Shovlin C L, Hughes J M, Scott J, Seidman C E, Seidman J G
Department of Genetics, Harvard Medical School, Boston, MA 02115, USA.
Am J Hum Genet. 1997 Jul;61(1):68-79. doi: 10.1086/513906.
To identify mutations that cause hereditary hemorrhagic telangiectasia (HHT, or Rendu-Osler-Weber syndrome), clinical evaluations and genetic studies were performed on 32 families. Linkage studies in four of eight families indicated an endoglin (ENG) gene mutation. ENG sequences of affected members of the four linked families and probands from the 24 small families were screened for mutations, by Southern blot analyses and by cycle sequencing of PCR-amplified DNA. Seven novel mutations were identified in eight families. Two mutations (a termination codon in exon 4 and a large genomic deletion extending 3' of intron 8) did not produce a stable ENG transcript in lymphocytes. Five other mutations (two donor splice-site mutations and three deletions) produce altered mRNAs that are predicted to encode markedly truncated ENG proteins. Mutations in other families are predicted to lie in ENG-regulatory regions or in one of the additional genes that may cause HHT. These data suggest that the molecular mechanism by which ENG mutations cause HHT is haploinsufficiency. Furthermore, because the clinical manifestation of disease in these eight families was similar, we hypothesize that phenotypic variation of HHT is not related to a particular ENG mutation.
为了鉴定导致遗传性出血性毛细血管扩张症(HHT,即遗传性出血性毛细血管扩张综合征)的突变,我们对32个家族进行了临床评估和基因研究。在八个家族中的四个家族进行的连锁研究表明存在内皮糖蛋白(ENG)基因突变。通过Southern印迹分析和对PCR扩增的DNA进行循环测序,对四个连锁家族的患病成员以及24个小家族的先证者的ENG序列进行突变筛查。在八个家族中鉴定出七个新的突变。两个突变(外显子4中的终止密码子和延伸至内含子8 3'端的大片段基因组缺失)在淋巴细胞中未产生稳定的ENG转录本。其他五个突变(两个供体剪接位点突变和三个缺失)产生了改变的mRNA,预计这些mRNA编码明显截短的ENG蛋白。其他家族中的突变预计位于ENG调控区域或可能导致HHT的其他基因之一中。这些数据表明ENG突变导致HHT的分子机制是单倍体不足。此外,由于这八个家族中疾病的临床表现相似,我们推测HHT的表型变异与特定的ENG突变无关。
