扩展COL7A1突变数据库:41例营养不良性大疱表皮松解症患者中新发和再发突变及少见的基因型-表型相互影响因素

Dystrophic epidermolysis bullosa (DEB), a heterogeneous hereditary skin disorder characterized by trauma-induced blistering and scarring, affects thousands of families world wide. The clinical manifestations extend from minor nail dystrophy to severe life-threatening blistering, making early molecular diagnosis and prognostication of utmost importance for the affected families. DEB is caused by mutations in the COL7A1 gene encoding collagen VII in the skin. Molecular diagnostics and genotype-phenotype correlations in DEB remain complex owing to the gene structure, large variety of mutations, high rate of novel mutations, complex protein structure and assembly, and the heterogeneity of phenotypes. Here, we report an efficient strategy for COL7A1mutation detection using direct automated DNA sequencing and implementation of software tools. With this approach, COL7A1 mutations of 41 DEB families were disclosed. Twenty-four mutations were novel and two recurrent. Elucidation of biological consequences of the mutations helped define disease mechanisms, but also revealed several unusual genotypic and/or phenotypic constellations, which impeded the diagnostics and prognostication. In addition, the studies disclosed a de novo mutation in recessive DEB and two new polymorphisms in the COL7A1 gene.

COL7A1基因突变导致营养不良型大疱性表皮松解症1例

目的研究1例营养不良型大疱表皮松解症(DEB)的基因突变情况及其临床意义。方法收集临床资料,取皮损行病理学、电镜检查,取患儿及其父母外周血行基因检查。结果皮肤病理学检查见表皮下水疱。电镜检查见表皮基底与表皮连接松解。患儿COL7A1基因复合杂合突变。结论患儿其父源基因突变为c.3157delG;母源基因突变为c.846+2T>C。2个位点突变尚未见先例报道,故本研究进一步补充了目前DEB的突变位点库,并为患儿及其家属遗传咨询提供可靠依据。

COL7A1基因复合杂合突变致隐性营养不良型大疱性表皮松解症1家系研究

目的 分析1例常染色体隐性营养不良型大疱性表皮松解症患者临床表型,探讨该家系COL7A1基因突变情况。方法 收集1例常染色体隐性营养不良型大疱性表皮松解症患者(先证者)及其家系临床资料。采集先证者及其母亲外周血(先证者父亲病逝),提取基因组DNA,采用高通量测序法对先证者皮肤病相关基因各外显子编码区进行测序,确定基因变异位点,采用PCR-Sanger测序法验证致病性突变情况。应用软件分析剪接突变、错义突变位点保守性及致病性。结果 先证者临床表现为双手背、腹部及双足多发红色斑块、结痂,瘙痒明显,指/趾甲营养不良及脱落,口腔舌体黏膜白斑;血清总蛋白、球蛋白、IgG水平升高,自然杀伤细胞绝对数、自然杀伤细胞百分比、淋巴细胞绝对数降低;心电图示多导联ST-T改变;家系3代仅先证者1人患病。先证者存在COL7A1基因c.841_846+1dup和c.5560G>A(p.Gly1854Arg)复合杂合突变;母亲存在c.5560G>A(p.Gly1854Arg)突变;c.841_846+1dup为剪接突变,突变导致6号外显子3′端正常供体剪接位点丢失,并在下游7 bp处激活形成新的供体剪接位点,使7号外显子发生提早终止密码子,此突变在人类基因突变数据库中未收录,为新突变。c.5560G>A(p.Gly1854Arg)为错义突变,65号外显子编码区第5 560位核苷酸由鸟嘌呤突变为腺嘌呤,编码蛋白第1 854位甘氨酸突变为精氨酸,COL7A1编码蛋白在多个物种第1 854位甘氨酸序列中呈完全保守,该突变具有致病性。根据先证者临床表现、辅助检查、基因检测及家系特征,诊断为常染色体隐性遗传营养不良型大疱性表皮松解症。结论 COL7A1基因c.841_846+1dup和c.5560G>A(p.Gly1854Arg)复合杂合突变是该先证者临床表型的可能原因。

锚原纤维与营养不良性大疱性表皮松解症

锚原纤维具有维持真表皮紧密连接的作用 ,其主要结构成分是 型胶原 , 型胶原基因 (COL7A1)突变是营养不良性大疱性表皮松解症 (DEB)的分子发病机制。本文主要综述如下两个方面的研究进展 :1 型胶原的分子结构、基因结构及其调控功能 ;2 COL7A1的提早终止密码突变 (PTC)和甘氨酸置换突变对锚原纤维分子生物学特性的影响—— 型胶原的数量变化和质量变化 (分子折叠、聚合和分泌等发生异常 )是