisomy of the short arm of chromosome 20 combined with the partial monosomy 22. Cytogenetic investigation with high resolution banding techniques is indicated in patients with thymic aplasia and suspected DiGeorge syndrome.

Published
1989
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462. On the stereospecificity of microsomal "26"-hydroxylation in bile acid biosynthesis.

Author

Gustafsson J and Sjöstedt S

Subjects
Animals, Carbon Radioisotopes, Cholesterol metabolism, Hydroxylation, Isotope Labeling, Male, Mevalonic Acid metabolism, Rats, Stereoisomerism, Bile Acids and Salts biosynthesis, Microsomes, Liver metabolism
Abstract

The stereospecificity of microsomal "26" -hydroxylation in bile acid biosynthesis was studied. Cholesterol was biosynthesized from [2-14C] mevalonate by a rat liver preparation. The cholesterol was converted stepwise into 3alpha, 7alpha, 12alpha-trihydroxy-5beta-cholestan-26-oic acid by microsomal and soluble fractions of rat liver homogenate. The 3alpha, 7alpha, 12alpha-trihydroxy-5beta-cholestan-26-oic acid was decarboxylated chemically and the carbon dioxide was assayed for 14C. The amount of radioactivity in the liberated carbon dioxide was assayed for 14C. The amount of radioactivity in the liberated carbon dioxide was such as to indicate complete stereospecificity of the microsomal "26" -hydroxylase system. The system hydroxylates the methyl group in position C-26 (the 25-pro-R methyl group) and its stereospecificity is opposite that of the mitochondrial "26" -hydroxylase system which hydroxylates the methyl group in position C-27 (the 25-pro-S methyl group).

Published
1978

463. Precocious 'feminization' of rat liver enzymes in the presence of ectopic pituitary tissue.

Author

Gustafsson J and Skett P

Subjects
Aging, Androstane-3,17-diol metabolism, Androstenedione metabolism, Animals, Female, Liver metabolism, Male, Pituitary Gland transplantation, Rats, Sex Characteristics, Transplantation, Homologous, Feminization metabolism, Liver enzymology
Abstract

The presence of ectopic pituitary tissue (derived from an adult rat) in prepubertal male and female rats caused the immature, masculine-type hepatic steroid metabolism to develop into female-type metabolism. It is concluded that the hypothalamus-pituitary system controls the ontogenesis of sex-dependent steroid metabolism in rat liver.

Published
1978
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464. Zellweger's cerebro-hepato-renal syndrome--variations in expressivity and in defects of bile acid synthesis.

Author

Gustafsson J, Gustavson KH, Karlaganis G, and Sjövall J

Subjects
Chenodeoxycholic Acid metabolism, Cholestanols metabolism, Cholic Acids metabolism, Female, Gas Chromatography-Mass Spectrometry, Gene Expression Regulation, Genetic Variation, Humans, Infant, Newborn, Liver metabolism, Male, Syndrome, Abnormalities, Multiple genetics, Bile Acids and Salts metabolism
Abstract

Two siblings with Zellweger's cerebro-hepato-renal syndrome are reported. The two children both had multiple anomalies associated with Zellweger's syndrome such as characteristic facial appearance, cerebral dysfunction, muscular hypotonia, liver abnormalities, failure to thrive, marasm and early death. One of the children, a girl, lacked several anomalies that were present in her brother. In one of the children bile acid analysis was performed by use of gas chromatography-mass spectrometry. 3 alpha,7 alpha,12 alpha-trihydroxy-5 beta-cholestanoic acid (THCA) and varanic acid, both precursors of cholic acid, were found. The defect bile acid synthesis may be due both to liver mitochondrial abnormalities and to the absence of liver peroxisomes, conditions known to occur in Zellweger's syndrome.

Published
1983

465. On the heterogeneity of the mitochondrial C27-steroid 26-hydroxylase system.

Author

Gustafsson J

Subjects
Animals, Calcium pharmacology, Cholestanes pharmacology, Cholesterol metabolism, Enzyme Activation drug effects, Gas Chromatography-Mass Spectrometry, Isocitrates pharmacology, Kinetics, Magnesium pharmacology, Male, Rats, Isoenzymes metabolism, Mitochondria, Liver enzymology, Steroid Hydroxylases metabolism
Abstract

Mitochondrial 26-hydroxylation of exogenous cholesterol, endogenous cholesterol, and 5beta-cholestane-3alpha,7alpha,12alpha-triol was studied. 26-Hydroxylation of endogenous cholesterol was measured by mass fragmentography. NADPH and isocitrate stimulated 26-hydroxylation of endogenous as well as exogenous cholesterol. 26-Hydroxylation of endogenous cholesterol was linear with time for 15 min, whereas that of exogenous cholesterol was linear with time for at least 40 min. This finding indicates that the fractions of exogenous and endogenous cholesterol that were 26-hydroxylated did not equilibrate. Mg2+ stimulated isocitrate- and NADPH-dependent 26-hydroxylation of exogenous cholesterol but inhibited in the case of endogenous cholesterol. Ca2+ stimulated NADPH-dependent and inhibited isocitrate-dependent 26-hydroxylation of both exogenous and endogenous cholesterol. It is suggested that the differing effect of Mg2+ on the 26-hydroxylation of exogenous and endogenous cholesterol is related to transfer of the steroid to the enzyme. Isocitrate- and NADPH-dependent 26-hydroxylation of exogenous 5beta-cholestane-3alpha,7alpha,12alpha-triol differed from that of exogenous cholesterol in response to Mg2+ and Ca2+. 26-Hydrocylation of 5beta-cholestane-3alpha,7alpha,12alpha-triol was stimulated by Mg2+ in low concentrations but inhibited by Mg2+ and Ca2+ in high concentrations. Mg2+ had the same influence on the 26-hydroxylation of three dioxygenated C27-steroids known to be intermediates in bile acid biosynthesis. The results are not only compatible with heterogeneity of the mitochondrial 26-hydroxylase system but also with differences in the transport of cholesterol and 5beta-cholestane-3alpha,7alpha,12alpha-triol to the enzyme. The finding of a differing effect of Mg2+ on 26-hydroxylation of exogenous and endogenous cholesterol seems to favor differences in transport rather than heterogeneity of the 26-hydroxylase as an explanation of the results.

Published
1976

466. Biosynthesis of bile acids in man. Hydroxylation of the C27-steroid side chain.

Author

Björkhem I, Gustafsson J, Johansson G, and Persson B

Subjects
Adult, Aged, Alanine Transaminase metabolism, Aspartate Aminotransferases metabolism, Child, Cholestanes metabolism, Cholestenes metabolism, Chromatography, Gas, Chromatography, Thin Layer, Female, Humans, Hydroxylation, Hydroxysteroids metabolism, Ketosteroids metabolism, Liver enzymology, Magnesium pharmacology, Male, Microsomes, Liver metabolism, Middle Aged, Mitochondria, Liver metabolism, Steroid Hydroxylases metabolism, Time Factors, Bile Acids and Salts biosynthesis, Cholesterol metabolism, Sterols metabolism
Abstract

The first step in the degradation of the steroid side chain during biosynthesis of bile acids from cholesterol in man was studied in microsomal and mitochondrial fraction of homogenate of livers from 14 patients. The microsomal fraction was found to catalyze an efficient 25-hydroxylation of 5,8-cholestane-3a,7a,12atriol. A small extent of 23-, 24-, and 26-hydroxylation of the same substrate was observed. 53-Cholestane-3a,7adiol was hydroxylated in the 25-position only to a very small extent. The mitochondrial fraction was found to catalyze 26-hydroxylation of cholesterol, 5-cholestene-3P,7a-diol, 5P-cholestane-3a,7a-diol, 7a-hydroxy-4-cholesten-3-one, and 5,0-cholestane-3a,7a,12a-triol. Addition of Mg++ stimulated the 26-hydroxylation of cholesterol but had no effect or an inhibitory effect on 26-hydroxylation of the other substrates, indicating a heterogeneity of the mitochondrial 26-hydroxylating system. The level of 26-hydroxylase activity towards different substrates varied considerably with different mitochondrial preparations. The roles of the microsomal and mitochondrial 26- hydroxylations as well as the microsomal 25-hydroxylation in biosynthesis of bile acids in man are discussed. The results indicate that microsomal 26-hydroxylation is less important than mitochondrial 26-hydroxylation under normal conditions. The possibility that microsomal 25-hydroxylation is important cannot be ruled out.

Published
1975
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467. Pyruvate-carboxylase deficiency with urea cycle impairment.

Author

Greter J, Gustafsson J, and Holme E

Subjects
Amino Acids blood, Chorionic Villi enzymology, Female, Fibroblasts enzymology, Humans, Infant, Newborn, Acidosis metabolism, Lactates blood, Pyruvate Carboxylase Deficiency Disease, Urea metabolism
Abstract

We report a case of pyruvate-carboxylase deficiency (EC 6.4.1.1, McKusick 26615) with neonatal onset of lactic acidosis, hyperammonemia, and citrullinemia. The patient developed signs of severe liver damage and died at 13 days of age after increasing metabolic acidosis and severe bleedings. The pyruvate-carboxylase activity in fibroblasts was less than 1% of controls, but normal activities of propionyl-CoA carboxylase (EC 6.4.1.3) and 3-methylcrotonyl-CoA carboxylase (EC 6.4.1.4) were found. To prepare for early prenatal diagnosis of pyruvate-carboxylase deficiency, the activity of the enzyme has been measured in chorionic villus samples.

Published
1985
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468. Bile acid metabolism during development: metabolism of taurodeoxycholic acid in human fetal liver.

Author

Gustafsson J, Andersson S, and Sjövall J

Subjects
Gestational Age, Humans, Hydroxylation, In Vitro Techniques, Liver metabolism, Microsomes, Liver metabolism, Taurocholic Acid biosynthesis, Deoxycholic Acid analogs & derivatives, Fetus metabolism, Liver embryology, Taurodeoxycholic Acid metabolism
Abstract

The metabolism of tauro-[24-14C]deoxycholic acid was studied in microsomal preparations from fetal liver. The livers were obtained at legal abortions performed between week 13 and 24. Taurodeoxycholic acid was efficiently hydroxylated in the 1 beta- and 7 alpha-positions. The hydroxylase activities did not increase with gestational age. A marked variation in extent of hydroxylation was noted between different preparations. The results are discussed in relation to earlier knowledge of fetal and neonatal bile acid metabolism.

Published
1985
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469. Purification of human thyroid peroxidase using ion exchange liquid chromatography.

Author

Gustafsson J, Mendel-Hartvig I, Tötterman TH, and Karlsson FA

Subjects
Autoantibodies, Electrophoresis, Polyacrylamide Gel, Enzyme-Linked Immunosorbent Assay, Humans, Iodide Peroxidase immunology, Microsomes enzymology, Thyroglobulin analysis, Thyroid Gland enzymology, Thyroiditis, Autoimmune enzymology, Chromatography, Ion Exchange, Iodide Peroxidase isolation & purification
Abstract

We have utilized a one step ion-exchange (FPLC Mono Q) purification procedure for the isolation of human thyroid peroxidase (TPO). The purified TPO had the properties of a major microsomal antigen and inhibited the binding of human microsomal autoantibodies to thyroid microsomal membranes. The isolated TPO was free from thyroglobulin and showed, compared with crude microsomal proteins, a reduced background binding with control sera in enzyme-linked immunoassay (ELISA). SDS-gel electrophoresis of the isolated TPO detected one major band with an apparent molecular weight of 105 kD. The antigenicity of the protein was demonstrated by immunoblotting using sera from patients with autoimmune thyroiditis. These results demonstrate that FPLC Mono Q chromatography offers a rapid, quantitative and precise method for large scale purification of TPO with retained enzymatic and antigenic activity for use in ELISA and for further studies on the structure and function of this protein.

Published
1987

471. Conversion of 3 alpha, 7 alpha, 12 alpha-trihydroxy-5 beta-cholestanoic acid into cholic acid by rat liver peroxisomes.

Author

Pedersen JI and Gustafsson J

Subjects
Adenosine Triphosphate metabolism, Animals, Coenzyme A metabolism, In Vitro Techniques, Magnesium metabolism, Male, Microsomes, Liver metabolism, Mitochondria, Liver metabolism, NAD metabolism, Rats, Cholic Acids biosynthesis, Cholic Acids metabolism, Liver metabolism, Microbodies metabolism, Organoids metabolism
Published
1980
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472. Mitochondrial omega-hydroxylation of cholesterol side chain.

Author

Björkhem I and Gustafsson J

Subjects
Animals, Calcium pharmacology, Carbon Radioisotopes, Cholestenes metabolism, Citrates pharmacology, Deuterium, Hydroxylation, Hydroxymercuribenzoates pharmacology, Hydroxysteroids metabolism, Isocitrates pharmacology, Liver cytology, Magnesium pharmacology, Male, Metals pharmacology, Mitochondria, Liver drug effects, Mitochondria, Liver enzymology, NAD pharmacology, NADP pharmacology, Oxygen, Oxygen Isotopes, Rats, Steroid Hydroxylases metabolism, Cholesterol metabolism, Mitochondria, Liver metabolism
Published
1974

473. Biosynthesis of cholic acid in rat liver. 24-Hydroxylation of 3alpha, 7alpha, 12alpha-trihydroxy-5beta-cholestanoic acid.

Author

Gustafsson J

Subjects
Animals, Cytosol metabolism, Hydrogen-Ion Concentration, Hydroxylation, Kinetics, Male, Microsomes, Liver metabolism, Mitochondria, Liver metabolism, Rats, Cholestanes metabolism, Cholic Acids biosynthesis, Liver metabolism
Abstract

Conversion of 3alpha, 7alpha, 12alpha-trihydroxy-5beta-[7beta-3H]cholestanoic acid into 3alpha, 7alpha, 12alpha, 24-tetrahydroxy-5beta-cholestanoic acid in rat liver was catalyzed either by the mitochondrial fraction fortified with the 100,000 times g supernatant fluid or the microsomal fraction fortified with 100,000 times g supernatant fluid and ATP. The microsomal system was more active than the mitochondrial system. With the microsomal system the rate of reaction was considerably faster with free 3alpha, 7alpha, 12alpha-trihydroxy-5beta-cholestanoic acid as substrate than with the corresponding coenzyme A ester. Addition of coenzyme A inhibited the activity. Addition of cofactors other than ATP and coenzyme A did not markedly influence the reaction. The 100,000 times g supernatant fluid could be substituted with a protein fraction obtained by ammonium sulfate precipitation and Sephadex chromatography of the 100,000 times g supernatant fluid. The reaction was not catalyzed by a mixed function oxidase since there was no incorporation of 18O into the product when the reaction was performed in an atmosphere containing 18O2. On the other hand, oxygen may be obligatory since there was almost complete inhibition when the reaction was performed in an atmosphere consisting of nitrogen. Carbon monoxide did not inhibit the reaction. One atom of deuterium was incorporated into the product when the reaction was performed in a medium containing deuterated water. It was concluded that microsomal 24-hydroxylation of 3alpha, 7alpha, 12alpha-trihydroxy-5beta-cholestanoic acid involves the combined action of a desaturase and a hydratase. The reaction catalyzed by the hydratase appears to be stereospecific since the 24alpha epimer of 3alpha, 7alpha,12alpha-trihydroxy-5beta-cholestanoic acid was the predominant product. In contrast to the microsomal system, the mitochondrial system was not stimulated by the addition of ATP and was not inhibited by coenzyme A. The coenzyme A ester of 3alpha, 7alpha, 12alpha-trihydroxy-5beta-cholestanoic acid was 24-hydroxylated more efficiently than the free acid.

Published
1975

474. Bile acid metabolism in cirrhosis. VIII. Quantitative evaluation of bile acid synthesis from [7 beta-3H]7 alpha-hydroxycholesterol and [G-3H]26-hydroxycholesterol.

Author

Goldman M, Vlahcevic ZR, Schwartz CC, Gustafsson J, and Swell L

Subjects
Adult, Bile Acids and Salts analysis, Chenodeoxycholic Acid metabolism, Cholic Acids metabolism, Humans, Kinetics, Middle Aged, Tritium, Bile Acids and Salts biosynthesis, Hydroxycholesterols metabolism, Liver Cirrhosis metabolism
Abstract

In order to evaluate more definitively the observed aberrations in the synthesis of cholic and chenodeoxycholic acids in patients with advanced cirrhosis, two bile acid biosynthesis pathways were examined by determining the efficiency of conversion of [3H]7 alpha-hydroxycholesterol and [3H] 26-hydroxycholesterol to primary bile acids. Bile acid kinetics were determined by administration of [14C]cholic and [14C]chenodeoxycholic acids. Cholic acid synthesis in cirrhotic patients was markedly depressed (170 vs. 927 mumoles per day)( while chenodeoxycholic acid synthesis was reduced to a much lesser degree (227 vs. 550 mumoles per day). The administration of [3H]7 alpha-hydroxycholesterol allowed for an evaluation of the major pathway of bile acid synthesis via the 7 alpha-hydroxylation of cholesterol. This compound was efficiently incorporated into primary bile acids by the two normal subjects (88 and 100%) and two cirrhotic patients (77 and 91%). However, the recovery of the label in cholic acid was slightly less in cirrhotic patients than in normal subjects. [3H]26-hydroxycholesterol was administered to ascertain the contribution of the 26-hydroxylation pathway to bile acid synthesis. All study subjects showed poor conversion (9 to 22%) of this intermediate into bile acids. The results of this study suggest that a major block in the bile acid synthesis pathway in cirrhosis is at the level of 7 alpha-hydroxylation of cholesterol (impairment of 7 alpha-hydroxylase) and /or in the feedback triggering mechanism regulating bile acid synthesis. The data also suggest that the 26-hydroxylation pathway in normal subjects and patients with cirrhosis is a minor contributor to synthesis of the primary bile acids. Therefore, the relative sparing of chenodeoxycholic acid synthesis observed in cirrhotic patients is not due to preferential synthesis of this bile acid via the 26-hydroxylation pathway.

Published
1982
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475. Unspecific DNA binding of the DNA binding domain of the glucocorticoid receptor studied with flow linear dichroism.

Author

Hagmar P, Dahlman K, Takahashi M, Carstedt-Duke J, Gustafsson J, and Nordén B

Subjects
DNA-Binding Proteins ultrastructure, Humans, In Vitro Techniques, Nucleic Acid Conformation, Protein Conformation, Receptors, Glucocorticoid ultrastructure, Spectrum Analysis, DNA metabolism, DNA-Binding Proteins metabolism, Receptors, Glucocorticoid metabolism
Abstract

The unspecific interaction between the DNA-binding domain of the human glucocorticoid receptor and DNA was studied using linear dichroism (LD) and circular dichroism (CD) spectroscopy. The amplitude of the LD signal was found to increase upon addition of protein at ionic strengths less than 60 nM Na+, indicating an increased persistence length of the complex compared to uncomplexed DNA. Analysis of the LD spectrum suggests that the binding does not involve intercalation of tyrosine residues. Evidence of saturation is found at a binding stoichiometry of approximately 5 DNA base pairs per protein monomer.

Published
1989
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476. Effect of biliary obstruction on 26-hydroxylation of C27-steroids in bile acid synthesis.

Author

Gustafsson J

Subjects
Animals, Kinetics, Ligation, Male, Microsomes, Liver metabolism, Mitochondria, Liver metabolism, Rats, Bile Acids and Salts biosynthesis, Bile Ducts physiology, Liver metabolism, Steroid Hydroxylases metabolism
Abstract

The effect of biliary obstruction on side chain hydroxylations in the biosynthesis and metabolism of bile acids was studied in the rat. For comparison, several other hydroxylation reactions in bile acid biosynthesis and metabolism were assayed. Biliary obstruction inhibited microsomal 26-hydroxylation of 5beta-cholestane-3alpha,7alpha-diol and microsomal 25- and 26-hydroxylation of 5beta-cholestane-3alpha,7alpha-12alpha-triol. Microsomal 7alpha-hydroxylation of cholesterol and 6beta-hydroxylation of lithocholic acid acid increased significantly, whereas the increase in microsomal 12alpha-hydroxylation of 5beta-cholestane-3alpha,7alpha-diol was less. Mitochondrial 26-hydroxylation of cholesterol, 5-cholestene-3beta,7alpha-diol, and 7alpha-hydroxy-4-cholesten-3-one was stimulated, whereas 26-hydroxylation of 5beta-cholestane-3alpha,7alpha-diol was not affected and that of 5beta-cholestane-3alpha,7alpha,12alpha-triol was markedly inhibited. The results indicate that mitochondrial 26-hydroxylation, particularly of substrates that primarily are precursors of chenodeoxycholic acid, plays a more important role in bile acid biosynthesis under conditions of biliary obstruction than under normal conditions.

Published
1978

477. S-100 protein and neuron-specific enolase in cerebrospinal fluid and serum: markers of cell damage in human central nervous system.

Author

Persson L, Hårdemark HG, Gustafsson J, Rundström G, Mendel-Hartvig I, Esscher T, and Påhlman S

Subjects
Craniocerebral Trauma diagnosis, Electrophoresis, Polyacrylamide Gel, Female, Humans, Male, Middle Aged, Radioimmunoassay methods, Cerebrovascular Disorders diagnosis, Phosphopyruvate Hydratase analysis, S100 Proteins analysis
Abstract

The development of a radioimmunoassay for S-100 protein is described. This method was used in combination with a recently developed radioimmunoassay for neuron-specific enolase in cerebrospinal fluid and serum from 47 patients with cerebral infarction, transient ischemic attack, intracerebral hemorrhage, subarachnoid hemorrhage, and head injury. In cerebrospinal fluid, increased concentrations of both S-100 and neuron-specific enolase were found after large infarcts, whereas after small infarcts and transient ischemic attacks, only neuron-specific enolase increased. The increased concentrations of S-100 and/or neuron-specific enolase were noted 18 hours to 4 days after cerebral infarction and transient ischemic attacks. Cerebrospinal fluid concentrations of these proteins also reflected the severity of the disease in patients with intracerebral hematoma, subarachnoid hemorrhage, or head injury. Temporal changes in serum S-100 and neuron-specific enolase concentrations reflected the clinical course in 4 patients. In stroke patients, the S-100 and neuron-specific enolase concentrations may reflect the extent of brain damage and could be useful in selecting patients with major stroke for more aggressive treatment during the acute phase.

Published
1987
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478. Bile acid metabolism during development: metabolism of lithocholic acid in human fetal liver.

Author

Gustafsson J, Anderson S, and Sjövall J

Subjects
Gas Chromatography-Mass Spectrometry, Gestational Age, Humans, Hydroxylation, Liver metabolism, Microsomes, Liver metabolism, Bile Acids and Salts metabolism, Lithocholic Acid metabolism, Liver embryology
Abstract

The metabolism of [24-14C]lithocholic acid was studied in the microsomal fraction of fetal human liver homogenates. Fetal livers were obtained at legal abortions performed between wk 14 and 24. Product formation was analyzed by thin-layer chromatography, liquid chromatography, and gas chromatography-mass spectrometry. From wk 14 lithocholic acid was hydroxylated in several positions. Hyodeoxycholic acid (3 alpha,6 alpha-dihydroxy-5 beta-cholanoic) and 1 beta,3 alpha-dihydroxy-5 beta-cholanoic acid were identified among the products. The 3 beta-isomer of the former acid, 6 alpha-hydroxy-3-oxo-5 beta-cholanoic acid and a 2-hydroxylithocholic acid were tentatively identified. Two other metabolites carried a hydroxyl group in an unknown position, one of them probably at an angular methyl group. The highest total conversions per mg of microsomal protein were obtained with preparations from 18 wk fetuses. The results are discussed with particular reference to the role of lithocholic acid in fetal hepatotoxicity.

Published
1987
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479. Omega-hydroxylation of steriod side-chain in biosynthesis of bile acids.

Author

Björkhem I and Gustafsson J

Subjects
Animals, Carbon Monoxide, Chenodeoxycholic Acid biosynthesis, Cholestanes, Cholestenes, Cholesterol, Hydroxylation, Male, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Mitochondria, Liver drug effects, Mitochondria, Liver enzymology, NAD, NADP, Phenobarbital pharmacology, Rats, Starvation, Steroid Hydroxylases metabolism, Bile Acids and Salts biosynthesis, Microsomes, Liver metabolism, Mitochondria, Liver metabolism
Published
1973
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482. On the effect of thyroid hormone on 26-hydroxylation of C 27 -steroids in rat liver.

Author

Björkhem I, Danielsson H, and Gustafsson J

Subjects
Animals, Carbon Isotopes, Cholestenes metabolism, Cholesterol metabolism, Hydroxylation, In Vitro Techniques, Male, Microsomes, Liver enzymology, Microsomes, Liver metabolism, Mitochondria, Liver enzymology, Mitochondria, Liver metabolism, Rats, Thyroid Gland physiology, Thyroidectomy, Triiodothyronine pharmacology, Tritium, Cholestanes metabolism, Liver metabolism, Mixed Function Oxygenases metabolism, Thyroid Hormones pharmacology
Published
1973
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