Familial Hepatocellular Cholestasis

Frederick J. Suchy; Benjamin L. Shneider

doi:10.1017/CBO9780511547409.016

14 - Familial Hepatocellular Cholestasis

from SECTION II - CHOLESTATIC LIVER DISEASES

Published online by Cambridge University Press: 18 December 2009

Frederick J. Suchy M.D. and

Benjamin L. Shneider M.D.

Edited by

Frederick J. Suchy ,

Ronald J. Sokol and

William F. Balistreri

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Frederick J. Suchy M.D.: Affiliation:
Professor and Chair, Department of Pediatrics, Mount Sinai School of Medicine of New York University, New York, New York; Pediatrician-in-Chief, Department of Pediatrics, Mount Sinai Hospital, New York, New York
Benjamin L. Shneider M.D.: Affiliation:
Visiting Professor, Department of Pediatrics, University of Pittsburgh, Pittsburgh, Pennsylvania; Director of Pediatric Hepatology, Department of Pediatrics/Gastroenterology, Children's Hospital of Pittsburgh, Pittsburgh, Pennsylvania
Frederick J. Suchy: Affiliation:
Mount Sinai School of Medicine, New York
Ronald J. Sokol: Affiliation:
University of Colorado, Denver
William F. Balistreri: Affiliation:
University of Cincinnati

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Summary

Inherited cholestasis of hepatocellular origin has long been described in the neonate or during the first year of life [1]. Many of these infants were categorized as having idiopathic neonatal hepatitis after biliary atresia, metabolic diseases, and congenital infections were excluded [2, 3]. The prognosis in familial cases was poor compared with sporadic cases that sometimes had an identifiable etiology. As the clinical and genotypic heterogeneity of these inherited disorders has become apparent, it is now recognized that patients may present initially and progress to end-stage liver disease at ages ranging from infancy to adulthood [4]. There may be significant overlap in clinical features such as intense pruritus and a low serum concentration of γ-glutamyl transpeptidase (γGT). The histopathology, immunohistochemical staining, and hepatic ultrastructure may provide additional diagnostic clues as to the underlying defect. However, the identification of the genes responsible for several of these disorders now allows a specific diagnosis in many cases, may suggest therapy with varying success based on the genotype of the patient, and has advanced our understanding of molecular mechanisms of bile secretion and acquired cholestasis. It is not surprising that, so far, mutations in three genes encoding adenosine triphosphate (ATP)-dependent transport proteins localized to the canalicular membrane that result in progressive cholestasis and liver injury have been discovered. The features of these disorders are compared in Table 14.1. Other genes encoding proteins involved in membrane transport, vesicular trafficking, and integrity of the cell junction may also be mutated in some patients.

Type: Chapter
Information: Liver Disease in Children , pp. 310 - 325

DOI: https://doi.org/10.1017/CBO9780511547409.016 [Opens in a new window]

Publisher: Cambridge University Press

Print publication year: 2007

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