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A novel c. 204 Ile68Met germline variant in exon 2 of the mutL homolog 1 gene in a colorectal cancer patient

机译:小说c。结肠直肠癌患者mutL homolog 1基因第2外显子中的204 Ile68Met种系变异

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摘要

Mutations in the mutL homolog 1 (MLH1) gene are frequent in patients with hereditary non-polyposis colorectal cancer (CRC). The MLH1 gene was screened for mutations in patients with sporadic CRC. The nucleotide sequences for all 19 exons of MLH1 were analyzed by high resolution melting and sequenced in a group of 104 sporadic CRC patients, and the results were verified in a replication group of 1,095 patients and 1,469 controls. Different melting profiles for exon 2 of the MLH1 gene were observed in the germline DNA of one patient. Sequencing of the patient's DNA resulted in the identification of a heterozygous C>G variant at c.204, which resulted in an Ile68Met change in the amino acid. A detailed search of the National Center for Biotechnology Information and the 1000 Genomes databases indicated that the detected variant was unique. According to the SIFT and PolyPhen-2 algorithms, the substitution of Ile to Met was predicted to decrease the activity of the MLH1 protein. The newly identified, functional germline variant was not present in any other CRC patient or control. Thus, a novel germline variant in the MLH1 gene was identified, representing a rare event in sporadic CRC. The occurrence and relevance of this mutation in other types of cancer requires additional investigation.
机译:遗传性非息肉病性结直肠癌(CRC)患者经常发生mutL homolog 1(MLH1)基因突变。筛查MLH1基因在散发性CRC患者中的突变。通过高分辨率熔解分析了MLH1的所有19个外显子的核苷酸序列,并对104名散发性CRC患者进行了测序,并在1,095名患者和1,469名对照的复制组中验证了结果。在一名患者的生殖系DNA中观察到了MLH1基因外显子2的不同熔解曲线。患者DNA的测序导致在c.204处鉴定出杂合的C> G变异体,从而导致Ile68Met氨基酸发生变化。对国家生物技术信息中心和1000个基因组数据库的详细搜索表明,检测到的变异是唯一的。根据SIFT和PolyPhen-2算法,预计将Ile取代为Met会降低MLH1蛋白的活性。新发现的功能种系变异体未出现在任何其他CRC患者或对照中。因此,鉴定出了MLH1基因中的新种系变体,代表了散发性CRC中的罕见事件。此突变在其他类型癌症中的发生和相关性需要进一步调查。

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