Nijbroek G, Sood S, McIntosh I, Francomano C A, Bull E, Pereira L, Ramirez F, Pyeritz R E, Dietz H C
Department of Pediatrics, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
Am J Hum Genet. 1995 Jul;57(1):8-21.
Mutations in the gene encoding fibrillin-1 (FBN1), a component of the extracellular microfibril, cause the Marfan syndrome (MFS). This statement is supported by the observations that the classic Marfan phenotype cosegregates with intragenic and/or flanking marker alleles in all families tested and that a significant number of FBN1 mutations have been identified in affected individuals. We have now devised a method to screen the entire coding sequence and flanking splice junctions of FBN1. On completion for a panel of nine probands with classic MFS, six new mutations were identified that accounted for disease in seven (78%) of nine patients. Nine additional new mutations have been characterized in the early stages of a larger screening project. These 15 mutations were equally distributed throughout the gene and, with one exception, were specific to single families. One-third of mutations created premature termination codons, and 6 of 15 substituted residues with putative significance for calcium binding to epidermal growth factor (EGF)-like domains. Mutations causing severe and rapidly progressive disease that presents in the neonatal period can occur in a larger region of the gene than previously demonstrated, and the nature of the mutation is as important a determinant as its location, in predisposing to this phenotype.
编码原纤维蛋白-1(FBN1)的基因突变可导致马凡综合征(MFS),原纤维蛋白-1是细胞外微原纤维的一个组成部分。这一观点得到了如下观察结果的支持:在所有被检测的家族中,典型的马凡表型与基因内和/或侧翼标记等位基因共分离,并且在受影响个体中已鉴定出大量FBN1突变。我们现已设计出一种方法来筛查FBN1的整个编码序列和侧翼剪接位点。在对一组9名患有典型MFS的先证者完成筛查后,鉴定出6个新突变,这6个新突变导致9名患者中的7名(78%)患病。在一个更大规模的筛查项目的早期阶段,又鉴定出另外9个新突变。这15个突变在整个基因中均匀分布,且除一个外,均为单个家族所特有。三分之一的突变产生了提前终止密码子,15个突变中有6个替换了对钙结合表皮生长因子(EGF)样结构域具有推定意义的残基。与之前所证明的相比,导致新生儿期出现严重且快速进展疾病的突变可发生在基因的更大区域,并且在易患此表型方面,突变的性质与其位置一样,都是重要的决定因素。
