An insertion mutation in ABCB4 is associated with gallbladder mucocele formation in dogs.

Katrina L Mealey, Jonathan D Minch, Stephen N White, Kevin R Snekvik, John S Mattoon
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引用次数: 33

Abstract

Background: ABCB4 functions as a phosphatidylcholine translocater, flipping phosphatidylcholine across hepatocyte canalicular membranes into biliary canaliculi. In people, ABCB4 gene mutations are associated with several disease syndromes including intrahepatic cholestasis of pregnancy, progressive familial intrahepatic cholestasis (type 3), primary biliary cirrhosis, and cholelithiasis. Hepatobiliary disease, specifically gallbladder mucocele formation, has been recognized with increased frequency in dogs during the past decade. Because Shetland Sheepdogs are considered to be predisposed to gallbladder mucoceles, we initially investigated ABCB4 as a candidate gene for gallbladder mucocele formation in that breed, but included affected dogs of other breeds as well.

Results: An insertion (G) mutation in exon 12 of canine ABCB4 (ABCB4 1583_1584G) was found to be significantly associated with hepatobiliary disease in Shetland Sheepdogs specifically (P < 0.0001) as well as other breeds (P < 0.0006). ABCB4 1583_1584G results in a frame shift generating four stop codons that prematurely terminate ABCB4 protein synthesis within exon 12, abolishing over half of the protein including critical ATP and a putative substrate binding site.

Conclusions: The finding of a significant association of ABCB4 1583_1584G with gallbladder mucoceles in dogs suggests that this phospholipid flippase may play a role in the pathophysiology of this disorder. Affected dogs may provide a useful model for identifying novel treatment strategies for ABCB4-associated hepatobiliary disease in people.

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ABCB4的插入突变与犬胆囊粘液囊肿的形成有关。
背景:ABCB4作为磷脂酰胆碱转运器,将磷脂酰胆碱通过肝细胞小管膜翻转到胆管。在人类中,ABCB4基因突变与几种疾病综合征相关,包括妊娠肝内胆汁淤积症、进行性家族性肝内胆汁淤积症(3型)、原发性胆汁性肝硬化和胆石症。肝胆疾病,特别是胆囊粘液囊肿形成,在过去十年中已被认为在狗中频率增加。由于设得兰牧羊犬被认为易患胆囊粘液囊肿,我们最初研究了ABCB4作为该品种胆囊粘液囊肿形成的候选基因,但也包括其他品种的受影响犬。结果:犬ABCB4基因第12外显子插入(G)突变(ABCB4 1583_1584G)与设得兰牧羊犬(P < 0.0001)以及其他犬种(P < 0.0006)的肝胆疾病有显著相关性。ABCB4 1583_1584G导致帧移位,产生四个终止密码子,提前终止ABCB4蛋白外显子12内的合成,消除超过一半的蛋白质,包括关键ATP和假定的底物结合位点。结论:ABCB4 1583_1584G与犬胆囊黏液囊肿的显著相关性表明,该磷脂翻转酶可能在该疾病的病理生理中发挥作用。受影响的狗可能为确定人类abcb4相关肝胆疾病的新治疗策略提供有用的模型。
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