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一个非裔美国家庭中TSC2基因的突变分析

Mutation analysis of the TSC2 gene in an African-American family.

作者信息

Kumar A, Kandt R S, Wolpert C, Roses A D, Pericak-Vance M A, Gilbert J R

机构信息

Division of Neurology, Duke Unversity Medical Center, Durham, NC 27710, USA.

出版信息

Hum Mol Genet. 1995 Dec;4(12):2295-8. doi: 10.1093/hmg/4.12.2295.

Abstract

Tuberous sclerosis complex is an autosomal dominant disorder with loci on chromosome 9q34 (TSC1) and chromosome 16p13.3 (TSC2). The TSC2 gene has been isolated. To date, only a small number of intragenic deletional and point mutations have been detected, almost exclusively in sporadic (no family history) cases. With the exception of a single parent/offspring pair, there have been no published reports of mutations in extended multigenerational chromosome 16-linked TSC2 families. For our TSC studies we ascertained and sampled a four-generation African-American TSC family that shows a high likelihood for linkage to chromosome 16 (z=1.53). Using single-strand conformation polymorphism analysis we identified a 4590/4591delC mutation in exon 34. The 4590/4591delC causes a frameshift mutation resulting in the creation of a premature stop codon. In addition, we have detected a 542del4 polymorphism in the two partially overlapping polyadenylation signals in exon 40 that segregates in the family. The polymorphism has been detected in six of 72 African-American control chromosomes examined, and has not been detected in 80 Caucasian control chromosomes examined.

摘要

结节性硬化症是一种常染色体显性疾病,其基因座位于9号染色体长臂3区4带(TSC1)和16号染色体短臂1区3带3亚带(TSC2)。TSC2基因已被分离出来。迄今为止,仅检测到少数基因内缺失和点突变,几乎都仅见于散发(无家族病史)病例。除了一对亲子外,尚无关于16号染色体连锁的TSC2基因在多代扩展家族中发生突变的报道。为了进行结节性硬化症的研究,我们确定并选取了一个四代非裔美国人结节性硬化症家族进行样本分析,该家族显示出与16号染色体连锁的高可能性(z = 1.53)。通过单链构象多态性分析,我们在第34外显子中鉴定出一个4590/4591delC突变。4590/4591delC导致移码突变,产生一个提前的终止密码子。此外,我们在第40外显子中两个部分重叠的聚腺苷酸化信号中检测到一个542del4多态性,该多态性在家族中呈分离状态。在所检测的72条非裔美国人对照染色体中有6条检测到该多态性,而在检测的80条白种人对照染色体中未检测到。

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