Genetic Services of Western Australia, King Edward Memorial Hospital, University of Western Australia, Perth, Australia.
Am J Med Genet A. 2011 Apr;155A(4):717-20. doi: 10.1002/ajmg.a.33906. Epub 2011 Mar 15.
We report on a 20-year-old man who presented in infancy with severe generalized lipodystrophy with a progeroid appearance and some Marfanoid features. He subsequently was diagnosed with bilateral lens subluxations at the age of 16 years which prompted analysis of the FBN1 gene. This analysis showed him to have a novel heterozygous, de novo, c.8156_8175del, p.Lys2719ThrfsX12, frameshift mutation in exon 64 of his FBN1 gene. His phenotype is similar to a patient described by Graul-Neumann et al. [2010] who was found to have a de novo, heterozygous, c.8155_8156del deletion in exon 64 of FBN1. Both mutations result in a truncated protein with an extremely charged C-terminus, containing two positive and four negative charges in the last eight amino acids. This most likely has a profound impact on protein–protein interactions, which are very important in the extracellular matrix. The similarities in the phenotypes, and overlapping molecular defects, provides further evidence that the phenotype with features of Marfan syndrome with neonatal progeroid syndrome-like lipodystrophy is a distinct clinical entity due to frameshift mutations in exon 64 of the FBN1 gene.
我们报告了一例 20 岁男性,其在婴儿期表现出严重的全身性脂肪营养不良,具有早衰样外观和一些马凡氏综合征特征。随后,他在 16 岁时被诊断出双侧晶状体半脱位,这促使我们对 FBN1 基因进行了分析。该分析显示他携带一种新的杂合性、新生的 c.8156_8175del 突变,导致第 64 外显子中的赖氨酸 2719 突变为苏氨酸并提前终止(p.Lys2719ThrfsX12)。他的表型与 Graul-Neumann 等人[2010]描述的患者相似,该患者被发现携带 FBN1 第 64 外显子中的新生杂合性 c.8155_8156del 缺失突变。这两种突变都导致截短的蛋白,其 C 末端带有极强的电荷,在最后八个氨基酸中含有两个正电荷和四个负电荷。这极有可能对蛋白质-蛋白质相互作用产生深远影响,而这些相互作用在细胞外基质中非常重要。表型的相似性以及重叠的分子缺陷进一步证明,具有马凡氏综合征特征的新生儿早衰样脂肪营养不良表型是一种独特的临床实体,是由于 FBN1 基因第 64 外显子的移码突变所致。
