Jansen J B M J, Morsche R H M Te, Drenth J P H
Universitair Medisch Centrum St Radboud, afd. Maag-, Darm- en Leverziekten, Postbus 9101, 6500 HB Nijmegen.
Ned Tijdschr Geneeskd. 2003 Jul 19;147(29):1408-12.
Polycystic liver disease (PCLD, MIM 174050) is a dominantly inherited condition characterised by the presence in the liver of multiple cysts of biliary epithelial origin. It must be distinguished from autosomal dominant polycystic kidney disease type 1 (ADPKD-1, MIM 173900) and type 2 (ADPKD-2). Both disorders may be complicated by polycystic liver disease, but renal involvement is absent in PCLD. PCLD is often asymptomatic, but if symptoms arise, they are usually due to the mass effect of cysts. The phenotype is more severe in females and correlates with the number of pregnancies or estrogen use. The gene for PCLD has been assigned to chromosome 19p13.2-13.1. Two separate large-scale positional cloning efforts have managed to identify PRKCSH as the gene underlying PCLD. Up to now, all mutations found in PRKCSH introduce stopcodons in the m-RNA, resulting in premature termination of translation to protein. This suggests a loss of function of the encoding protein. The protein, designated by us as hepatocystin, is predicted to be localised in the endoplasmic reticulum. Multiple biological roles have been suggested for hepatocystin, such as a substrate for phosphorylation by protein kinase C, binding to advanced glycation endproducts, and a function as the non-catalytic beta-subunit of glucosidase-II. The role of hepatocystin in PCLD, however, remains to be elucidated.
多囊肝病(PCLD,MIM 174050)是一种常染色体显性遗传病,其特征是肝脏中存在多个源于胆管上皮的囊肿。它必须与1型常染色体显性多囊肾病(ADPKD - 1,MIM 173900)和2型(ADPKD - 2)相区分。这两种疾病都可能并发多囊肝病,但PCLD不存在肾脏受累情况。PCLD通常无症状,但如果出现症状,通常是由于囊肿的占位效应。女性的表型更严重,且与怀孕次数或雌激素使用有关。PCLD的基因已被定位于19号染色体的p13.2 - 13.1区域。两项独立的大规模定位克隆研究已成功确定PRKCSH是PCLD的致病基因。到目前为止,在PRKCSH中发现的所有突变都会在mRNA中引入终止密码子,导致蛋白质翻译提前终止。这表明编码蛋白功能丧失。我们将该蛋白命名为肝囊肿素,预计其定位于内质网。肝囊肿素具有多种生物学作用,如作为蛋白激酶C磷酸化的底物、与晚期糖基化终产物结合以及作为葡糖苷酶II的非催化β亚基发挥作用。然而,肝囊肿素在PCLD中的作用仍有待阐明。
