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叙利亚 GIST 患者 KIT 跨膜区突变的生物信息学分析:完成拼图。

Bioinformatic analysis of KIT juxtamembrane domain mutations in Syrian GIST patients: jigsaw puzzle completed.

机构信息

Department of Biochemistry and Microbiology, Faculty of Pharmacy, Damascus University, Damascus, Syria.

Clinical Laboratories Department, Al-Assad Hospital, Damascus University, PO Box 10769, Damascus, Syria.

出版信息

J Egypt Natl Canc Inst. 2023 Aug 14;35(1):25. doi: 10.1186/s43046-023-00185-0.

Abstract

BACKGROUND

The huge number of detected somatic KIT mutations highlights the necessity of in silico analyses that are almost absent in the relevant medical literature. The aim of this study is to report the mutation spectrum analysis of exon 11 encoding the juxtamembrane (JM) domain of the KIT gene in a group of Syrian GIST patients.

METHODS

Forty-eight formalin-fixed paraffin-embedded GIST tissue samples, collected between 2006 and 2016, were retrieved from the pathological archives and analyzed for KIT exon 11 mutations by DNA sequencing. Structural/functional impact of detected variants was predicted using several bioinformatic tools.

RESULTS

Twenty-one different variants have been detected in intron 10, exon 11, and intron 11 of the KIT gene, eight of which were novel changes. Mutations in exon 11 of the KIT gene were detected in 28 of 48 (58.3%) GIST patients and predicted to be pathogenic and cancer promoting. Specifically, age above 60 was very significantly associated with the negative selection of deletion mutations (p = .007), a phenomenon that points to deletion severity.

CONCLUSIONS

Six bioinformatic tools have proved efficient in predicting the impact of detected KIT variations in view of published structural, experimental, and clinical findings.

摘要

背景

大量检测到的体细胞 KIT 突变突出表明需要进行计算机分析,而这在相关的医学文献中几乎不存在。本研究的目的是报告一组叙利亚 GIST 患者中编码 KIT 基因跨膜区(JM)结构域的外显子 11 的突变谱分析。

方法

从病理档案中检索了 2006 年至 2016 年间收集的 48 例福尔马林固定石蜡包埋的 GIST 组织样本,并通过 DNA 测序分析 KIT 外显子 11 突变。使用多种生物信息学工具预测检测到的变异的结构/功能影响。

结果

在 KIT 基因的内含子 10、外显子 11 和内含子 11 中检测到 21 种不同的变异,其中 8 种是新的变化。在 48 例 GIST 患者中的 28 例(58.3%)检测到 KIT 基因外显子 11 的突变,预测为致病性和促进癌症的突变。具体来说,年龄超过 60 岁与缺失突变的负选择非常显著相关(p=.007),这一现象表明缺失的严重程度。

结论

鉴于已发表的结构、实验和临床发现,六种生物信息学工具已被证明在预测检测到的 KIT 变异的影响方面非常有效。

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