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2. Improvement of cholestatic episodes in patients with benign recurrent intrahepatic cholestasis (BRIC) treated with rifampicin. A long-term follow-up.

Author

Helgadottir, Holmfridur, Folvik, Geir, and Vesterhus, Mette

Subjects
*RIFAMPIN, *CHOLESTASIS, *CHOLANGITIS, *ALKALINE phosphatase
Abstract

Patients with benign recurrent intrahepatic cholestasis (BRIC) suffer from recurrent episodes of cholestatic jaundice. Treatment options remain limited and are mainly symptomatic. In case reports rifampicin, plasmapheresis, and nasobiliary drainage have been reported to be effective. In this case series, we present long-term experience indicating disease-modifying effects of non-invasive treatment with rifampicin for recurrent cholestasis in BRIC type 1 (BRIC1). We included all adult BRIC1 patients diagnosed and followed up at a single centre in Bergen, Norway. Data regarding clinical and biochemical features during BRIC attacks with and without rifampicin treatment were retrieved from medical journals and a data registry. Five males with BRIC1 were included. Median age at diagnosis was 22 years (range 15–41). Together they had suffered from 65 cholestatic attacks (including four documented abortive attacks). Twenty-eight attacks were treated with rifampicin alone over the last 12 years; all cases showed symptomatic relief and reduction in the levels of bilirubin and alkaline phosphatase in blood. The attacks treated with rifampicin seemed to have shorter duration and were less likely to result in complications or hospitalization compared to attacks prior to the introduction of rifampicin. No side effects attributable to rifampicin were noted. Episodic treatment of recurrent BRIC1 attacks with rifampicin seems to ameliorate severity and shorten the duration of attacks. Timely diagnosis and effective treatment are of major importance in BRIC, not only to decrease complications but also improving patients' quality of life. [ABSTRACT FROM AUTHOR]

Published
2023
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3. Ivacaftor-Mediated Potentiation of ABCB4 Missense Mutations Affecting Critical Motifs of the NBDs: Repositioning Perspectives for Hepatobiliary Diseases.

Author

Delaunay, Jean-Louis, Elbahnsi, Ahmad, Bruneau, Alix, Madry, Claire, Durand-Schneider, Anne-Marie, Stary, Anne, Housset, Chantal, Gautheron, Jérémie, Callebaut, Isabelle, and Aït-Slimane, Tounsia

Subjects
*MISSENSE mutation, *ATP-binding cassette transporters, *BILIOUS diseases & biliousness, *LIVER transplantation, *CYSTIC fibrosis transmembrane conductance regulator, *LECITHIN
Abstract

ABCB4 (ATP-binding cassette subfamily B member 4) is a hepatocanalicular floppase involved in biliary phosphatidylcholine (PC) secretion. Variations in the ABCB4 gene give rise to several biliary diseases, including progressive familial intrahepatic cholestasis type 3 (PFIC3), an autosomal recessive disease that can be lethal in the absence of liver transplantation. In this study, we investigated the effect and potential rescue of ten ABCB4 missense variations in NBD1:NBD2 homologous positions (Y403H/Y1043H, K435M/K1075M, E558K/E1200A, D564G/D1206G and H589Y/H1231Y) all localized at the conserved and functionally critical motifs of ABC transporters, six of which are mutated in patients. By combining structure analysis and in vitro studies, we found that all ten mutants were normally processed and localized at the canalicular membrane of HepG2 cells, but showed dramatically impaired PC transport activity that was significantly rescued by treatment with the clinically approved CFTR potentiator ivacaftor. Our results provide evidence that functional ABCB4 mutations are rescued by ivacaftor, paving the way for the repositioning of this potentiator for the treatment of selected patients with PFIC3 caused by mutations in the ATP-binding sites of ABCB4. [ABSTRACT FROM AUTHOR]

Published
2023
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5. Diagnostic approach to neonatal and infantile cholestasis: A position paper by the SIGENP liver disease working group.

Author

Ranucci, Giusy, Della Corte, Claudia, Alberti, Daniele, Bondioni, Maria Pia, Boroni, Giovanni, Calvo, Pier Luigi, Cananzi, Mara, Candusso, Manila, Clemente, Maria Grazia, D'Antiga, Lorenzo, Degrassi, Irene, De Ville De Goyet, Jean, Di Dato, Fabiola, Di Giorgio, Angelo, Vici, Carlo Dionisi, Ferrari, Federica, Francalanci, Paola, Fuoti, Maurizio, Fusaro, Fabio, and Gaio, Paola

Abstract

Neonatal and infantile cholestasis (NIC) can represent the onset of a surgically correctable disease and of a genetic or metabolic disorder worthy of medical treatment. Timely recognition of NIC and identification of the underlying etiology are paramount to improve outcomes. Upon invitation by the Italian National Institute of Health (ISS), an expert working grouped was formed to formulate evidence-based positions on current knowledge about the diagnosis of NIC. A systematic literature search was conducted to collect evidence about epidemiology, etiology, clinical aspects and accuracy of available diagnostic tests in NIC. Evidence was scored using the GRADE system. All recommendations were approved by a panel of experts upon agreement of at least 75% of the members. The final document was approved by all the panel components. This position document summarizes the collected statements and defines the best-evidence diagnostic approach to cholestasis in the first year of life. [ABSTRACT FROM AUTHOR]

Published
2022
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6. Ivacaftor-Mediated Potentiation of ABCB4 Missense Mutations Affecting Critical Motifs of the NBDs: Repositioning Perspectives for Hepatobiliary Diseases

Author

Jean-Louis Delaunay, Ahmad Elbahnsi, Alix Bruneau, Claire Madry, Anne-Marie Durand-Schneider, Anne Stary, Chantal Housset, Jérémie Gautheron, Isabelle Callebaut, and Tounsia Aït-Slimane

Subjects
bile secretion, genetic liver disease, PFIC3, ABC transporter, potentiators, ivacaftor, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

ABCB4 (ATP-binding cassette subfamily B member 4) is a hepatocanalicular floppase involved in biliary phosphatidylcholine (PC) secretion. Variations in the ABCB4 gene give rise to several biliary diseases, including progressive familial intrahepatic cholestasis type 3 (PFIC3), an autosomal recessive disease that can be lethal in the absence of liver transplantation. In this study, we investigated the effect and potential rescue of ten ABCB4 missense variations in NBD1:NBD2 homologous positions (Y403H/Y1043H, K435M/K1075M, E558K/E1200A, D564G/D1206G and H589Y/H1231Y) all localized at the conserved and functionally critical motifs of ABC transporters, six of which are mutated in patients. By combining structure analysis and in vitro studies, we found that all ten mutants were normally processed and localized at the canalicular membrane of HepG2 cells, but showed dramatically impaired PC transport activity that was significantly rescued by treatment with the clinically approved CFTR potentiator ivacaftor. Our results provide evidence that functional ABCB4 mutations are rescued by ivacaftor, paving the way for the repositioning of this potentiator for the treatment of selected patients with PFIC3 caused by mutations in the ATP-binding sites of ABCB4.

Published
2023
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8. Analysis of the mechanism underlying liver diseases using human induced pluripotent stem cells

Author

Sei Kakinuma and Mamoru Watanabe

Subjects
Cholangiocytes, genetic liver disease, hepatitis B virus, hepatic stellate cells, hepatocytes, Immunologic diseases. Allergy, RC581-607
Abstract

Results of recent studies have shown that disease models using human induced pluripotent stem (iPS) cells have recapitulated the pathophysiology of genetic liver diseases, viral hepatitis and hepatic fibrosis. The utilization of human iPS cells as a model of liver diseases has several substantial advantages compared with primary hepatocytes and cancer cell lines, such as the potential for unlimited expansion and similarity of biological characteristics to normal liver cells. In this review, we have focused on modeling liver diseases using human iPS cells and discussed the experimental evidence that supports the utility of such disease models, including that in our recent studies. Genetically modified or patient-derived human iPS cells can mimic congenital liver disease phenotypes. Human iPS-derived hepatic cells can be infected with the hepatitis viruses. The co-culture of human iPS-derived hepatocytes and mesenchyme partially mimics the process of liver fibrosis. Human iPS cell-derived hepatic cells and the co-culture system of such cells will contribute to the progress of studies on the pathophysiology of genetic and non-genetic liver diseases and development of novel therapeutic strategies for treating liver diseases.

Published
2019
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9. Jaundice revisited: recent advances in the diagnosis and treatment of inherited cholestatic liver diseases

Author

Huey-Ling Chen, Shang-Hsin Wu, Shu-Hao Hsu, Bang-Yu Liou, Hui-Ling Chen, and Mei-Hwei Chang

Subjects
Cholestasis, Genetic liver disease, Pediatric, Progressive familial intrahepatic cholestasis, Next generation sequencing, Bile acids, Medicine
Abstract

Abstract Background Jaundice is a common symptom of inherited or acquired liver diseases or a manifestation of diseases involving red blood cell metabolism. Recent progress has elucidated the molecular mechanisms of bile metabolism, hepatocellular transport, bile ductular development, intestinal bile salt reabsorption, and the regulation of bile acids homeostasis. Main body The major genetic diseases causing jaundice involve disturbances of bile flow. The insufficiency of bile salts in the intestines leads to fat malabsorption and fat-soluble vitamin deficiencies. Accumulation of excessive bile acids and aberrant metabolites results in hepatocellular injury and biliary cirrhosis. Progressive familial intrahepatic cholestasis (PFIC) is the prototype of genetic liver diseases manifesting jaundice in early childhood, progressive liver fibrosis/cirrhosis, and failure to thrive. The first three types of PFICs identified (PFIC1, PFIC2, and PFIC3) represent defects in FIC1 (ATP8B1), BSEP (ABCB11), or MDR3 (ABCB4). In the last 5 years, new genetic disorders, such as TJP2, FXR, and MYO5B defects, have been demonstrated to cause a similar PFIC phenotype. Inborn errors of bile acid metabolism also cause progressive cholestatic liver injuries. Prompt differential diagnosis is important because oral primary bile acid replacement may effectively reverse liver failure and restore liver functions. DCDC2 is a newly identified genetic disorder causing neonatal sclerosing cholangitis. Other cholestatic genetic disorders may have extra-hepatic manifestations, such as developmental disorders causing ductal plate malformation (Alagille syndrome, polycystic liver/kidney diseases), mitochondrial hepatopathy, and endocrine or chromosomal disorders. The diagnosis of genetic liver diseases has evolved from direct sequencing of a single gene to panel-based next generation sequencing. Whole exome sequencing and whole genome sequencing have been actively investigated in research and clinical studies. Current treatment modalities include medical treatment (ursodeoxycholic acid, cholic acid or chenodeoxycholic acid), surgery (partial biliary diversion and liver transplantation), symptomatic treatment for pruritus, and nutritional therapy. New drug development based on gene-specific treatments, such as apical sodium-dependent bile acid transporter (ASBT) inhibitor, for BSEP defects are underway. Short conclusion Understanding the complex pathways of jaundice and cholestasis not only enhance insights into liver pathophysiology but also elucidate many causes of genetic liver diseases and promote the development of novel treatments.

Published
2018
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10. Promoterless gene targeting without nucleases rescues lethality of a Crigler‐Najjar syndrome mouse model

Author

Fabiola Porro, Giulia Bortolussi, Adi Barzel, Alessia De Caneva, Alessandra Iaconcig, Simone Vodret, Lorena Zentilin, Mark A Kay, and Andrés F Muro

Subjects
brain damage, genetic liver disease, homologous recombination, hyperbilirubinemia, kernicterus, Medicine (General), R5-920, Genetics, QH426-470
Abstract

Abstract Crigler‐Najjar syndrome type I (CNSI) is a rare monogenic disease characterized by severe neonatal unconjugated hyperbilirubinemia with a lifelong risk of neurological damage and death. Liver transplantation is the only curative option, which has several limitations and risks. We applied an in vivo gene targeting approach based on the insertion, without the use of nucleases, of a promoterless therapeutic cDNA into the albumin locus of a mouse model reproducing all major features of CNSI. Neonatal transduction with the donor vector resulted in the complete rescue from neonatal lethality, with a therapeutic reduction in plasma bilirubin lasting for at least 12 months, the latest time point analyzed. Mutant mice, which expressed about 5–6% of WT Ugt1a1 levels, showed normal liver histology and motor‐coordination abilities, suggesting no functional liver or brain abnormalities. These results proved that the promoterless gene therapy is applicable for CNSI, providing therapeutic levels of an intracellular ER membrane‐bound enzyme responsible for a lethal liver metabolic disease.

Published
2017
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11. Analysis of the mechanism underlying liver diseases using human induced pluripotent stem cells.

Author

Kakinuma, Sei and Watanabe, Mamoru

Subjects
LIVER disease treatment, PLURIPOTENT stem cells, LIVER cells, CELL lines, PATHOLOGICAL physiology
Abstract

Results of recent studies have shown that disease models using human induced pluripotent stem (iPS) cells have recapitulated the pathophysiology of genetic liver diseases, viral hepatitis and hepatic fibrosis. The utilization of human iPS cells as a model of liver diseases has several substantial advantages compared with primary hepatocytes and cancer cell lines, such as the potential for unlimited expansion and similarity of biological characteristics to normal liver cells. In this review, we have focused on modeling liver diseases using human iPS cells and discussed the experimental evidence that supports the utility of such disease models, including that in our recent studies. Genetically modified or patient-derived human iPS cells can mimic congenital liver disease phenotypes. Human iPS-derived hepatic cells can be infected with the hepatitis viruses. The co-culture of human iPS-derived hepatocytes and mesenchyme partially mimics the process of liver fibrosis. Human iPS cell-derived hepatic cells and the co-culture system of such cells will contribute to the progress of studies on the pathophysiology of genetic and non-genetic liver diseases and development of novel therapeutic strategies for treating liver diseases. [ABSTRACT FROM AUTHOR]

Published
2019
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12. Diagnostic approach to neonatal and infantile cholestasis: A position paper by the SIGENP liver disease working group

Author

Maurizio Fuoti, Mara Cananzi, Giulia Paolella, Manila Candusso, Paola Francalanci, Lidia Monti, Emanuele Nicastro, Lorenzo D'Antiga, Carlo Dionisi Vici, Michele Pinon, Lorenza Matarazzo, Irene Degrassi, P. Gaio, Angelo Di Giorgio, Giusy Ranucci, Pier Luigi Calvo, Giuseppe Indolfi, Claudia Mandato, Fabio Mosca, Pietro Vajro, Maria Pia Bondioni, Maria Iascone, Maria Grazia Clemente, Federica Nuti, Marco Sciveres, Jean de Ville de Goyet, Claudia Della Corte, Marco Spada, Chiara Grimaldi, Federica Ferrari, Gabriella Nebbia, Giuseppe Maggiore, Fabio Fusaro, Daniele Serranti, Daniele Alberti, Fabiola Di Dato, Paola Roggero, Raffaele Iorio, and Giovanni Boroni

Subjects
Male, medicine.medical_specialty, Genetic liver disease, Alagille syndrome, Biliary atresia, Diagnosis, Inborn errors of metabolism, Jaundice, Monogenic liver disease, Newborn, Female, Gastroenterology, Humans, Infant, Infant, Newborn, Cholestasis, Evidence-Based Medicine, Infant, Newborn, Diseases, Practice Guidelines as Topic, Diseases, Disease, Liver disease, Epidemiology, medicine, Intensive care medicine, Hepatology, business.industry, medicine.disease, Etiology, Position paper, medicine.symptom, business
Abstract

Neonatal and infantile cholestasis (NIC) can represent the onset of a surgically correctable disease and of a genetic or metabolic disorder worthy of medical treatment. Timely recognition of NIC and identification of the underlying etiology are paramount to improve outcomes. Upon invitation by the Italian National Institute of Health (ISS), an expert working grouped was formed to formulate evidence-based positions on current knowledge about the diagnosis of NIC. A systematic literature search was conducted to collect evidence about epidemiology, etiology, clinical aspects and accuracy of available diagnostic tests in NIC. Evidence was scored using the GRADE system. All recommendations were approved by a panel of experts upon agreement of at least 75% of the members. The final document was approved by all the panel components. This position document summarizes the collected statements and defines the best-evidence diagnostic approach to cholestasis in the first year of life.

Published
2022

13. Diagnostic approach to neonatal and infantile cholestasis: A position paper by the SIGENP liver disease working group

Author

Ranucci, G, Della Corte, C, Alberti, D, Bondioni, M, Boroni, G, Calvo, P, Cananzi, M, Candusso, M, Clemente, M, D'Antiga, L, Degrassi, I, De Ville De Goyet, J, Di Dato, F, Di Giorgio, A, Vici, C, Ferrari, F, Francalanci, P, Fuoti, M, Fusaro, F, Gaio, P, Grimaldi, C, Iascone, M, Indolfi, G, Iorio, R, Maggiore, G, Mandato, C, Matarazzo, L, Monti, L, Mosca, F, Nebbia, G, Nuti, F, Paolella, G, Pinon, M, Roggero, P, Sciveres, M, Serranti, D, Spada, M, Vajro, P, Nicastro, E, Ranucci G., Della Corte C., Alberti D., Bondioni M. P., Boroni G., Calvo P. L., Cananzi M., Candusso M., Clemente M. G., D'Antiga L., Degrassi I., De Ville De Goyet J., Di Dato F., Di Giorgio A., Vici C. D., Ferrari F., Francalanci P., Fuoti M., Fusaro F., Gaio P., Grimaldi C., Iascone M., Indolfi G., Iorio R., Maggiore G., Mandato C., Matarazzo L., Monti L., Mosca F., Nebbia G., Nuti F., Paolella G., Pinon M., Roggero P., Sciveres M., Serranti D., Spada M., Vajro P., Nicastro E., Ranucci, G, Della Corte, C, Alberti, D, Bondioni, M, Boroni, G, Calvo, P, Cananzi, M, Candusso, M, Clemente, M, D'Antiga, L, Degrassi, I, De Ville De Goyet, J, Di Dato, F, Di Giorgio, A, Vici, C, Ferrari, F, Francalanci, P, Fuoti, M, Fusaro, F, Gaio, P, Grimaldi, C, Iascone, M, Indolfi, G, Iorio, R, Maggiore, G, Mandato, C, Matarazzo, L, Monti, L, Mosca, F, Nebbia, G, Nuti, F, Paolella, G, Pinon, M, Roggero, P, Sciveres, M, Serranti, D, Spada, M, Vajro, P, Nicastro, E, Ranucci G., Della Corte C., Alberti D., Bondioni M. P., Boroni G., Calvo P. L., Cananzi M., Candusso M., Clemente M. G., D'Antiga L., Degrassi I., De Ville De Goyet J., Di Dato F., Di Giorgio A., Vici C. D., Ferrari F., Francalanci P., Fuoti M., Fusaro F., Gaio P., Grimaldi C., Iascone M., Indolfi G., Iorio R., Maggiore G., Mandato C., Matarazzo L., Monti L., Mosca F., Nebbia G., Nuti F., Paolella G., Pinon M., Roggero P., Sciveres M., Serranti D., Spada M., Vajro P., and Nicastro E.

Abstract

Neonatal and infantile cholestasis (NIC) can represent the onset of a surgically correctable disease and of a genetic or metabolic disorder worthy of medical treatment. Timely recognition of NIC and identification of the underlying etiology are paramount to improve outcomes. Upon invitation by the Italian National Institute of Health (ISS), an expert working grouped was formed to formulate evidence-based positions on current knowledge about the diagnosis of NIC. A systematic literature search was conducted to collect evidence about epidemiology, etiology, clinical aspects and accuracy of available diagnostic tests in NIC. Evidence was scored using the GRADE system. All recommendations were approved by a panel of experts upon agreement of at least 75% of the members. The final document was approved by all the panel components. This position document summarizes the collected statements and defines the best-evidence diagnostic approach to cholestasis in the first year of life.

Published
2022

14. Mild Iron Overload as Seen in Individuals Homozygous for the Alpha-1 Antitrypsin Pi*Z Variant Does Not Promote Liver Fibrogenesis in HFE Knockout Mice

Author

Nurdan Guldiken, Karim Hamesch, Shari Malan Schuller, Mahmoud Aly, Cecilia Lindhauer, Carolin V. Schneider, Malin Fromme, Christian Trautwein, and Pavel Strnad

Subjects
iron metabolism, α1-antitrypsin deficiency, rare liver disease, genetic liver disease, serpina1, hfe, liver fibrosis, Cytology, QH573-671
Abstract

The presence of the homozygous ‘Pi*Z’ variant of alpha-1 antitrypsin (AAT) (‘Pi*ZZ’ genotype) predisposes to liver fibrosis development, but the role of iron metabolism in this process remains unknown. Therefore, we assessed iron metabolism and variants in the Homeostatic Iron Regulator gene (HFE) as the major cause of hereditary iron overload in a large cohort of Pi*ZZ subjects without liver comorbidities. The human cohort comprised of 409 Pi*ZZ individuals and 254 subjects without evidence of an AAT mutation who were recruited from ten European countries. All underwent a comprehensive work-up and transient elastography to determine liver stiffness measurements (LSM). The corresponding mouse models (Pi*Z overexpressors, HFE knockouts, and double transgenic [DTg] mice) were used to evaluate the impact of mild iron overload on Pi*Z-induced liver injury. Compared to Pi*Z non-carriers, Pi*ZZ individuals had elevated serum iron, transferrin saturation, and ferritin levels, but relevant iron overload was rare. All these parameters were higher in individuals with signs of significant liver fibrosis (LSM ≥ 7.1 kPa) compared to those without signs of significant liver fibrosis. HFE knockout and DTg mice displayed similar extent of iron overload and of fibrosis. Loss of HFE did not alter the extent of AAT accumulation. In Pi*ZZ individuals, presence of HFE mutations was not associated with more severe liver fibrosis. Taken together, Pi*ZZ individuals display minor alterations in serum iron parameters. Neither mild iron overload seen in these individuals nor the presence of HFE mutations (C282Y and H63D) constitute a major contributor to liver fibrosis development.

Published
2019
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15. Promoterless gene targeting without nucleases rescues lethality of a Crigler-Najjar syndrome mouse model.

Author

Porro, Fabiola, Bortolussi, Giulia, Barzel, Adi, De Caneva, Alessia, Iaconcig, Alessandra, Vodret, Simone, Zentilin, Lorena, Kay, Mark A, and Muro, Andrés F

Abstract

Crigler-Najjar syndrome type I ( CNSI) is a rare monogenic disease characterized by severe neonatal unconjugated hyperbilirubinemia with a lifelong risk of neurological damage and death. Liver transplantation is the only curative option, which has several limitations and risks. We applied an in vivo gene targeting approach based on the insertion, without the use of nucleases, of a promoterless therapeutic cDNA into the albumin locus of a mouse model reproducing all major features of CNSI. Neonatal transduction with the donor vector resulted in the complete rescue from neonatal lethality, with a therapeutic reduction in plasma bilirubin lasting for at least 12 months, the latest time point analyzed. Mutant mice, which expressed about 5-6% of WT Ugt1a1 levels, showed normal liver histology and motor-coordination abilities, suggesting no functional liver or brain abnormalities. These results proved that the promoterless gene therapy is applicable for CNSI, providing therapeutic levels of an intracellular ER membrane-bound enzyme responsible for a lethal liver metabolic disease. [ABSTRACT FROM AUTHOR]

Published
2017
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16. Long-term Outcomes of Patients With Wilson Disease in a Large Austrian Cohort.

Author

Beinhardt, Sandra, Leiss, Waltraud, Stättermayer, Albert Friedrich, Graziadei, Ivo, Zoller, Heinz, Stauber, Rudolf, Maieron, Andreas, Datz, Christian, Steindl-Munda, Petra, Hofer, Harald, Vogel, Wolfgang, Trauner, Michael, and Ferenci, Peter

Abstract

Background & Aims: Wilson disease is an autosomal recessive disorder that affects copper metabolism, leading to copper accumulation in liver, central nervous system, and kidneys. There are few data on long-term outcomes and survival from large cohorts; we studied these features in a well-characterized Austrian cohort of patients with Wilson disease. Methods: We analyzed data from 229 patients diagnosed with Wilson disease from 1961 through 2013; 175 regularly attended a Wilson disease outpatient clinic and/or their physicians were contacted for information on disease and treatment status and outcomes. For 53 patients lost during the follow-up period, those that died and reasons for their death were identified from the Austrian death registry. Results: The mean observation period was 14.8 ± 11.4 years (range, 0.5–52.0 years), resulting in 3116 patient-years. Of the patients, 61% presented with hepatic disease, 27% with neurologic symptoms, and 10% were diagnosed by family screening at presymptomatic stages. Patients with a hepatic presentation were diagnosed younger (21.2 ± 12.0 years) than patients with neurologic disease (28.8 ± 12.0; P < .001). In 2% of patients, neither symptoms nor onset of symptoms could be determined with certainty. Most patients stabilized (35%) or improved on chelation therapy (26% fully recovered, 24% improved), but 15% deteriorated; 8% required a liver transplant, and 7.4% died within the observation period (71% of deaths were related to Wilson disease). A lower proportion of patients with Wilson disease survived for 20 years (92%) than healthy Austrians (97%), adjusted for age and sex (P = .03). Cirrhosis at diagnosis was the best predictor of death (odds ratio, 6.8; 95% confidence interval, 1.5–31.03; P = .013) and need for a liver transplant (odds ratio, 07; 95% confidence interval, 0.016–0.307; P < .001). Only 84% of patients with cirrhosis survived 20 years after diagnosis (compared with healthy Austrians, P =.008). Conclusion: Overall, patients who receive adequate care for Wilson disease have a good long-term prognosis. However, cirrhosis increases the risk of death and liver disease. Early diagnosis, at a precirrhotic stage, might increase survival times and reduce the need for a liver transplant. [Copyright &y& Elsevier]

Published
2014
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17. Bone marrow stem-cell therapy for genetic and chronic liver diseases.

Author

Kochat, Veena, Baligar, Prakash, Maiwall, Rakhi, and Mukhopadhyay, Asok

Abstract

There are no permanent remedies for patients suffering from genetic liver diseases (GLDs) and liver cirrhosis (LC). In such cases, liver transplantation has resulted in improved quality of life, but it is not affordable by most patients. Therefore, a cost-effective, safe, and permanent cure for these diseases is desirable. Cell therapy seems an encouraging option for treatment of these liver diseases in the future. Animal experiments and clinical studies have demonstrated that, depending on the nature of the liver disease and the patient, autologous and/or allogeneic bone marrow (BM)-derived stem-cell therapy could be a promising treatment option. Although no clinical trials using BM-derived stem cells for treatment of GLD have yet been conducted, many phase I clinical trials have been conducted and a few such trials for the treatment of LC by use of autologous and/or allogeneic cells are in progress. Overall, the results of these trials are indicative of clinical benefits with no adverse effect on the patients. This review focuses on the current status of BM stem-cell therapy for treatment of GLD and LC in experimental animals and human subjects. It also proposes safer approaches to immune-regulation in allogeneic transplantation of cells. [ABSTRACT FROM AUTHOR]

Published
2014
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18. Mild Iron Overload as Seen in Individuals Homozygous for the Alpha-1 Antitrypsin Pi*Z Variant Does Not Promote Liver Fibrogenesis in HFE Knockout Mice

Author

Pavel Strnad, C Lindhauer, Nurdan Guldiken, Christian Trautwein, Mahmoud Aly, Carolin V. Schneider, Karim Hamesch, Malin Fromme, and Shari Malan Schuller

Subjects
0301 basic medicine, Liver Cirrhosis, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Iron Overload, genetic liver disease, Alpha (ethology), Mice, Transgenic, hfe, α1-antitrypsin deficiency, Article, serpina1, 03 medical and health sciences, Mice, 0302 clinical medicine, Fibrosis, Internal medicine, ddc:570, medicine, Animals, iron metabolism, Hemochromatosis Protein, lcsh:QH301-705.5, Gene knockout, liver fibrosis, Liver injury, Mice, Knockout, medicine.diagnostic_test, Transferrin saturation, business.industry, Homozygote, General Medicine, medicine.disease, Disease Models, Animal, 030104 developmental biology, Endocrinology, lcsh:Biology (General), alpha 1-Antitrypsin, Knockout mouse, Mutation, Serum iron, 030211 gastroenterology & hepatology, SERPINA1, rare liver disease, HFE, Disease Susceptibility, Transient elastography, business
Abstract

The presence of the homozygous &lsquo, Pi*Z&rsquo, variant of alpha-1 antitrypsin (AAT) (&lsquo, Pi*ZZ&rsquo, genotype) predisposes to liver fibrosis development, but the role of iron metabolism in this process remains unknown. Therefore, we assessed iron metabolism and variants in the Homeostatic Iron Regulator gene (HFE) as the major cause of hereditary iron overload in a large cohort of Pi*ZZ subjects without liver comorbidities. The human cohort comprised of 409 Pi*ZZ individuals and 254 subjects without evidence of an AAT mutation who were recruited from ten European countries. All underwent a comprehensive work-up and transient elastography to determine liver stiffness measurements (LSM). The corresponding mouse models (Pi*Z overexpressors, HFE knockouts, and double transgenic [DTg] mice) were used to evaluate the impact of mild iron overload on Pi*Z-induced liver injury. Compared to Pi*Z non-carriers, Pi*ZZ individuals had elevated serum iron, transferrin saturation, and ferritin levels, but relevant iron overload was rare. All these parameters were higher in individuals with signs of significant liver fibrosis (LSM &ge, 7.1 kPa) compared to those without signs of significant liver fibrosis. HFE knockout and DTg mice displayed similar extent of iron overload and of fibrosis. Loss of HFE did not alter the extent of AAT accumulation. In Pi*ZZ individuals, presence of HFE mutations was not associated with more severe liver fibrosis. Taken together, Pi*ZZ individuals display minor alterations in serum iron parameters. Neither mild iron overload seen in these individuals nor the presence of HFE mutations (C282Y and H63D) constitute a major contributor to liver fibrosis development.

Published
2019
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20. Lebertransplantation bei Familiärer Amyloid Polyneuropathie Fallbericht und Literaturübersicht.

Author

Krüger, M., Altland, K., Linke, R. P., Maschek, H., Ringe, B., Oehler, G., Pichlmayr, R., and Manns, M. P.

Abstract

Copyright of Der Internist is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
1997
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21. Promoterless gene targeting without nucleases rescues lethality of a Crigler-Najjar syndrome mouse model

Author

Alessandra Iaconcig, Fabiola Porro, Mark A. Kay, Andrés F. Muro, Alessia De Caneva, Lorena Zentilin, Simone Vodret, Adi Barzel, and Giulia Bortolussi

Subjects
0301 basic medicine, hyperbilirubinemia, Crigler–Najjar syndrome, Genetic enhancement, medicine.medical_treatment, Mutant, genetic liver disease, homologous recombination, Biology, Liver transplantation, 03 medical and health sciences, Transduction (genetics), Mice, Transduction, Genetic, Report, medicine, kernicterus, Animals, Humans, Glucuronosyltransferase, Promoter Regions, Genetic, Crigler-Najjar Syndrome, Albumin, Gene targeting, Brain, Bilirubin, Genetic Therapy, brain damage, medicine.disease, Survival Analysis, Mice, Mutant Strains, 3. Good health, Disease Models, Animal, 030104 developmental biology, Liver, Immunology, Gene Targeting, Cancer research, Molecular Medicine, Kernicterus, Genetics, Gene Therapy & Genetic Disease, Reports
Abstract

Crigler‐Najjar syndrome type I (CNSI) is a rare monogenic disease characterized by severe neonatal unconjugated hyperbilirubinemia with a lifelong risk of neurological damage and death. Liver transplantation is the only curative option, which has several limitations and risks. We applied an in vivo gene targeting approach based on the insertion, without the use of nucleases, of a promoterless therapeutic cDNA into the albumin locus of a mouse model reproducing all major features of CNSI. Neonatal transduction with the donor vector resulted in the complete rescue from neonatal lethality, with a therapeutic reduction in plasma bilirubin lasting for at least 12 months, the latest time point analyzed. Mutant mice, which expressed about 5–6% of WT Ugt1a1 levels, showed normal liver histology and motor‐coordination abilities, suggesting no functional liver or brain abnormalities. These results proved that the promoterless gene therapy is applicable for CNSI, providing therapeutic levels of an intracellular ER membrane‐bound enzyme responsible for a lethal liver metabolic disease.

Published
2017

22. Genome editing in the human liver: Progress and translational considerations.

Author

Ginn SL, Christina S, and Alexander IE

Subjects
Genetic Therapy, Genome, Humans, Liver, CRISPR-Cas Systems, Gene Editing
Abstract

Liver-targeted genome editing offers the prospect of life-long therapeutic benefit following a single treatment and is set to rapidly supplant conventional gene addition approaches. Combining progress in liver-targeted gene delivery with genome editing technology, makes this not only feasible but realistically achievable in the near term. However, important challenges remain to be addressed. These include achieving therapeutic levels of editing, particularly in vivo, avoidance of off-target effects on the genome and the potential impact of pre-existing immunity to bacteria-derived nucleases, when used to improve editing rates. In this chapter, we outline the unique features of the liver that make it an attractive target for genome editing, the impact of liver biology on therapeutic efficacy, and disease specific challenges, including whether the approach targets a cell autonomous or non-cell autonomous disease. We also discuss strategies that have been used successfully to achieve genome editing outcomes in the liver and address translational considerations as genome editing technology moves into the clinic., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published
2021
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23. Non-Invasive Assessment and Management of Liver Involvement in Adults With Alpha-1 Antitrypsin Deficiency.

Author

Hamesch K and Strnad P

Abstract

Alpha-1 antitrypsin deficiency (AATD) is a systemic disorder affecting mainly the lung and the liver and is caused by mutations in SERPINA1 , the AAT gene. A homozygous "Pi*Z" mutation (Pi*ZZ genotype) may cause liver fibrosis on its own independently of pulmonary AATD manifestation, while heterozygous Pi*Z carriage (Pi*MZ genotype) is considered a strong risk factor for development of liver cirrhosis in patients with concomitant liver disease such as alcoholic and non-alcoholic liver disease. In Pi*ZZ homozygotes, liver disease constitutes the second leading cause of death and is highly heterogeneous. About 35% of Pi*ZZ individuals display significant liver fibrosis on biopsy (i.e., fibrosis stage ≥ 2 on scale 0-4). Among non-invasive methods for liver fibrosis assessment, liver stiffness measurement (LSM) via vibration-controlled transient elastography (VCTE) has been most widely evaluated. Based on these data, Pi*ZZ adults have 20x increased odds of developing advanced liver fibrosis (i.e., fibrosis stage ≥ 3) than adults without AAT mutation. Risk factors for accelerated fibrosis progression are male sex, age ≥ 50 years, alcohol misuse, obesity, diabetes mellitus, or metabolic syndrome. Unlike VCTE, other ultrasound- and magnetic resonance-based elastography methods have been assessed in small cohorts of Pi*ZZ individuals and remain to be comprehensively validated. Among blood-based fibrosis tests, AST-to-platelet ratio index (APRI) correlates moderately with histologic fibrosis stage and LSM. Given APRI's wide availability, it can be used for risk stratification as an adjunct to LSM or when LSM is not at hand. Despite recent efforts, AATD-related liver disease, especially for genotypes other than Pi*ZZ, remains greatly understudied. AATD individuals should be offered liver biochemistry, liver ultrasound, and non-invasive fibrosis assessment at the time of diagnosis to detect potential complications and for proper risk stratification. If signs of AATD-related liver disease occur (i.e., pathologic fibrosis test or repeatedly elevated liver enzymes), patients should be referred to a health care center specialized in AATD-related liver disease and be screened for potentially treatable comorbidities. To exclude the latter, they may need a liver biopsy. Moreover, every health care provider of an AATD individual should be aware of the potential liver manifestation, counsel their patient on modifiable hepatic risk factors, and offer them regular liver check-ups., (JCOPDF © 2020.)

Published
2020
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24. Mild Iron Overload as Seen in Individuals Homozygous for the Alpha-1 Antitrypsin Pi*Z Variant Does Not Promote Liver Fibrogenesis in HFE Knockout Mice.

Author

Guldiken, Nurdan, Hamesch, Karim, Schuller, Shari Malan, Aly, Mahmoud, Lindhauer, Cecilia, Schneider, Carolin V., Fromme, Malin, Trautwein, Christian, and Strnad, Pavel

Subjects
*KNOCKOUT mice, *TRYPSIN inhibitors, *IRON, *LIVER, *IRON metabolism, *TRANSFERRIN, *FERRITIN
Abstract

The presence of the homozygous 'Pi*Z' variant of alpha-1 antitrypsin (AAT) ('Pi*ZZ' genotype) predisposes to liver fibrosis development, but the role of iron metabolism in this process remains unknown. Therefore, we assessed iron metabolism and variants in the Homeostatic Iron Regulator gene (HFE) as the major cause of hereditary iron overload in a large cohort of Pi*ZZ subjects without liver comorbidities. The human cohort comprised of 409 Pi*ZZ individuals and 254 subjects without evidence of an AAT mutation who were recruited from ten European countries. All underwent a comprehensive work-up and transient elastography to determine liver stiffness measurements (LSM). The corresponding mouse models (Pi*Z overexpressors, HFE knockouts, and double transgenic [DTg] mice) were used to evaluate the impact of mild iron overload on Pi*Z-induced liver injury. Compared to Pi*Z non-carriers, Pi*ZZ individuals had elevated serum iron, transferrin saturation, and ferritin levels, but relevant iron overload was rare. All these parameters were higher in individuals with signs of significant liver fibrosis (LSM ≥ 7.1 kPa) compared to those without signs of significant liver fibrosis. HFE knockout and DTg mice displayed similar extent of iron overload and of fibrosis. Loss of HFE did not alter the extent of AAT accumulation. In Pi*ZZ individuals, presence of HFE mutations was not associated with more severe liver fibrosis. Taken together, Pi*ZZ individuals display minor alterations in serum iron parameters. Neither mild iron overload seen in these individuals nor the presence of HFE mutations (C282Y and H63D) constitute a major contributor to liver fibrosis development. [ABSTRACT FROM AUTHOR]

Published
2019
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25. [Inherited metabolic diseases and liver transplantation].

Author

Kuerbanjiang A and Wang JS

Subjects
Humans, Metabolic Diseases, Quality of Life, Liver Diseases, Liver Transplantation
Abstract

Worldwide, liver transplantation for adults and children is rapidly developing with the advancement of surgical techniques, market availability of new immunosuppressant drugs, and improved post-surgical management. Previously, liver transplantation was limited to end-stage liver disease, but recently many patients with inherited metabolic diseases achieves prolong survival and better quality of life. This article reviews the latest trends in the relationship between inherited metabolic diseases and liver, characteristics of inherited metabolic liver diseases, inherited metabolic disorders that may need liver transplantation, indications for liver transplant, and the key points of perioperative management.

Published
2019
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26. Resolved Psychosis after Liver Transplantation in a Patient with Wilson's Disease

Author

Margherita Sini, Mauro Giovanni Carta, Daniela Riccio, Orazio Sorbello, and Luigi Demelia

Subjects
Psychosis, medicine.medical_specialty, Pediatrics, Cirrhosis, Orthotopic liver transplantation, Epidemiology, business.industry, Copper metabolism, medicine.medical_treatment, genetic liver disease, Disease, OLT, Liver transplantation, medicine.disease, Article, Wilson's disease, Psychiatry and Mental health, psychiatric illness, Medicine, Liver function, psychosis, Wilson’s disease, business, Psychiatry
Abstract

A psychiatric involvement is frequently present in Wilson’s disease. Psychiatric symptoms are sometimes the first and only manifestation of Wilson’s disease. More often a psychiatric involvement is present beside a neurologic or hepatic disease. We describe the case of a 18 years-old male patient who shows a clinic and laboratoristic pattern of cirrhosis and an history of subchronic hallucinatory psychosis, behavioral symptoms and mood disturbances with depressed mood. He hadn’t familiar history of liver or psychiatric disease. Laboratory and imaging tests confirmed the diagnosis of Wilson’s disease with psichiatric involvement. After liver transplantation copper metabolism and liver function normalised and we noticed no recurrency of the psichiatric illness. Very few cases of psychiatric improvement after orthotopic liver transplantation (OLT) has been described until now.

Published
2010

27. Epidemiología y factores de riesgo de carcinoma hepatocelular

Author

BOTERO TORO, ALEJANDRA, LONDOÑO SANIN, MARCELA, and NAVAS NAVAS, MARIA-CRISTINA

Subjects
TABACO, HORMONAL FACTORS, GENETIC LIVER DISEASE, DIABETES MELLITUS, HEPATITIS B VIRUS, ALCOHOL, EPIDEMIOLOGY, HEPATOCELLULAR CARCINOMA, CARCINOMA HEPATOCELULAR, HEPATOPATÍAS GENÉTICAS, TOBACCO, DIABETES MELLI, FACTORES HORMONALES, VIRUS DE LA HEPATITIS B, VIRUS DE LA HEPATITIS C, HEPATITIS C VIRUS, PREVALENCIA, ESTEATOHEPATITIS NO ALCOHÓLICA (NASH), AFLATOXINS, PREVALENCE, FACTORES DE RIESGO, OBESIDAD, INCIDENCIA, OBESITY, RISK FACTORS, NON ALCOHOLIC STEATO HEPATITIS (NASH), EPIDEMIOLOGÍA, AFLATOXINAS, INCIDENCE
Abstract

El cáncer primario de hígado es en el mundo la quinta neoplasia más común en hombres y la octava en mujeres, con gran impacto debido a su alta mortalidad, ya que representa la tercera causa de mortalidad relacionada con cáncer en población masculina. Se ha descrito una fuerte asociación con factores de riesgo como las hepatitis virales crónicas, las hepatopatías de origen genético, el consumo de alcohol, el tabaquismo y enfermedades metabólicas, entre otras. En este artículo se analizan publicaciones originales y de revisión en las que se evalúan dichos factores y su asociación con el carcinoma hepatocelular (CHC). Además, se recopila información actualizada sobre datos epidemiológicos por regiones del mundo. Primary liver cancer is the 5th neoplasia more common among men and 8th among women worldwide. It has a great impact because of its high mortality; Liver cancer ranks third amongst the causes of cancer-related deaths in men. It has been associated with some risk factors as chronic viral hepatitis, genetic liver disease, intake of alcohol, use of tobacco, metabolic disease and others. This document corresponds to a review of original papers of evaluation of those factors and its association with liver cancer and also reviewed articles. Additionally, updated epidemiological information of liver cancer worldwide is included.

Published
2007

28. Resolved Psychosis after Liver Transplantation in a Patient with Wilson's Disease.

Author

Sorbello O, Riccio D, Sini M, Carta M, and Demelia L

Abstract

A psychiatric involvement is frequently present in Wilson's disease. Psychiatric symptoms are sometimes the first and only manifestation of Wilson's disease. More often a psychiatric involvement is present beside a neurologic or hepatic disease.We describe the case of a 18 years-old male patient who shows a clinic and laboratoristic pattern of cirrhosis and an history of subchronic hallucinatory psychosis, behavioral symptoms and mood disturbances with depressed mood. He hadn't familiar history of liver or psychiatric disease. Laboratory and imaging tests confirmed the diagnosis of Wilson's disease with psichiatric involvement. After liver transplantation copper metabolism and liver function normalised and we noticed no recurrency of the psichiatric illness. Very few cases of psychiatric improvement after orthotopic liver transplantation (OLT) has been described until now.

Published
2011
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