Your search keyword '"Crigler-Najjar Syndrome metabolism"' showing total 61 results

1. Induction of fecal cholesterol excretion is not effective for the treatment of hyperbilirubinemia in Gunn rats.

Author

Blankestijn M, van de Peppel IP, Dvorak A, Capkova N, Vitek L, Jonker JW, and Verkade HJ

Subjects

Animals, Bile chemistry, Bile Acids and Salts metabolism, Bilirubin chemistry, Chenodeoxycholic Acid pharmacology, Chenodeoxycholic Acid therapeutic use, Crigler-Najjar Syndrome metabolism, Dietary Fats pharmacokinetics, Ezetimibe pharmacology, Haptoglobins analysis, Hydrocarbons, Fluorinated pharmacology, Intestines drug effects, Intestines metabolism, Lipids blood, Liver X Receptors metabolism, Male, PPAR delta metabolism, Random Allocation, Rats, Rats, Gunn, Receptors, Cytoplasmic and Nuclear metabolism, Sulfonamides pharmacology, Chenodeoxycholic Acid analogs & derivatives, Cholesterol metabolism, Crigler-Najjar Syndrome therapy, Ezetimibe therapeutic use, Feces chemistry, Hydrocarbons, Fluorinated therapeutic use, Hyperbilirubinemia therapy, Sulfonamides therapeutic use

Abstract

Background: Unconjugated hyperbilirubinemia, a feature of neonatal jaundice or Crigler-Najjar syndrome, can lead to neurotoxicity and even death. We previously demonstrated that unconjugated bilirubin (UCB) can be eliminated via transintestinal excretion in Gunn rats, a model of unconjugated hyperbilirubinemia, and that this is stimulated by enhancing fecal fatty acid excretion. Since transintestinal excretion also occurs for cholesterol (TICE), we hypothesized that increasing fecal cholesterol excretion and/or TICE could also enhance fecal UCB disposal and subsequently lower plasma UCB concentrations., Methods: To determine whether increasing fecal cholesterol excretion could ameliorate unconjugated hyperbilirubinemia, we treated hyperbilirubinemic Gunn rats with ezetimibe (EZE), an intestinal cholesterol absorption inhibitor, and/or a liver X receptor (LXR) and farnesoid X receptor (FXR) agonist (T0901317 (T09) and obeticholic acid (OCA), respectively), known to stimulate TICE., Results: We found that EZE treatment alone or in combination with T09 or OCA increased fecal cholesterol disposal but did not lower plasma UCB levels., Conclusions: These findings do not support a link between the regulation of transintestinal excretion of cholesterol and bilirubin. Furthermore, induction of fecal cholesterol excretion is not a potential therapy for unconjugated hyperbilirubinemia., Impact: Increasing fecal cholesterol excretion is not effective to treat unconjugated hyperbilirubinemia. This is the first time a potential relation between transintestinal excretion of cholesterol and unconjugated bilirubin is investigated. Transintestinal excretion of cholesterol and unconjugated bilirubin do not seem to be quantitatively linked. Unlike intestinal fatty acids, cholesterol cannot "capture" unconjugated bilirubin to increase its excretion. These results add to our understanding of ways to improve and factors regulating unconjugated bilirubin disposal in hyperbilirubinemic conditions.

Published

2021

2. Ultrasound-guided in Utero Transplantation of Placental Stem Cells into the Liver of Crigler-Najjar Syndrome Model Rat.

Author

Grubbs BH, Ching MM, Parducho KR, Chmait RH, and Miki T

Subjects

Animals, Cell Survival, Crigler-Najjar Syndrome diagnostic imaging, Crigler-Najjar Syndrome embryology, Crigler-Najjar Syndrome metabolism, Disease Models, Animal, Female, Gestational Age, Graft Survival, Humans, Liver diagnostic imaging, Liver embryology, Liver metabolism, Pregnancy, Rats, Gunn, Time Factors, Transplantation, Heterologous, Crigler-Najjar Syndrome surgery, Fetal Therapies adverse effects, Liver surgery, Placenta cytology, Stem Cell Transplantation adverse effects, Ultrasonography, Interventional

Abstract

Background: Advances in prenatal screening and early diagnosis of genetic disease will potentially allow for preemptive treatment of anticipated postnatal disease by in utero cell transplantation (IUCT). This strategy carries potential benefits over postnatal treatment, which might allow for improved engraftment and function of the transplanted cells. Congenital metabolic disorders may be an ideal target for this type of therapy, as in most cases, they require replacement of a single deficient hepatic enzyme, and multiple small-animal models exist for preclinical testing., Methods: The Gunn rat, a Crigler-Najjar syndrome model animal lacking UDP-glucuronosyltransferase (UGT1A1), was used as recipient. Human amniotic epithelial cells (hAECs), which possess hepatic differentiation potential, were transplanted into the midgestation fetal Gunn rat liver via ultrasound-guided IUCT. The impact of IUCT on live birth and postnatal survival was evaluated. Human cell engraftment was immunohistochemically analyzed on postnatal day 21., Results: Ultrasound-guided IUCT was conducted in rat fetuses on embryonic day 16. Following IUCT, the antihuman mitochondria-positive cells were detected in the liver of recipient rats at postnatal day 21., Conclusions: Here, we have introduced ultrasound-guided IUCT of hAEC using a small-animal model of a congenital metabolic disorder without immunosuppression. The immunological advantage of IUCT was demonstrated with xenogeneic IUCT. This procedure is suitable to conduct preclinical studies for exploring the feasibility and efficacy of ultrasound-guided transuterine cell injection using rodent disease models.

Published

2019

3. Quantitative Systems Pharmacology Model of hUGT1A1-modRNA Encoding for the UGT1A1 Enzyme to Treat Crigler-Najjar Syndrome Type 1.

Author

Apgar JF, Tang JP, Singh P, Balasubramanian N, Burke J, Hodges MR, Lasaro MA, Lin L, Millard BL, Moore K, Jun LS, Sobolov S, Wilkins AK, and Gao X

Subjects

Animals, Bilirubin blood, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Disease Models, Animal, Genetic Therapy, Glucuronosyltransferase metabolism, Humans, Liver chemistry, Models, Theoretical, Nanoparticles, RNA, Messenger blood, RNA, Messenger metabolism, Rats, Rats, Gunn, Treatment Outcome, Crigler-Najjar Syndrome therapy, Glucuronosyltransferase genetics, RNA administration & dosage, RNA pharmacokinetics

Abstract

Crigler-Najjar syndrome type 1 (CN1) is an autosomal recessive disease caused by a marked decrease in uridine-diphosphate-glucuronosyltransferase (UGT1A1) enzyme activity. Delivery of hUGT1A1-modRNA (a modified messenger RNA encoding for UGT1A1) as a lipid nanoparticle is anticipated to restore hepatic expression of UGT1A1, allowing normal glucuronidation and clearance of bilirubin in patients. To support translation from preclinical to clinical studies, and first-in-human studies, a quantitative systems pharmacology (QSP) model was developed. The QSP model was calibrated to plasma and liver mRNA, and total serum bilirubin in Gunn rats, an animal model of CN1. This QSP model adequately captured the observed plasma and liver biomarker behavior across a range of doses and dose regimens in Gunn rats. First-in-human dose projections made using the translated model indicated that 0.5 mg/kg Q4W dose should provide a clinically meaningful and sustained reduction of >5 mg/dL in total bilirubin levels., (© 2018 The Authors CPT: Pharmacometrics & Systems Pharmacology published by Wiley Periodicals, Inc. on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2018

4. Disruption of HNF1α binding site causes inherited severe unconjugated hyperbilirubinemia.

Author

van Dijk R, Mayayo-Peralta I, Aronson SJ, Kattentidt-Mouravieva AA, van der Mark VA, de Knegt R, Oruc N, Beuers U, and Bosma PJ

Subjects

Adult, Base Sequence, Binding Sites genetics, Constitutive Androstane Receptor, Crigler-Najjar Syndrome classification, Female, Homozygote, Humans, Liver metabolism, Molecular Sequence Data, Mutagenesis, Insertional, Promoter Regions, Genetic, Receptors, Cytoplasmic and Nuclear metabolism, Sequence Analysis, DNA, Transcription, Genetic drug effects, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Glucuronosyltransferase deficiency, Glucuronosyltransferase genetics, Hepatocyte Nuclear Factor 1-alpha metabolism

Abstract

Crigler-Najjar syndrome presents as severe unconjugated hyperbilirubinemia and is characteristically caused by a mutation in the UGT1A1 gene, encoding the enzyme responsible for bilirubin glucuronidation. Here we present a patient with Crigler-Najjar syndrome with a completely normal UGT1A1 coding region. Instead, a homozygous 3 nucleotide insertion in the UGT1A1 promoter was identified that interrupts the HNF1α binding site. This mutation results in almost complete abolishment of UGT1A1 promoter activity and prevents the induction of UGT1A1 expression by the liver nuclear receptors CAR and PXR, explaining the lack of a phenobarbital response in this patient. Although animal studies have revealed the importance of HNF1α for normal liver function, this case provides the first clinical proof that mutations in its binding site indeed result in severe liver pathology stressing the importance of promoter sequence analysis., (Copyright © 2015 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published

2015

5. Metastable and equilibrium phase diagrams of unconjugated bilirubin IXα as functions of pH in model bile systems: Implications for pigment gallstone formation.

Author

Berman MD and Carey MC

Subjects

Animals, Bile metabolism, Bilirubin metabolism, Calcium Chloride chemistry, Cholesterol metabolism, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Disease Models, Animal, Gallstones metabolism, Hemolysis, Humans, Hydrogen-Ion Concentration, Hydrophobic and Hydrophilic Interactions, Lecithins chemistry, Mice, Micelles, Rats, Gunn, Rats, Sprague-Dawley, Sodium Chloride chemistry, Solubility, Spectrophotometry, Ultraviolet, Temperature, Urea chemistry, Bile chemistry, Bilirubin chemistry, Gallstones chemistry, Models, Chemical

Abstract

Metastable and equilibrium phase diagrams for unconjugated bilirubin IXα (UCB) in bile are yet to be determined for understanding the physical chemistry of pigment gallstone formation. Also, UCB is a molecule of considerable biomedical importance because it is a potent antioxidant and an inhibitor of atherogenesis. We employed principally a titrimetric approach to obtain metastable and equilibrium UCB solubilities in model bile systems composed of taurine-conjugated bile salts, egg yolk lecithin (mixed long-chain phosphatidylcholines), and cholesterol as functions of total lipid concentration, biliary pH values, and CaCl2 plus NaCl concentrations. Metastable and equilibrium precipitation pH values were obtained, and average pKa values of the two carboxyl groups of UCB were calculated. Added lecithin and increased temperature decreased UCB solubility markedly, whereas increases in bile salt concentrations and molar levels of urea augmented solubility. A wide range of NaCl and cholesterol concentrations resulted in no specific effects, whereas added CaCl2 produced large decreases in UCB solubilities at alkaline pH values only. UV-visible absorption spectra were consistent with both hydrophobic and hydrophilic interactions between UCB and bile salts that were strongly influenced by pH. Reliable literature values for UCB compositions of native gallbladder biles revealed that biles from hemolytic mice and humans with black pigment gallstones are markedly supersaturated with UCB and exhibit more acidic pH values, whereas biles from nonstone control animals and patients with cholesterol gallstone are unsaturated with UCB., (Copyright © 2015 the American Physiological Society.)

Published

2015

6. Inherited disorders of bilirubin transport and conjugation: new insights into molecular mechanisms and consequences.

Author

Erlinger S, Arias IM, and Dhumeaux D

Subjects

Animals, Bile metabolism, Biological Transport, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Genetic Predisposition to Disease, Gilbert Disease genetics, Gilbert Disease metabolism, Hepatocytes metabolism, Heredity, Humans, Hyperbilirubinemia, Hereditary genetics, Hyperbilirubinemia, Hereditary physiopathology, Jaundice, Chronic Idiopathic genetics, Jaundice, Chronic Idiopathic metabolism, Membrane Transport Proteins genetics, Pedigree, Phenotype, Bile Acids and Salts metabolism, Hyperbilirubinemia, Hereditary metabolism, Liver metabolism, Membrane Transport Proteins metabolism

Abstract

Inherited disorders of bilirubin metabolism might reduce bilirubin uptake by hepatocytes, bilirubin conjugation, or secretion of bilirubin into bile. Reductions in uptake could increase levels of unconjugated or conjugated bilirubin (Rotor syndrome). Defects in bilirubin conjugation could increase levels of unconjugated bilirubin; the effects can be benign and frequent (Gilbert syndrome) or rare but severe, increasing the risk of bilirubin encephalopathy (Crigler-Najjar syndrome). Impairment of bilirubin secretion leads to accumulation of conjugated bilirubin (Dubin-Johnson syndrome). We review the genetic causes and pathophysiology of disorders of bilirubin transport and conjugation as well as clinical and therapeutic aspects. We also discuss the possible mechanisms by which hyperbilirubinemia protects against cardiovascular disease and the metabolic syndrome and the effects of specific genetic variants on drug metabolism and cancer development., (Copyright © 2014 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2014

7. Truncated UDP-glucuronosyltransferase (UGT) from a Crigler-Najjar syndrome type II patient colocalizes with intact UGT in the endoplasmic reticulum.

Author

Suzuki M, Hirata M, Takagi M, Watanabe T, Iguchi T, Koiwai K, Maezawa S, and Koiwai O

Subjects

Glucuronosyltransferase chemistry, Glucuronosyltransferase genetics, Green Fluorescent Proteins metabolism, HEK293 Cells, Humans, Photobleaching, Protein Binding, Protein Transport, Subcellular Fractions metabolism, Crigler-Najjar Syndrome enzymology, Crigler-Najjar Syndrome metabolism, Endoplasmic Reticulum enzymology, Mutant Proteins metabolism

Abstract

Mutations in the gene encoding bilirubin UDP-glucuronosyltransferase (UGT1A1) are known to cause Crigler-Najjar syndrome type II (CN-II). We previously encountered a patient with a nonsense mutation (Q331X) on one allele and with no other mutations in the promoter region or other exons, and proposed that CN-II is inherited as a dominant trait due to the formation of a heterologous subunit structure comprised of the altered UGT1A1 gene product (UGT1A1-p.Q331X) and the intact UGT1A1. Here, we investigated the molecular basis of CN-II in this case by expressing UGT1A1-p.Q331X in cells. UGT1A1-p.Q331X overexpressed in Escherichia coli or mammalian cells directly bound or associated with intact UGT1A1 in vitro or in vivo, respectively. Intact UGT1A1 was observed as a dimer using atomic force microscopy. Fluorescent-tagged UGT1A1-p.Q331X and intact UGT1A1 were colocalized in 293T cells, and fluorescence recovery after photobleaching analysis showed that UGT1A1-p.Q331X was retained in the endoplasmic reticulum (ER) without rapid degradation. These findings support the idea that UGT1A1-p.Q331X and UGT1A1 form a dimer and provide an increased mechanistic understanding of CN-II.

Published

2014

8. [Neonatal hyperbilirubinemia and molecular mechanisms of jaundice].

Author

Jirsa M and Sticová E

Subjects

Humans, Hyperbilirubinemia, Neonatal classification, Infant, Newborn, Jaundice classification, Jaundice metabolism, Jaundice, Chronic Idiopathic classification, Jaundice, Neonatal classification, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Hyperbilirubinemia, Hereditary metabolism, Hyperbilirubinemia, Neonatal metabolism, Jaundice, Chronic Idiopathic metabolism, Jaundice, Neonatal metabolism

Abstract

The introductory summarises the classical path of heme degradation and classification of jaundice. Subsequently, a description of neonatal types of jaundice is given, known as Crigler Najjar, Gilberts, DubinJohnson and Rotor syndromes, emphasising the explanation of the molecular mechanisms of these metabolic disorders. Special attention is given to a recently discovered molecular mechanism of the Rotor syndrome. The mechanism is based on the inability of the liver to retrospectively uptake the conjugated bilirubin fraction primarily excreted into the blood, not bile. A reduced ability of the liver to uptake the conjugated bilirubin contributes to the development of hyperbilirubinemia in common disorders of the liver and bile ducts and to the toxicity of xenobiotics and drugs using transport proteins for conjugated bilirubin.

Published

2013

9. Gilbert and Crigler Najjar syndromes: an update of the UDP-glucuronosyltransferase 1A1 (UGT1A1) gene mutation database.

Author

Canu G, Minucci A, Zuppi C, and Capoluongo E

Subjects

Crigler-Najjar Syndrome metabolism, Gilbert Disease metabolism, Humans, Crigler-Najjar Syndrome genetics, Databases, Nucleic Acid, Gilbert Disease genetics, Glucuronosyltransferase genetics, Mutation

Abstract

UGT1A1 enzyme defects are responsible of both Gilbert syndrome (GS) and Crigler-Najjar syndrome (CNS). GS depends on a variant TATAA element (which contains two extra TA nucleotides as compared to the wild type genotype) in the UGT1A1 gene promoter resulting in a reduced gene expression. On the contrary, CNS forms are classified in two types depending on serum total bilirubin concentrations (STBC): the more severe (CNS-I) is characterized by high levels of STBC (342-684μmol/L), due to total deficiency of the UGT1A1 enzyme, while the milder one, namely CNS-II, is characterized by partial UGT1A1 deficiency with STBC ranging from 103 to 342μmol/L. GS and CNS are caused by genetic lesions involving a complex locus encoding the UGT1A1 gene. The present report provides an update of all reported UGT1A1 gene mutations associated to GS and CNS., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

10. Beyond plasma bilirubin: the effects of phototherapy and albumin on brain bilirubin levels in Gunn rats.

Author

Cuperus FJ, Schreuder AB, van Imhoff DE, Vitek L, Vanikova J, Konickova R, Ahlfors CE, Hulzebos CV, and Verkade HJ

Subjects

Acute Disease, Animals, Bilirubin blood, Chronic Disease, Disease Models, Animal, Hyperbilirubinemia metabolism, Hyperbilirubinemia therapy, Jaundice metabolism, Jaundice therapy, Male, Random Allocation, Rats, Rats, Gunn, Albumins pharmacology, Bilirubin metabolism, Brain metabolism, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome therapy, Phototherapy methods

Abstract

Background & Aims: Severe unconjugated hyperbilirubinemia, as occurs in Crigler-Najjar disease and neonatal jaundice, carries the risk of neurotoxicity. This neurotoxicity is related to the increased passage of free bilirubin (UCB(free)), the fraction of bilirubin that is not bound to plasma proteins, into the brain. We hypothesized that albumin treatment would lower the UCB(free) fraction, and thus decrease bilirubin accumulation in the brain., Methods: We treated chronic (e.g., as a model for Crigler-Najjar disease) and acute hemolytic (e.g., as a model for neonatal jaundice) moderate hyperbilirubinemic Gunn rats with phototherapy, human serum albumin (HSA) or phototherapy+HSA., Results: In the chronic model, adjunct HSA increased the efficacy of phototherapy; it decreased plasma UCB(free) and brain bilirubin by 88% and 67%, respectively (p<0.001). In the acute model, adjunct HSA also increased the efficacy of phototherapy; it decreased plasma UCB(free) by 76% (p<0.001) and completely prevented the hemolysis-induced deposition of bilirubin in the brain. Phototherapy alone failed to prevent the deposition of bilirubin in the brain during acute hemolytic jaundice., Conclusions: We showed that adjunct HSA treatment decreases brain bilirubin levels in phototherapy-treated Gunn rats. We hypothesize that HSA decreases these levels by lowering UCB(free) in the plasma. Our results support the feasibility of adjunct albumin treatment in patients with Crigler-Najjar disease or neonatal jaundice., (Copyright © 2012 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published

2013

11. Compound heterozygote of a novel missense mutation (p.K402T) and a double missense mutation (p.[G71R;Y486D]) in type II Crigler-Najjar syndrome.

Author

Maruo Y, Ozgenc F, Mimura Y, Ota Y, Matsui K, Takahashi H, Mori A, Taga T, Takano T, Sato H, and Takeuchi Y

Subjects

Crigler-Najjar Syndrome metabolism, DNA Mutational Analysis, Glucuronosyltransferase metabolism, Heterozygote, Humans, Infant, Male, Crigler-Najjar Syndrome genetics, Glucuronosyltransferase genetics, Mutation, Missense

Published

2011

12. Functional characterization of hepatocytes for cell transplantation: customized cell preparation for each receptor.

Author

Bonora-Centelles A, Donato MT, Lahoz A, Pareja E, Mir J, Castell JV, and Gómez-Lechón MJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Cell Separation methods, Cell Survival physiology, Cells, Cultured, Child, Child, Preschool, Cold Ischemia methods, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome physiopathology, Crigler-Najjar Syndrome surgery, Donor Selection methods, Donor Selection standards, Female, Glucuronosyltransferase analysis, Glucuronosyltransferase metabolism, Hepatocytes cytology, Humans, Infant, Infant, Newborn, Liver Diseases metabolism, Liver Diseases physiopathology, Male, Middle Aged, Receptors, Cell Surface analysis, Receptors, Cell Surface metabolism, Urea metabolism, Urea Cycle Disorders, Inborn metabolism, Urea Cycle Disorders, Inborn physiopathology, Urea Cycle Disorders, Inborn surgery, Young Adult, Biological Assay methods, Cell Transplantation methods, Graft Survival physiology, Hepatocytes metabolism, Hepatocytes transplantation, Liver Diseases surgery

Abstract

The first indication of hepatocyte transplantation is inborn liver-based metabolic disorders. Among these, urea cycle disorders leading to the impairment to detoxify ammonia and Crigler-Najjar Syndrome type I, a deficiency in the hepatic UDP-glucuronosyltransferase 1A1 present the highest incidence. Metabolically qualified human hepatocytes are required for clinical infusion. We proposed fast and sensitive procedures to determine their suitability for transplantation. For this purpose, viability, attachment efficiency, and metabolic functionality (ureogenic capability, cytochrome P450, and phase II activities) are assayed prior to clinical cell infusion to determine the quality of hepatocytes. Moreover, the evaluation of urea synthesis from ammonia and UDP-glucuronosyltransferase 1A1 activity, a newly developed assay using beta-estradiol as substrate, allows the possibility of customizing cell preparation for receptors with urea cycle disorders or Crigler-Najjar Syndrome type I. Sources of human liver and factors derived from the procurement of the liver sample (warm and cold ischemia) have also been investigated. The results show that grafts with a cold ischemia time exceeding 15 h and steatosis should not be accepted for hepatocyte transplantation. Finally, livers from non-heart-beating donors are apparently a potential suitable source of hepatocytes, which could enlarge the liver donor pool.

Published

2010

13. Towards liver-directed gene therapy for Crigler-Najjar syndrome.

Author

Miranda PS and Bosma PJ

Subjects

Animals, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Disease Models, Animal, Genetic Vectors genetics, Genetic Vectors metabolism, Humans, Liver Diseases therapy, Rats, Crigler-Najjar Syndrome therapy, Genetic Therapy methods

Abstract

Crigler-Najjar (CN) syndrome is a recessive inherited disorder caused by deficiency of uridine diphospho-glucuronosyl transferase 1A1. This hepatic enzyme catalyzes the glucuronidation of bilirubin, an essential step in excretion into bile of this neurotoxic compound. As a result, CN patients suffer from severe unconjugated hyperbilirubinemia and are at risk of bilirubin encephalopathy. Over the last decades ex vivo and in vivo gene therapy using viral and non-viral vectors has been used to correct hyperbilirubinemia in the relevant animal model for CN syndrome, the Gunn rat. Several of these approaches did result in long-term correction of serum bilirubin levels in this animal model. However, none have been translated into a clinical trial. In this review we will recapitulate the strategies used and discuss their suitability for clinical application in the near future. We will also address specific safety measures in the gene therapy protocol needed to prevent adverse effects such as bilirubin toxicity. Since CN seems an ideal model for other monogenetic inherited metabolic liver disorders, development of liver-directed gene-therapy has relevance beyond this rare disease.

Published

2009

14. I read with great interest the article by Hafkamp et al.

Author

Makay B

Subjects

Anti-Obesity Agents adverse effects, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Diarrhea chemically induced, Diarrhea metabolism, Enterohepatic Circulation, Feces chemistry, Humans, Lactones adverse effects, Lipid Metabolism drug effects, Orlistat, Treatment Outcome, Anti-Obesity Agents therapeutic use, Crigler-Najjar Syndrome drug therapy, Lactones therapeutic use

Published

2009

15. Small animal models of hepatocyte transplantation.

Author

Seppen J, Filali EE, and Elferink RO

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, Animal Feed, Animals, Bile metabolism, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome pathology, Crigler-Najjar Syndrome therapy, DNA-Binding Proteins genetics, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Hepatocytes metabolism, Hepatocytes pathology, Interleukin Receptor Common gamma Subunit genetics, Mice, Mice, Knockout, Rats, Rats, Gunn, ATP-Binding Cassette Sub-Family B Member 4, Hepatocytes transplantation, Liver Transplantation methods, Models, Animal

Abstract

In this chapter, we describe techniques used to determine the efficiency of hepatocyte transplantation in animal models of liver disease. We have included the Gunn rat as a model of an inherited liver disease without hepatocyte damage and Abcb4 knockout mice as a model for an inherited liver disease with hepatocyte damage. Immunodeficient mice are included as an animal model for human hepatocyte transplantation.We describe problems that can be encountered in the maintenance and breeding of Gunn rats and immunodeficient Rag2/gamma common knockout mice. Protocols for the collection of bile in rats and mice are described, and we have also detailed the detection of green fluorescent protein (GFP)-labelled human hepatocytes in immunodeficient mice in this chapter.

Published

2009

16. Orlistat treatment of unconjugated hyperbilirubinemia in Crigler-Najjar disease: a randomized controlled trial.

Author

Hafkamp AM, Nelisse-Haak R, Sinaasappel M, Oude Elferink RP, and Verkade HJ

Subjects

Adolescent, Adult, Anti-Obesity Agents adverse effects, Anti-Obesity Agents therapeutic use, Child, Combined Modality Therapy, Crigler-Najjar Syndrome blood, Crigler-Najjar Syndrome drug therapy, Crigler-Najjar Syndrome metabolism, Cross-Over Studies, Dietary Fats metabolism, Double-Blind Method, Drug Therapy, Combination, Eating, Feces chemistry, Female, Humans, Lactones adverse effects, Lipid Metabolism drug effects, Male, Middle Aged, Orlistat, Patient Compliance, Treatment Outcome, Bilirubin blood, Crigler-Najjar Syndrome therapy, Lactones therapeutic use, Phenobarbital therapeutic use, Phototherapy

Abstract

Unconjugated hyperbilirubinemia in Crigler-Najjar (CN) disease is conventionally treated with phototherapy and phenobarbital. Orlistat treatment increases fecal fat excretion and decreases plasma unconjugated bilirubin (UCB) concentrations in Gunn rats, the animal model for CN disease. We determined in CN patients the effects of orlistat treatment on plasma UCB concentrations, and on fecal excretion of fat and UCB. A randomized, placebo-controlled, double-blind, cross-over trial was conducted in 16 patients, simultaneous with their regular treatment (phototherapy, n = 11, and/or phenobarbital, n = 6). Patients received orlistat or placebo, each for 4-6 wk. Compared with placebo, orlistat increased fecal fat excretion (+333%) and fecal UCB excretion (+43%). Orlistat treatment significantly decreased plasma UCB concentration (-9%). In 7 of 16 patients, the decrease in plasma UCB levels was clinically relevant (>10%, mean 21%). In patients with a clinically relevant response, plasma UCB concentrations during orlistat were strongly, negatively correlated with fecal fat excretion (r = -0.93). Clinically relevant response to orlistat treatment was not correlated with age, sex, CN type, BMI, or co-treatment with phototherapy or phenobarbital, but appeared correlated with a relatively lower dietary fat intake. In conclusion, orlistat treatment decreases plasma UCB concentrations, particularly in a subgroup of CN patients. Dietary fat intake may determine the responsiveness to orlistat treatment.

Published

2007

17. Molecular cloning of the baboon UDP-glucuronosyltransferase 1A gene family: evolution of the primate UGT1 locus and relevance for models of human drug metabolism.

Author

Caspersen CS, Reznik B, Weldy PL, Abildskov KM, Stark RI, and Garland M

Subjects

Amino Acid Sequence, Animals, Base Sequence, Bilirubin metabolism, Cloning, Molecular, Conserved Sequence, Crigler-Najjar Syndrome enzymology, Crigler-Najjar Syndrome metabolism, Humans, Molecular Sequence Data, Phylogeny, Sequence Alignment, Evolution, Molecular, Glucuronosyltransferase genetics, Models, Animal, Multigene Family, Papio genetics, Pharmacogenetics

Abstract

Background: Glucuronidation by the UDP glucuronosyltransferase 1A enzymes (UGT1As) is a major pathway for elimination of drugs and endogenous substances, such as bilirubin., Objective: To identify the baboon UGT1A gene family, compare it with that of the human, and evaluate the baboon as a model for human glucuronidation., Methods and Results: Aligning the human and baboon UGT1 loci identified rearrangements occurring since the divergence of baboons and humans. The baboon UGT1A cDNAs were cloned and shown to have an orthologous relationship with several genes in the human UGT1A family. This indicates that most protein encoding UGT1A first exons were duplicated before the divergence of baboons and humans. Gene conversions interfered with the phylogenetic signal for exons 1A4, 1A5, and 1A10, and led to concerted evolution of exon groups 1A2-1A5 and 1A7-1A13. The activity of the baboon UGT1As resembled those of their human counterparts in glucuronidating endobiotics, such as serotonin, bilirubin, and various xenobiotics., Conclusion: These insights demonstrate that the baboon has significant clinical relevance as a model for examining toxicological metabolism in humans.

Published

2007

18. N-Glucuronidation of the antiepileptic drug retigabine: results from studies with human volunteers, heterologously expressed human UGTs, human liver, kidney, and liver microsomal membranes of Crigler-Najjar type II.

Author

Borlak J, Gasparic A, Locher M, Schupke H, and Hermann R

Subjects

Anticonvulsants metabolism, Anticonvulsants pharmacokinetics, Anticonvulsants urine, Carbamates urine, Carbon Isotopes pharmacokinetics, Cell Line, Chromatography, High Pressure Liquid, Crigler-Najjar Syndrome drug therapy, Drug Interactions, Humans, Kidney enzymology, Kinetics, Liver enzymology, Male, Mass Spectrometry, Microsomes enzymology, Monosaccharide Transport Proteins metabolism, Phenylenediamines urine, Carbamates metabolism, Carbamates pharmacokinetics, Crigler-Najjar Syndrome metabolism, Glucuronides metabolism, Phenylenediamines metabolism, Phenylenediamines pharmacokinetics

Abstract

Retigabine (D-23129), an N-2-amino-4-(4-fluorobenzylamino)phenylcarbamine acid ethyl ester, is a novel antiepileptic drug which is currently in phase II clinical development. This drug undergoes N-glucuronidation. We aimed to identify the principal enzymes involved in the N-glucuronidation pathway of retigabine and compared our findings with those obtained from human liver (a pool of 30 donors) and kidney microsomes (a pool of 3 donors) and with results from a human absorption, distribution, metabolism, and excretion study upon administration of 200 microCi of [(14)C]-D-23129. Essentially, microsomal assays with UGT1A1 produced only one of the 2 N-glucuronides, whereas UGT1A9 is capable of forming both N-glucuronides. The rates of metabolism for UGT1A9, human liver microsomes, and UGT1A1 were 200, 100, and 100 pmol N-glucuronide per minute per milligram of protein, respectively. At the 50 micromol/L uridine diphosphate glucoronic acid (UDPGA) concentration, UGT1A4 also catalyzed the N-glucuronidation of retigabine, the rates being approximately 5 and 6 pmol/(min.mg protein). With UGT1A9, the production of metabolites 1 and 2 proceeded at a K(m) of 38+/-25 and 45+/-15 micromol/L, whereas the K(m) for retigabine N-glucuronidation by human liver microsomal fractions was 145+/-39 micromol/L. Furthermore, a V(max) of 1.2+/-0.3 (nmol/[min.mg protein]) was estimated for human liver microsomes (4 individual donors). We investigated the potential for drug-drug interaction using the antiepileptic drugs valproic acid, lamotrigine, the tricyclic antidepressant imipramine, and the anesthetic propofol. These are commonly used medications and are extensively glucuronidated. No potential for drug-drug interactions was found at clinically relevant concentrations (when assayed with human liver microsomes or UGT1A9 enzyme preparations). Notably, the biosynthesis of retigabine-N-glucuronides was not inhibited in human liver microsomal assays in the presence of 330 micromol/L bilirubin, and glucuronidation of retigabine was also observed with microsomal preparations from human kidney and Crigler-Najjar type II liver. This suggests that lack of a particular UDP-glucuronosyltransferase (UGT) isoform (eg, UGT1A1 in kidney) or functional loss of an entire UGT1A gene does not completely abolish disposal of the drug. Finally, chromatographic separations of extracts from microsomal assays and human urine of volunteers receiving a single dose of (14)C-retigabine provided clear evidence for the presence of the 2 N-glucuronides known to be produced by UGT1A9. We therefore suggest N-glucuronidation of retigabine to be of importance in the metabolic clearance of this drug.

Published

2006

19. Nonviral gene transfer into liver and muscle for treatment of hyperbilirubinemia in the gunn rat.

Author

Dankó I, Jia Z, and Zhang G

Subjects

Alanine Transaminase blood, Animals, Bile metabolism, Bilirubin blood, Bilirubin metabolism, Blotting, Western, Chromatography, High Pressure Liquid, Creatine Kinase blood, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Disease Models, Animal, Gene Transfer Techniques, Glucuronosyltransferase deficiency, Humans, Liver metabolism, Muscle, Skeletal metabolism, Rats, Rats, Gunn, Rats, Sprague-Dawley, Rats, Wistar, Time Factors, Crigler-Najjar Syndrome therapy, Genetic Therapy, Glucuronosyltransferase genetics, Hyperbilirubinemia therapy, Liver enzymology, Muscle, Skeletal enzymology

Abstract

We evaluated naked plasmid DNA (pDNA)-mediated expression of human hepatic bilirubin UDP-glucuronosyltransferase (hUGT1A1) in skeletal muscle to correct hyperbilirubinemia in the UGT1A1-deficient Gunn rat, an animal model of Crigler-Najjar syndrome type I (CN-I). After delivery of pDNA encoding hUGT1A1 via hepatic vein or femoral artery, in vitro bilirubin glucuronidation activity was detectable in Gunn rat liver and muscle extracts. Expression of hUGT1A1 in Gunn rat liver or muscle resulted in excretion of bilirubin glucuronides in bile. Total biliary bilirubin concentrations increased from a pretreatment average of 10.5 +/- 2.1 microM to 29.2 +/- 4.2 microM after gene transfer into the liver, and to 28.6 +/- 3.8 microM after gene transfer into muscle. Total serum bilirubin decreased by up to 31.2 +/- 6.9 and 29.2 +/- 3.7% and remained significantly lower for at least 1 and 2 weeks, respectively. Tissue damage associated with the procedure was minimal and reversible. Our results demonstrate that muscle can be genetically modified to glucuronidate bilirubin, leading to elimination in bile. A 30% decrease in serum bilirubin, if sustained, would provide meaningful clinical benefit for CN-I patients. However, to be clinically useful, this method needs further optimization and stable gene expression must be achieved.

Published

2004

20. Rapid proteasomal degradation of translocation-deficient UDP-glucuronosyltransferase 1A1 proteins in patients with Crigler-Najjar type II.

Author

Ohnishi A and Emi Y

Subjects

Animals, Arginine chemistry, COS Cells, Cell Membrane metabolism, Endoplasmic Reticulum metabolism, Female, Glucuronosyltransferase chemistry, Glycoside Hydrolases metabolism, Humans, Leucine chemistry, Middle Aged, Mutation, Plasmids metabolism, Precipitin Tests, Protease Inhibitors pharmacology, Proteasome Endopeptidase Complex, Protein Sorting Signals, Protein Transport, Time Factors, Transfection, Trypsin pharmacology, Crigler-Najjar Syndrome metabolism, Cysteine Endopeptidases metabolism, Glucuronosyltransferase metabolism, Multienzyme Complexes metabolism

Abstract

UDP-glucuronosyltransferase form 1A1 (UGT1A1) is the only bilirubin-glucuronidating isoform of this protein, and genetic deficiencies of UGT1A1 cause Crigler-Najjar syndrome, a disorder resulting from nonhemolytic unconjugated hyperbilirubinemia. Here we have focused on the instability of a translocation-deficient UGT1A1 protein, which has been found in patients with Crigler-Najjar type II, to elucidate the molecular basis underlying the deficiency in glucuronidation of bilirubin. A substitution of leucine to arginine at position 15 (L15R/1A1) is predicted to disrupt the hydrophobic core of the signal peptide of UGT1A1. L15R/1A1 was synthesized in similar amounts to wild-type UGT1A1 protein (WT/1A1) in transfected COS cells. However, L15R/1A1 did not translocate across the endoplasmic reticulum membrane and was degraded rapidly with a half-life of about 50min, in contrast to the much longer half-life of about 12.8h for WT/1A1. Our findings demonstrate that L15R/1A1 was rapidly degraded by the proteasome owing to its mislocalization in the cell.

Published

2003

21. A novel strategy for in vivo expansion of transplanted hepatocytes using preparative hepatic irradiation and FasL-induced hepatocellular apoptosis.

Author

Takahashi M, Deb NJ, Kawashita Y, Lee SW, Furgueil J, Okuyama T, Roy-Chowdhury N, Vikram B, Roy-Chowdhury J, and Guha C

Subjects

Adenoviridae genetics, Animals, Apoptosis, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome pathology, Fas Ligand Protein, Genetic Vectors administration & dosage, Genetic Vectors genetics, Glucuronosyltransferase deficiency, Liver metabolism, Liver pathology, Liver radiation effects, Male, Membrane Glycoproteins genetics, Membrane Glycoproteins metabolism, Models, Animal, Rats, Rats, Gunn, Rats, Wistar, Transduction, Genetic methods, Crigler-Najjar Syndrome therapy, Genetic Therapy methods, Hepatocytes transplantation

Abstract

A strategy for inducing preferential proliferation of the engrafted hepatocytes over host liver cells should markedly increase the benefit of hepatocyte transplantation for the treatment of liver diseases and ex vivo gene therapy. We hypothesized that preparative hepatic irradiation (HIR) to inhibit host hepatocellular regeneration in combination with the mitotic stimulus of host hepatocellular apoptosis should permit repopulation of the liver by transplanted cells. To test this hypothesis, congeneic normal rat hepatocytes were transplanted into UDP-glucuronosyltransferase (UGT1A1)-deficient jaundiced Gunn rats (a model of Crigler-Najjar syndrome type I), following HIR and adenovirus-mediated FasL gene transfer. Progressive repopulation of the liver by engrafted UGT1A1-proficient hepatocytes over 5 months was demonstrated by the appearance of UGT1A1 protein and enzyme activity in the liver, biliary bilirubin glucuronides secretion, and long-term normalization of serum bilirubin levels. This is the first demonstration of massive hepatic repopulation by transplanted cells by HIR and FasL-induced controlled apoptosis of host liver cells.

Published

2003

22. Bile bilirubin pigment analysis in disorders of bilirubin metabolism in early infancy.

Author

Lee WS, McKiernan PJ, Beath SV, Preece MA, Baty D, Kelly DA, Burchell B, and Clarke DJ

Subjects

Bilirubin analysis, Chromatography, High Pressure Liquid, Crigler-Najjar Syndrome complications, Crigler-Najjar Syndrome metabolism, Diagnosis, Differential, Diagnostic Errors, Female, Genetic Testing, Gilbert Disease complications, Gilbert Disease diagnosis, Gilbert Disease metabolism, Humans, Hyperbilirubinemia diagnosis, Hyperbilirubinemia etiology, Hypnotics and Sedatives, Infant, Infant, Newborn, Male, Mutation, Phenobarbital, Predictive Value of Tests, Retrospective Studies, Bile Pigments analysis, Crigler-Najjar Syndrome diagnosis, Hyperbilirubinemia metabolism

Abstract

Background: Early and accurate diagnosis of Crigler-Najjar syndrome, which causes prolonged unconjugated hyperbilirubinaemia in infancy, is important, as orthotopic liver transplantation is the definitive treatment., Aim: To determine whether bilirubin pigment analysis of bile in infants with prolonged unconjugated hyperbilirubinaemia provides useful diagnostic information in the first 3 months of life., Methods: Retrospective review of patients with prolonged unconjugated hyperbilirubinaemia referred to the liver unit, Birmingham Children's Hospital, for the diagnosis of Crigler-Najjar syndrome. Bile bilirubin pigment composition was determined by high performance liquid chromatography. Initial diagnoses were made based on the result of bile bilirubin pigment composition. Final diagnoses were made after reviewing the clinical course, response to phenobarbitone, repeat bile bilirubin pigment composition analysis, and genetic studies., Results: Between 1992 and 1999, nine infants aged less than 3 months of age with prolonged hyperbilirubinaemia underwent bile bilirubin pigment analyses. Based on these, two children were diagnosed with Crigler-Najjar syndrome (CNS) type 1, six with CNS type 2, and one with Gilbert's syndrome. Five children whose initial diagnosis was CNS type 2 had resolution of jaundice and normalisation of serum bilirubin after discontinuing phenobarbitone, and these cases were thought to be normal or to have Gilbert's syndrome. One of the initial cases of CNS type 1 responded to phenobarbitone with an 80% reduction in serum bilirubin consistent with CNS type 2. In all, the diagnoses of six cases needed to be reviewed., Conclusions: Early bile pigment analysis, performed during the first 3 months of life, often shows high levels of unconjugated bilirubin or bilirubin monoconjugates, leading to the incorrect diagnosis of both type 1 and type 2 Crigler-Najjar syndrome.

Published

2001

23. Supplement of liver enzyme by intestinal and kidney transplants in congenitally enzyme-deficient rat.

Author

Kokudo N, Takahashi S, Sugitani K, Okazaki T, and Nozawa M

Subjects

Animals, Animals, Congenic, Bile chemistry, Bilirubin analysis, Crigler-Najjar Syndrome metabolism, Digestive System Surgical Procedures methods, Disease Models, Animal, Male, Rats, Rats, Gunn, Rats, Wistar, Time Factors, Glucuronosyltransferase deficiency, Intestine, Small enzymology, Intestine, Small transplantation, Kidney enzymology, Kidney Transplantation methods, Liver enzymology

Abstract

Gunn rats have a congenital deficiency of bilirubin-uridine diphosphate glucuronyltransferase (B-UDP-GT) activity and are unable to glucuronidate bilirubin in the bile, resulting in unconjugated hyperbilirubinemia. Other than the liver, several organs, including small bowel and kidneys, are known to have B-UDP-GT activity in normal rats. We performed total- or partial-small-bowel transplantation as well as kidney transplantation for Gunn rats in congenic combination and compared the effects of these procedures. Serum total bilirubin (TBil) levels significantly decreased from 7.84 +/- 0.24 mg/dl to 2.19 +/- 0.43 mg/dl 2 weeks after total-small-bowel transplantation (n = 12). Correlation of hyperbilirubinemia was roughly proportional to the length of the transplanted small bowel. There were no difference in metabolic correction between jejunal and ileal transplantation. Serum TBil levels significantly decreased from 7.83 +/- 0.21 mg/dl to 2.24 +/- 0.98 mg/dl 2 weeks after kidney transplantation (n = 5). In conclusion, small-bowel and kidney transplantation were effective in correcting metabolic abnormality in Gunn rats for the period of 4-6 months. Estimated total B-UDP-GT activity supplemented by small-bowel or kidney transplantation was about 1/5-1/4 of the minimal requirement for the complete normalization of serum total bilirubin levels.

Published

1999

24. Hepatocyte transplantation.

Author

Lake JR

Subjects

Bilirubin blood, Crigler-Najjar Syndrome metabolism, Glucuronosyltransferase metabolism, Humans, Cell Transplantation methods, Crigler-Najjar Syndrome therapy, Liver cytology

Published

1998

25. Genetic predisposition to the metabolism of irinotecan (CPT-11). Role of uridine diphosphate glucuronosyltransferase isoform 1A1 in the glucuronidation of its active metabolite (SN-38) in human liver microsomes.

Author

Iyer L, King CD, Whitington PF, Green MD, Roy SK, Tephly TR, Coffman BL, and Ratain MJ

Subjects

Animals, Bilirubin metabolism, Camptothecin metabolism, Causality, Crigler-Najjar Syndrome metabolism, Guanine analogs & derivatives, Guanine metabolism, Humans, Irinotecan, Isoenzymes genetics, Nitrophenols metabolism, Oxidation-Reduction, Rats, Rats, Sprague-Dawley, Zidovudine metabolism, Antineoplastic Agents, Phytogenic metabolism, Camptothecin analogs & derivatives, Glucuronosyltransferase genetics, Glucuronosyltransferase metabolism, Isoenzymes metabolism, Microsomes, Liver metabolism, Uridine Diphosphate

Abstract

Irinotecan (CPT-11) is a promising antitumor agent, recently approved for use in patients with metastatic colorectal cancer. Its active metabolite, SN-38, is glucuronidated by hepatic uridine diphosphate glucuronosyltransferases (UGTs). The major dose-limiting toxicity of irinotecan therapy is diarrhea, which is believed to be secondary to the biliary excretion of SN-38, the extent of which is determined by SN-38 glucuronidation. The purpose of this study was to identify the specific isoform of UGT involved in SN-38 glucuronidation. In vitro glucuronidation of SN-38 was screened in hepatic microsomes from normal rats (n = 4), normal humans (n = 25), Gunn rats (n = 3), and patients (n = 4) with Crigler-Najjar type I (CN-I) syndrome. A wide intersubject variability in in vitro SN-38 glucuronide formation rates was found in humans. Gunn rats and CN-I patients lacked SN-38 glucuronidating activity, indicating the role of UGT1 isoform in SN-38 glucuronidation. A significant correlation was observed between SN-38 and bilirubin glucuronidation (r = 0.89; P = 0.001), whereas there was a poor relationship between para-nitrophenol and SN-38 glucuronidation (r = 0.08; P = 0.703). Intact SN-38 glucuronidation was observed only in HK293 cells transfected with the UGT1A1 isozyme. These results demonstrate that UGT1A1 is the isoform responsible for SN-38 glucuronidation. These findings indicate a genetic predisposition to the metabolism of irinotecan, suggesting that patients with low UGT1A1 activity, such as those with Gilbert's syndrome, may be at an increased risk for irinotecan toxicity.

Published

1998

26. Complementation of the genetic defect in Gunn rat hepatocytes in vitro by highly efficient gene transfer with cationic liposomes.

Author

Wilke M, Bijma A, Timmers-Reker AJ, Scholte BJ, and Sinaasappel M

Subjects

Animals, Cations, Cells, Cultured, Crigler-Najjar Syndrome metabolism, Lac Operon, Liposomes, Plasmids, Rats, Rats, Gunn, Crigler-Najjar Syndrome therapy, Genetic Therapy methods, Liver metabolism, Transfection methods

Abstract

In this article, we report complementation of the genetic defect of isolated Gunn rat hepatocytes by a highly efficient method for lipofection. Transfections were performed 24 h after plating by using the cationic liposome DOTAP. On average, transfection efficiencies of 21% lacZ+ cells with Wag/Rij rat cells and 27% lacZ+ cells with Gunn rat cells could be obtained when the parenchymal cells were transfected in a hormone-defined, serum-free medium. LacZ expression vectors with the CMV promoter were more effective than constructs containing the RSV or the TK promoter. A linear relationship between the viability of hepatocytes after isolation and the percentage of lacZ+ cells was observed with both rat strains, with a maximum of 40% lacZ+ cells at a viability of 94%. The transfection efficiencies were significantly lower in the absence of growth factors, in dexamethasone-containing medium, or when serum was present during plating. Our data are consistent with the assumption that a mitotic event is required for efficient lipofection. Bilirubin conjugation activity could be detected in microsomes from Gunn rat hepatocytes after transfection with two different B-UDPGT expression constructs. Highest conjugation activity was achieved with a vector containing a terminal intron. With this construct on average 4% of the bilirubin conjugation activity of normal human liver microsomes could be achieved in total microsomes of transfected Gunn rat hepatocytes. The implications of our data for gene therapy of hepatic disease with nonviral vectors, in particular bilirubin conjugation deficiency (Crigler-Najjar disease) are discussed.

Published

1997

27. [Constitutional jaundice].

Author

Adachi Y and Kamisako T

Subjects

Crigler-Najjar Syndrome metabolism, Gilbert Disease metabolism, Humans, Jaundice, Chronic Idiopathic metabolism, Hyperbilirubinemia metabolism

Published

1997

28. The glucuronidation of exogenous and endogenous compounds by stably expressed rat and human UDP-glucuronosyltransferase 1.1.

Author

King CD, Green MD, Rios GR, Coffman BL, Owens IS, Bishop WP, and Tephly TR

Subjects

Animals, Bilirubin metabolism, Buprenorphine metabolism, Cell Line, Crigler-Najjar Syndrome metabolism, Glucuronates metabolism, Glucuronosyltransferase deficiency, Glucuronosyltransferase genetics, Humans, In Vitro Techniques, Kinetics, Liver metabolism, Molecular Structure, Nalorphine metabolism, Naltrexone metabolism, Narcotics chemistry, Narcotics metabolism, Rats, Recombinant Proteins genetics, Recombinant Proteins metabolism, Species Specificity, Substrate Specificity, Transfection, Xenobiotics chemistry, Xenobiotics metabolism, Glucuronosyltransferase metabolism

Abstract

Rat and human UDP-glucuronosyltransferase (UGT) 1.1 share > 70% identity in their deduced primary amino acid sequences. We have previously shown that rat UGT1.1, stably expressed in human embryonic kidney 293 cells, catalyzes the glucuronidation of bilirubin and the mixed opioid agonist/antagonist buprenorphine with high efficiency. The present study was designed to characterize the reactivity of expressed human UGT1.1 with opioid compounds and compare its substrate specificity for opioids to that of the expressed rat enzyme. The results show that both rat and human UGT1.1 catalyze the glucuronidation of opioids with a relative reactivity of buprenorphine > > nalorphine approximately naltrexone. Comparison of glucuronidation activities in livers from Crigler-Najjar type 1 patients and normal patients indicates that UGT1.1 catalyzes at least 75% of buprenorphine conjugation in normal human liver. In separate studies, the reactivity of expressed rat UGT1.1 was characterized toward various xeno-and endobiotics of various compound classes. It was found that both rat and human UGT1.1 exhibited comparable substrate specificities and efficiencies (Vmax/Km) of glucuronide formation for anthraquinones, coumarins, estrogens, flavonoids, and phenolic compounds. Neither rat nor human UGT1.1 catalyzed the glucuronidation of amines, monoterpenoid alcohols, androgens, or progestins. In general, these data indicate that rat and human UGT1.1 are functionally identical and can be considered orthologous enzymes.

Published

1996

29. Complete correction of hyperbilirubinemia in the Gunn rat model of Crigler-Najjar syndrome type I following transient in vivo adenovirus-mediated expression of human bilirubin UDP-glucuronosyltransferase.

Author

Askari FK, Hitomi Y, Mao M, and Wilson JM

Subjects

Adenoviridae, Animals, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Gene Expression, Gene Transfer Techniques, Genetic Vectors, Glucuronosyltransferase deficiency, Humans, In Situ Hybridization, Rats, Rats, Gunn, Bilirubin metabolism, Crigler-Najjar Syndrome therapy, Genetic Therapy, Glucuronosyltransferase genetics, Hyperbilirubinemia therapy

Abstract

Recombinant adenoviral vectors are useful for the in vivo expression of genes in hepatocytes. Adenoviral vectors deleted in E1a, E1b, and E3b were constructed and used to study in vivo expression of the major human bilirubin UDP-glucuronosyltransferase isoform (HUG Br1) under the transcriptional control of the cytomegalovirus (CMV) immediate-early promoter-enhancer (H5.010CMV hugBr1). As a control, a recombinant adenoviral vector containing the beta-galactosidase reporter gene driven by the CMV promoter-enhancer was employed (H5. 010CMVlacZ). Recombinant virus was expanded following exposure to E1 transcomplementing (293) cells and concentrated to t titer of approximately 10(13) particles per milliliter. A rat model for Crigler-Najjar syndrome type I deficient in HUG Br1 (ie the Gunn rat) was injected with 5 X 10(9) plaque-forming units (p.f.u.) via the portal vein of either H5.010CMVhugBr1 or H5. 010CMVlacZ. Rats from each set were killed at 3 days, 11 days and 22 days after infusion. Liver total cellular DNA, RNA and protein were analyzed for the transgene and the transgene product at the specified times. Analysis of livers by Southern blot hybridization demonstrates sequence-specific hybridization to adenoviral vector DNA, and Northern blot hybridization demonstrates sequence-specific hybridization to transgene-derived RNA. DNA levels peak at approximately one copy number at 3 days and decline over 22 days. RNA and Western blot analyses demonstrate overexpression of message and protein at 3 days, declining over 22 days. In virto functional assay for bilirubin glucuronosyl-transferase activity demonstrates overexpression of bilirubin UDP-glucurosyltransferase function. In situ hybridization of frozen sections to detect expressed mRNA using beta-galactosidasederived 35S-labeled riboprobes demonstrates adenovirus-derived transgene expression in hepatocytes. Significant drops in serum bilirubin levels were noted following expression of HUG Br1 but not beta-galactosidase. The drop in serum bilirubin correlates with the appearance of bilirubin glucuronides in bile. In summary, recombinant adenoviral vectors were used to demonstrate in vivo complementation of the genetic defect in Gunn rat livers with the HUG Br1 cDNA leading to a resolution of hyperbilirubinemia lasting approximately 7 weeks. These studies suggest that delivery of the HUG Br1 cDNA might provide a reasonable therapeutic benefit for Crigler-Najjar syndrome type I patients, as safe and efficacious gene delivery systems are developed.

Published

1996

30. Glucuronidation of diflunisal, (-)-morphine, 4-nitrophenol, and propofol in liver microsomes of two patients with Crigler-Najjar syndrome type I.

Author

Brunelle FM, Raoof AA, de ville de Goyet J, and Verbeeck RK

Subjects

Analgesics, Opioid metabolism, Anesthetics, Intravenous metabolism, Anti-Inflammatory Agents, Non-Steroidal metabolism, Child, Preschool, Crigler-Najjar Syndrome enzymology, Cytochrome P-450 Enzyme System metabolism, Diflunisal metabolism, Female, Glucuronosyltransferase metabolism, Humans, In Vitro Techniques, Male, Microsomes, Liver enzymology, Morphine metabolism, Nitrophenols metabolism, Propofol metabolism, Crigler-Najjar Syndrome metabolism, Glucuronates metabolism, Microsomes, Liver metabolism

Abstract

In vitro glucuronidation was studied in liver microsomes from two patients with Crigler-Najjar type I (CN-I) disease and compared with the activity measured in microsomes prepared from six control human livers. The UDP-glucuronosyltransferase (UGT) activity was determined toward the following substrates: 4-nitrophenol, propofol, (-)-morphine (formation of the 3-glucuronide), and diflunisal (formation of the phenolic and acyl glucuronides). Glucuronidation of 4-nitrophenol was reduced in one of the CN-I livers (CN-I No. 1) (0.9 nmol min(-1)mg(-1)) and normal in the other CN-I liver (CN-I No. 2) (3.5 nmol min(-1) mg(-l)) compared to the control livers (5.6 +/- 29 nmol min(-1) mg(-1)), mean +/- S.D.). Propofol glucuronidation was not detectable (i.e. less than 0.100 nmol min(-l) mg(-1) in the CN-I No. 1 liver and normal in the CN-I No. 2 liver (1.78 nmol min(-1) mg(-1) against 1.52 +/ 0.72 nmol min(-l) mg(-) in the control livers). The glucuronidation of (-)-morphine to the 3-glucuronide and the formation of the phenolic and acyl glucuronides of diflunisal were normal in both CN-I livers compared to the control livers. Our results show that CN-I patients are heterogeneous regarding UGT activity toward the phenolic substances 4-nitrophenol and propofol.

Published

1996

31. [Crigler-Najjar syndrome (types I and II)].

Author

Tazuma S, Yamashita G, Nakanishi T, and Kajiyama G

Subjects

Humans, Crigler-Najjar Syndrome metabolism

Published

1995

32. Molecular biology of bilirubin metabolism.

Author

Jansen PL, Bosma PJ, and Chowdhury JR

Subjects

Animals, Cloning, Molecular, Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome therapy, DNA, Complementary genetics, Disease Models, Animal, Genetic Therapy, Glucuronosyltransferase chemistry, Glucuronosyltransferase genetics, Glucuronosyltransferase metabolism, Humans, Liver metabolism, Liver Transplantation, Models, Biological, Molecular Biology, Mutation, Rats, Rats, Gunn, Bilirubin metabolism

Abstract

As the genes encoding the glucuronidating enzymes are discovered, it is evident that glucuronidation is a magnificent example of how in evolution, man became adapted to his "intoxicating" environment. A superfamily of genes is necessary to dispose of the toxins and carcinogens that are encountered by inhalation and ingestion. The enzymes that glucuronidate endogenous compounds are members of this large family. For the clinician, it is important to remember that jaundice may sometimes be the result of interactions at the level of bilirubin glucuronidation. When jaundice results from inactivation of members of the UGT1 family, conjugation of certain phenols, such as the anesthetic propofol, or synthetic estrogens, such as ethinylestradiol, can also be impaired. In the case of severe bilirubin glucuronidation deficiencies, such as the Crigler Najjar syndrome type I, there are exciting prospects for a possible cure by gene therapy.

Published

1995

33. The familial unconjugated hyperbilirubinemias.

Subjects

Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome pathology, Crigler-Najjar Syndrome therapy, Gilbert Disease genetics, Gilbert Disease metabolism, Gilbert Disease pathology, Gilbert Disease therapy, Humans, Prognosis, Hyperbilirubinemia, Hereditary genetics, Hyperbilirubinemia, Hereditary metabolism, Hyperbilirubinemia, Hereditary pathology, Hyperbilirubinemia, Hereditary therapy

Published

1994

34. Serum and bile bilirubin pigments in the differential diagnosis of Crigler-Najjar disease.

Author

Rubaltelli FF, Novello A, Zancan L, Vilei MT, and Muraca M

Subjects

Administration, Oral, Chromatography, High Pressure Liquid, Crigler-Najjar Syndrome classification, Crigler-Najjar Syndrome drug therapy, Crigler-Najjar Syndrome metabolism, Diagnosis, Differential, Female, Humans, Infant, Infant, Newborn, Male, Phenobarbital therapeutic use, Bile chemistry, Bile Pigments analysis, Bilirubin analysis, Crigler-Najjar Syndrome diagnosis

Abstract

Objective: To differentiate between Crigler-Najjar (CN) disease types 1 and 2., Design: The patterns of serum bilirubins, bile pigment composition, and phenobarbital response were studied., Patients: Three infants, affected by high serum unconjugated bilirubin concentrations, previously classified as type 1 CN., Methods: Serum and bile bilirubin pigment composition, both before and after phenobarbital (PB) treatment, were determined by alkaline methanolysis and high-pressure liquid chromatography. PB was given for at least 3 weeks by oral administration (5 mg/kg bw per day)., Results: No diconjugated bilirubin was found either before or after PB treatment in the serum of the three studied infants. In two patients traces of monoconjugated bilirubin were detected before PB therapy, and the ratio of conjugated/total bilirubin (percent) was increased by the PB response. In the third patient, traces of monoconjugated bilirubin appeared only after PB administration. However, the serum unconjugated bilirubin concentration decreased significantly only in the second patient, following the second cycle of PB treatment, leading to the diagnosis of type 2 CN. The analysis of the methyl ester derivatives of bile pigments was also performed on bile samples obtained in two patients by Entero-Test (R) both before and after PB treatment. An absolute increment in monoesterified bilirubin concentration was found after PB administration, although the percent concentration increased in one case and decreased in the other. No diesterified bilirubin was detected in the bile samples., Conclusions: The present results show that in types 1 and 2 CN disease it is possible to detect traces of monoconjugated but not diconjugated bilirubin both in serum and in bile. Whereas PB treatment is effective in slightly increasing the serum monoconjugated bilirubin concentration even in type 1 CN disease, the diagnosis of type 1 or 2 is based on finding a substantial decrease of serum unconjugated bilirubin following PB administration.

Published

1994

35. [Congenital diseases of bilirubin metabolism].

Author

Sinaasappel M

Subjects

Adolescent, Biological Transport, Child, Child, Preschool, Crigler-Najjar Syndrome metabolism, Gilbert Disease metabolism, Humans, Hyperbilirubinemia, Hereditary metabolism, Infant, Jaundice, Chronic Idiopathic metabolism, Bilirubin metabolism, Metabolism, Inborn Errors metabolism

Abstract

The metabolism of bilirubin is a complicated process. Recently the genetic background of the conjugation of bilirubin is uncovered but the mechanism of bilirubin excretion in the liver and gut, and its toxic effects in the brain are largely unknown. The congenital defects in the bilirubin metabolism exists of four rare and one common disease. The clinical implications of these diseases vary but some are of great impact for the patient. The chronic character of these diseases requires an accurate management. It is to be expected that in the future new therapeutic strategies will be developed.

Published

1993

36. Unveiling the mysteries of inherited disorders of bilirubin glucuronidation.

Author

Chowdury JR and Chowdury NR

Subjects

Crigler-Najjar Syndrome metabolism, Gilbert Disease genetics, Glucuronosyltransferase deficiency, Humans, Bilirubin metabolism, Crigler-Najjar Syndrome genetics, Glucuronates metabolism, Glucuronosyltransferase genetics

Published

1993

37. [A case of Crigler-Najjar syndrome of type II].

Author

Mori Y, Kimura H, Suehiro K, Naritomi Y, Maeda Y, Kusaba T, and Ishibashi D

Subjects

Adolescent, Bilirubin blood, Crigler-Najjar Syndrome drug therapy, Crigler-Najjar Syndrome metabolism, Glucuronosyltransferase metabolism, Humans, Liver enzymology, Male, Phenobarbital therapeutic use, Crigler-Najjar Syndrome diagnosis

Published

1991

38. Tin-protoporphyrin in the management of children with Crigler-Najjar disease.

Author

McDonagh AF

Subjects

Crigler-Najjar Syndrome metabolism, Drug Evaluation, Humans, Infant, Newborn, Metalloporphyrins adverse effects, Metalloporphyrins pharmacokinetics, Photosensitivity Disorders chemically induced, Protoporphyrins adverse effects, Protoporphyrins pharmacokinetics, Crigler-Najjar Syndrome drug therapy, Hyperbilirubinemia, Hereditary drug therapy, Metalloporphyrins therapeutic use, Porphyrins therapeutic use, Protoporphyrins therapeutic use

Published

1990

39. New insights into the classification and mechanisms of hereditary, chronic, non-haemolytic hyperbilirubinaemias.

Author

Berthelot P and Dhumeaux D

Subjects

Bilirubin metabolism, Chronic Disease, Coproporphyrins urine, Crigler-Najjar Syndrome etiology, Crigler-Najjar Syndrome metabolism, Female, Gilbert Disease diagnosis, Gilbert Disease metabolism, Glucuronosyltransferase metabolism, Humans, Hyperbilirubinemia, Hereditary metabolism, Jaundice, Chronic Idiopathic etiology, Jaundice, Chronic Idiopathic metabolism, Liver metabolism, Male, Sulfobromophthalein metabolism, Hyperbilirubinemia, Hereditary classification

Abstract

Gilbert's syndrome is typically associated with a deficiency in hepatic bilirubin UDP-glucuronosyltransferase activity (B-GTA). The overproduction of bilirubin that is often found in this condition could be a fortuitous coincidence that leads to the unmasking of the disease, which otherwise often remains latent. Some cases of chronic unconjugated hyperbilirubinaemia could, however, be related to a defect in hepatic uptake, as reflected by alterations in BSP kinetics. Severe deficiencies of hepatic B-GTA exist in all types of Crigler-Najjar disease. An increased proportion of bilirubin monoglucuronide is always found in bile when a B-GTA deficiency is present. This observation strongly suggests a common biochemical defect in Gilbert's syndrome and in Crigler-Najjar disease, and thus renders the suggestion that the latter condition may be separated into two groups somewhat inappropriate. There is, however, no doubt that further knowledge of the conjugating enzyme, or enzymes, is required: such information may lead to the characterisation of several types of enzymic defects. Whereas little is new as far as the Dubin-Johnson syndrome is concerned, Rotor's syndrome can no longer be considered to be a variant of the former. The transport defect which is involved in most cases of Rotor's syndrome, if not in all, is an impairment of hepatic storage, thus distinguishing it from the impairment of excretion which is involved in the Dubin-Johnson syndrome. The distinct patterns of urinary coproporphyrin excretion, which were recently reported in Dubin-Johnson and Rotor's syndromes, offer additional evidence for a clear differentiation between these two entities.

Published

1978

40. [The conjugation of bilirubin: clinico-experimental studies].

Author

Fevery J

Subjects

Animals, Bile Pigments analysis, Chromatography, Thin Layer, Crigler-Najjar Syndrome metabolism, Erythropoiesis, Gilbert Disease metabolism, Glucuronates metabolism, Hemolysis, Humans, Hyperbilirubinemia metabolism, Hyperbilirubinemia, Hereditary, Infant, Newborn, Kidney metabolism, Liver Diseases metabolism, Microsomes, Liver enzymology, Pyrroles analysis, Tetrapyrroles, Bilirubin metabolism, Liver metabolism

Published

1980

41. Unconjugated bilirubin and an increased proportion of bilirubin monoconjugates in the bile of patients with Gilbert's syndrome and Crigler-Najjar disease.

Author

Fevery J, Blanckaert N, Heirwegh KP, Préaux AM, and Berthelot P

Subjects

Adolescent, Adult, Azo Compounds metabolism, Bile analysis, Bile Pigments analysis, Bilirubin analysis, Biotransformation, Child, Preschool, Female, Glucuronosyltransferase metabolism, Humans, Infant, Liver enzymology, Male, Middle Aged, Pyrroles analysis, Bile metabolism, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Gilbert Disease metabolism, Hyperbilirubinemia, Hereditary metabolism

Abstract

Bilirubin pigments were studied in the bile of 20 normal adults, 25 patients with Gilbert's syndrome, 9 children with Crigler-Najjar disease, and 6 patients with hemolysis, to determine how a deficiency of hepatic bilirubin UDP-glucuronosyltransferase would affect the end products of bilirubin biotransformation. In the bile from patients with Gilbert's syndrome, a striking increase was found in the proportion of bilirubin monoconjugates (48.6+/-9.8% of total conjugates) relative to that in normal bile (27.2+/-7.8%). This increase was even more pronounced in children with Crigler-Najjar disease, in whom, even in the most severe cases, glucuronide could always be demonstrated in the bile. Furthermore, unconjugated bilirubin-IXalpha was unquestionably present in the bile of these children and amounted to 30-57% of their total bilirubin pigments (<1% in the controls). It was not possible to predict from the biliary bilirubin composition whether a child would respond to phenobarbital therapy or not. Bile composition was normal in patients with hemolysis, except when there was associated deficiency of hepatic glucuronosyltransferase. Therefore, the observed alterations were not a simple consequence of unconjugated hyperbilirubinemia. The present findings suggest that Crigler-Najjar disease represents a more pronounced expression than Gilbert's syndrome of a common biochemical defect. Hepatic bilirubin UDP-glucuronosyltransferase deficiency leads to decreased formation of diconjugates with an ensuing increase in the proportion of bilirubin monoconjugates in bile; in the most severe cases, an elevated content of biliary unconjugated bilirubin is also found.

Published

1977

42. Bilirubin metabolism.

Author

Spivak W

Subjects

Bilirubin blood, Biological Transport, Crigler-Najjar Syndrome metabolism, Crigler-Najjar Syndrome therapy, Gilbert Disease metabolism, Gilbert Disease therapy, Glucuronosyltransferase metabolism, Heme metabolism, Humans, Hyperbilirubinemia, Hereditary metabolism, Hyperbilirubinemia, Hereditary therapy, Infant, Newborn, Jaundice, Neonatal metabolism, Jaundice, Neonatal therapy, Liver metabolism, Milk, Human metabolism, Phototherapy, Bilirubin metabolism

Published

1985

43. Tin-protoporphyrin in the management of children with Crigler-Najjar disease.

Author

Rubaltelli FF, Guerrini P, Reddi E, and Jori G

Subjects

Crigler-Najjar Syndrome genetics, Crigler-Najjar Syndrome metabolism, Female, Humans, Infant, Newborn, Metalloporphyrins pharmacokinetics, Pedigree, Protoporphyrins pharmacokinetics, Crigler-Najjar Syndrome drug therapy, Hyperbilirubinemia, Hereditary drug therapy, Metalloporphyrins therapeutic use, Porphyrins therapeutic use, Protoporphyrins therapeutic use

Published

1989

44. [Binding of bilirubin to serum albumin in Crigler-Najjar syndrome, type I].

Author

Ihara H, Aoki Y, Aoki T, and Toyoda M

Subjects

Bilirubin analysis, Child, Crigler-Najjar Syndrome complications, Humans, Infant, Newborn, Male, Nervous System Diseases etiology, Protein Binding, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Hyperbilirubinemia, Hereditary metabolism, Serum Albumin metabolism

Published

1986

45. Characteristics of a photoproduct of bilirubin found in vitro and in vivo, and its effect on the bilirubin binding affinity of serum.

Author

Kapitulnik J, Kaufmann NA, Alayoff A, and Blondheim SH

Subjects

Albumins metabolism, Charcoal, Crigler-Najjar Syndrome metabolism, Humans, In Vitro Techniques, Infant, Newborn, Jaundice, Neonatal metabolism, Jaundice, Neonatal therapy, Phototherapy, Protein Binding drug effects, Bilirubin metabolism, Pigments, Biological pharmacology

Abstract

The 430 pigment isolated from bilirubin-albumin solutions illuminated in vitro, decreased the bilirubin binding affinity of serum. This effect was demonstrated for both tightly and loosely bound bilirubin in serum, but in albumin solutions pretreated with charcoal only the binding of loosely bound bilirubin was decreased. This finding is of importance because a similar pigment has been isolated from the body fluids of an infant with Crigler-Najjar syndrome. The production and accumulation of 430 pigment during phototherapy might decrease the binding of bilirubin to albumin in the circulation.

Published

1976

46. Mechanisms and significance of fasting and dietary hyperbilirubinemia.

Author

Whitmer DI and Gollan JL

Subjects

Adult, Animals, Bilirubin biosynthesis, Bilirubin blood, Crigler-Najjar Syndrome blood, Crigler-Najjar Syndrome metabolism, Diagnosis, Differential, Energy Intake, Gilbert Disease blood, Gilbert Disease diagnosis, Humans, Infant, Newborn, Jaundice etiology, Kinetics, Liver metabolism, Liver Diseases blood, Liver Diseases diagnosis, Rats, Rats, Gunn, Bilirubin metabolism, Fasting, Gilbert Disease metabolism, Hyperbilirubinemia metabolism, Hyperbilirubinemia, Hereditary metabolism

Published

1983

47. Formation and elimination of bilirubin.

Author

Bissell DM

Subjects

Animals, Bilirubin biosynthesis, Crigler-Najjar Syndrome metabolism, Diagnosis, Differential, Gilbert Disease metabolism, Half-Life, Heme metabolism, Hemeproteins metabolism, Hemoglobins metabolism, Hemopexin metabolism, Humans, Hyperbilirubinemia metabolism, Jaundice, Chronic Idiopathic diagnosis, Kinetics, Liver metabolism, Methemoglobin metabolism, Microsomes metabolism, Bilirubin metabolism

Published

1975

48. Bilirubin secretion and conjujation in the Crigler-Najjar syndrome type II.

Author

Gordon ER, Shaffer EA, and Sass-Kortsak A

Subjects

Adolescent, Bile metabolism, Bile Pigments metabolism, Chromatography, Thin Layer, Crigler-Najjar Syndrome diagnosis, Diagnosis, Differential, Duodenum metabolism, Humans, Male, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Hyperbilirubinemia, Hereditary metabolism

Abstract

Features characteristic of the Crigler-Najjar syndrome (type II) are described in an adolescent boy with severe congenital unconjugated hyperbilirubinemia. Bilirubin encephalopathy developed only in early puberty after surgery and fasting, coincident with a dramatic rise in serum bilirubin, which responded to intensive therapy. Fasting was later shown to increase markedly the serum bilirubin levels and probably was a major factor in precipitating the initial acute event. One year later, while the patient was in a metabolic steady state, the secretion rate of bilirubin was measured by aduodenal marker-perfusion technique, and the nature of the secreted bilirubin conjugates was characterized. Total bilirubin secretion rates were low, 4.39 mg per hr and 4.44 mg per hr on two separate studies. The major pigment detected in bile was bilirubin monoglucuronide. Bilirubin diglucuronide comprised only a minor fraction of the pigments, and other conjugates were not detected. The present study documents a reduced biliary bilirubin secretion and suggests that the addition of the second glucuronic acid moiety to the bilirubin molecule may be defective in Crigler-Najjar syndrome (type II).

Published

1976

49. The effect of repeated phlebotomy on bilirubin turnover, bilirubin clearance and unconjugated hyperbilirubinaemia in the Crigler-Najjar syndrome and the jaundiced Gunn rat: application of computers to experimental design.

Author

Berk PD, Scharschmidt BF, Waggoner JG, and White SC

Subjects

Adult, Animals, Bilirubin blood, Computers, Disease Models, Animal, Erythrocyte Aging, Erythrocytes metabolism, Female, Humans, Kinetics, Liver metabolism, Mathematics, Models, Biological, Rats, Bilirubin metabolism, Crigler-Najjar Syndrome metabolism, Hyperbilirubinemia metabolism, Hyperbilirubinemia, Hereditary metabolism, Jaundice metabolism, Veins physiology

Abstract

1. A multicompartmental model of erythrokinetics and bilirubin production has been developed to predict the consequences of chronic phlebotomy on daily bilirubin turnover. 2. Control values for four physiological variables including bilirubin turnover were determined in a 20-year-old woman with type I congenital nonhaemolytic jaundice (Crigler-Najjar syndrome). With these base-line data, the model predicted the following changes during phlebotomy: a 34% fall in bilirubin turnover; a 240% increase in the haemoglobin content of bone-marrow erythroid precursors; a 25% fall in the half-life of 51Cr-labelled erythrocytes; a characteristic alteration of the erythrocyte survival curve after labelling with [2-14C]glycine. 3. On the assumption, previously validated in normal volunteer subjects and patients with Gilbert's syndrome, that hepatic bilirubin clearance was independent of turnover and would therefore remain unchanged, a fall in plasma unconjugated bilirubin concentration during phlebotomy from 436 to 282 mumol/1 was expected. 4. Accordingly, the patient underwent phlebotomy 350 ml/week for 2 months, and 500 ml/week during an additional 3 months. Appropriate studies during phlebotomy confirmed each of the predictions in paragraph 2 above. In particular, turnover fell by 31%. Unexpectedly, plasma unconjugated bilirubin remained essentially unchanged. Analogous results were observed in phlebotomized jaundiced Gunn rats. 5. Kinetic studies in both the patient and the rats demonstrated that the failure of plasma unconjugated bilirubin to fall in parallel with bilirubin turnover resulted from a prolongation of the terminal half-life of radioactively labelled bilirubin and a fall in bilirubin clearance in every instance. 6. These studies indicate that (a) in congenital non-haemolytic jaundice, bilirubin clearance is uniquely influenced by bilirubin turnover and (b) compartmental modelling and kinetic studies are useful for predicting and interpreting the results of both physiological experiments and experimental therapeutic regimens.

Published

1976

50. Bilirubin metabolism and congenital jaundice.

Author

Gollan JL and Knapp AB

Subjects

Adult, Biological Transport, Crigler-Najjar Syndrome metabolism, Gilbert Disease metabolism, Humans, Hyperbilirubinemia metabolism, Hyperbilirubinemia, Hereditary metabolism, Infant, Newborn, Jaundice metabolism, Jaundice, Neonatal therapy, Liver metabolism, Phototherapy, Bilirubin metabolism, Jaundice congenital

Published

1985