2018
DOI: 10.1186/s12929-018-0475-8
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Jaundice revisited: recent advances in the diagnosis and treatment of inherited cholestatic liver diseases

Abstract: BackgroundJaundice 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 bodyThe major genetic diseases causing jaundice involve disturbances of bile flow. The insufficiency of bile salts in the intestines leads to fat malabsor… Show more

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Cited by 111 publications
(95 citation statements)
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“…Infantile low/normal GGT cholestasis comprises a series of monogenic defects. Except for ARC syndrome, other defects usually manifest a spectrum of familial cholestasis of different severity, or varied phenotypes from intractable watery diarrhea to isolated cholestasis (Bull & Thompson, ; Chen et al, ). In addition, hereditary diseases that typically result in multiorgan disorders may manifest isolated hepatopathy at times.…”
Section: Introductionmentioning
confidence: 99%
“…Infantile low/normal GGT cholestasis comprises a series of monogenic defects. Except for ARC syndrome, other defects usually manifest a spectrum of familial cholestasis of different severity, or varied phenotypes from intractable watery diarrhea to isolated cholestasis (Bull & Thompson, ; Chen et al, ). In addition, hereditary diseases that typically result in multiorgan disorders may manifest isolated hepatopathy at times.…”
Section: Introductionmentioning
confidence: 99%
“…Given that patients with ALGS and PFIC have intrahepatic accumulations of bile acids that can damage tissues in the liver and spill over into systemic circulation, SBD procedures were developed to interrupt enterohepatic circulation and reduce the bile acid pool in these patients. 8,15 SBD is often associated with reductions in serum bile acids and pruritus as well as improvements in sleep disturbance, quality of life, fibrosis and growth. [53][54][55] In the case of PFIC, most of the currently available data on SBD are based on ATP8B1-and ABCB11-deficient patients.…”
Section: Interrup Ti On Of the Enterohepati C Circul Ati On A S A Tmentioning
confidence: 99%
“…4,5 Cholestasis is defined as the impaired formation or flow of bile in the hepatobiliary system and may be intrahepatic (involving hepatocytes, bile canaliculi or intrahepatic bile ducts) or extrahepatic (involving the bile ducts outside the liver or the gallbladder). [6][7][8] In cholestasis, which can present with features of jaundice or pruritus, the accumulation of bile acids may damage liver cells such that fibrotic and inflammatory pathways are activated that lead to liver injury. 1,2,6 Common cholestatic liver diseases include Alagille syndrome (ALGS), progressive familial intrahepatic cholestasis (PFIC) and biliary atresia in children and primary biliary cholangitis (PBC) or primary sclerosing cholangitis (PSC) in adults.…”
Section: Introductionmentioning
confidence: 99%
“…Notably, biochemical criteria of hepatotoxicity in adults with cholestatic disease may not apply to paediatric populations due to development‐related differences in the normal ranges of common liver tests including total bilirubin, aminotransferases, and ALP from early infancy through the pubertal growth spurt. In addition, certain hereditary cholestatic liver diseases in infants and children are not associated with the characteristic rise in GGT that are seen in PBC or PSC and cannot be relied upon as a marker of cholestatic injury . During growth in normal paediatric study subjects, ALP levels are affected by fluctuations of the enzyme derived from bone.…”
Section: Paediatric Cholestatic Liver Diseasementioning
confidence: 99%
“…In addition, certain hereditary cholestatic liver diseases in infants and children are not associated with the characteristic rise in GGT that are seen in PBC or PSC and cannot be relied upon as a marker of cholestatic injury. 169 During growth in normal paediatric study subjects, ALP levels are affected by fluctuations of the enzyme derived from bone. Changes of ALP in paediatric patients are also typically observed with vitamin D deficiency.…”
Section: Paed Iatri C Chole S Tati C Liver Dise a Sementioning
confidence: 99%