Gallione C J, Klaus D J, Yeh E Y, Stenzel T T, Xue Y, Anthony K B, McAllister K A, Baldwin M A, Berg J N, Lux A, Smith J D, Vary C P, Craigen W J, Westermann C J, Warner M L, Miller Y E, Jackson C E, Guttmacher A E, Marchuk D A
Department of Genetics, Duke University Medical Center, Durham, North Carolina 27710, USA.
Hum Mutat. 1998;11(4):286-94. doi: 10.1002/(SICI)1098-1004(1998)11:4<286::AID-HUMU6>3.0.CO;2-B.
Hereditary Hemorrhagic Telangiectasia (HHT) is an autosomal dominant disorder characterized by multisystemic vascular dysplasia and recurrent hemorrhage from the sites of vascular lesions. Two genes have been identified for HHT. Endoglin, a TGF-beta binding protein which maps to chromosome 9q3, is the gene for HHT1. The type and location of most of the previously described mutations in the endoglin (ENG) gene suggested a dominant-negative model of receptor-complex dysfunction for the molecular basis of this disorder. In this article we describe 11 novel ENG mutations in HHT kindreds, which include missense and splice-site mutations. Two identical missense mutations in unrelated families disrupt the start codon of the gene. In addition, some frameshift and nonsense mutations lead to very low or undetectable levels of transcript from the mutant allele. These combined data suggest that the nature of most ENG mutations is to create a null (nonfunctional) allele, and that there is no requirement for the synthesis of a truncated endoglin protein in the pathogenesis of HHT.
遗传性出血性毛细血管扩张症(HHT)是一种常染色体显性疾病,其特征为多系统血管发育异常以及血管病变部位反复出血。已确定与HHT相关的两个基因。内皮糖蛋白是一种转化生长因子β结合蛋白,定位于9号染色体长臂3区,是HHT1的致病基因。内皮糖蛋白(ENG)基因中大多数先前描述的突变类型和位置提示,受体复合物功能障碍的显性负性模型是该疾病分子基础。在本文中,我们描述了HHT家系中的11种新的ENG突变,包括错义突变和剪接位点突变。在不相关的家族中有两个相同的错义突变破坏了该基因的起始密码子。此外,一些移码突变和无义突变导致突变等位基因的转录水平非常低或无法检测到。这些综合数据表明,大多数ENG突变的本质是产生一个无效(无功能)等位基因,并且在HHT发病机制中不需要合成截短的内皮糖蛋白。
