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对韩国重型血友病 A 患者因子 VIII 的突变分析。

Mutation analysis of factor VIII in Korean patients with severe hemophilia A.

机构信息

Department of Pediatrics, Eulji University School of Medicine, Daejeon, 301-832, Korea.

出版信息

Int J Hematol. 2010 Jun;91(5):784-91. doi: 10.1007/s12185-010-0593-x. Epub 2010 Jun 10.

Abstract

Hemophilia A is an X-linked recessive disorder caused by mutations of the factor VIII gene. The mutation spectrum has been reported in various populations, but not in Koreans. Mutation analysis of the factor VIII gene was performed in 22 unrelated Korean patients with severe hemophilia A. We extracted genomic DNA from their blood, and assessed intron inversions, deletions, and point mutations by direct DNA sequencing. A multiplex ligation-dependent probe amplification gene dosage assay was also performed to identify exon deletions. Disease-causing mutations were identified in all patients, of which four cases were previously unreported. Seven intron 22 inversions, nine point mutations (6 nonsense mutations and 3 missense mutations), and four small rearrangements were identified. One multi-exon deletion and one 5'-donor splicing site mutation were also observed. Four novel mutations (one small deletion, one multiple exon deletion, one missense, and one splice site mutation) were detected, and point mutations were predominant (40.9%), followed by intron 22 inversions (31.8%). Further studies are required in order to establish a solid conclusion regarding the prevalence of various mutations in the Korean population.

摘要

血友病 A 是一种 X 连锁隐性遗传病,由凝血因子 VIII 基因的突变引起。已经在不同人群中报道了突变谱,但在韩国人群中尚未报道。对 22 名无亲缘关系的严重血友病 A 韩国患者的凝血因子 VIII 基因进行了突变分析。我们从他们的血液中提取基因组 DNA,并通过直接 DNA 测序评估内含子倒位、缺失和点突变。还进行了多重连接依赖性探针扩增基因剂量测定以鉴定外显子缺失。在所有患者中均发现了致病突变,其中 4 例为先前未报道的病例。鉴定出 7 例内含子 22 倒位、9 个点突变(6 个无义突变和 3 个错义突变)和 4 个小重排。还观察到 1 例多外显子缺失和 1 例 5'供体位点突变。检测到 4 种新的突变(1 种小缺失、1 种多外显子缺失、1 种错义突变和 1 种剪接位点突变),点突变占主导地位(40.9%),其次是内含子 22 倒位(31.8%)。需要进一步研究才能确定韩国人群中各种突变的流行率。

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