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利用法医 STR 试剂盒检测胃肠道肿瘤的遗传高突变性。

Detecting genetic hypermutability of gastrointestinal tumor by using a forensic STR kit.

机构信息

State Key Laboratory of Genetic Engineering, Institute of Genetics, School of Life Sciences, Fudan University, Shanghai, 200433, China.

Shanghai Key Laboratory of Forensic Medicine, Shanghai Forensic Service Platform, Institute of Forensic Sciences, Ministry of Justice, Shanghai, 200063, China.

出版信息

Front Med. 2020 Feb;14(1):101-111. doi: 10.1007/s11684-019-0698-4. Epub 2019 Jul 31.

DOI:10.1007/s11684-019-0698-4
PMID:31368030
Abstract

Growing evidence suggests that somatic hypermutational status and programmed cell death-1 overexpression are potential predictive biomarkers indicating treatment benefits from immunotherapy using immune checkpoint inhibitors. However, biomarker-matched trials are still limited, and many of the genomic alterations remain difficult to target. To isolate the potential somatic hypermutational tumor from microsatellite instability low/microsatellite stability (MSI-L/MSS) cases, we employed two commercial kits to determine MSI and forensic short tandem repeat (STR) alternations in 250 gastrointestinal (GI) tumors. Three types of forensic STR alternations, namely, allelic loss, Aadd, and Anew, were identified. 62.4% (156/250) of the patients with GI exhibited STR alternation, including 100% (15/15) and 60% (141/235) of the microsatellite high instability and MSI-L/MSS cases, respectively. 30% (75/250) of the patients exhibited STR instability with more than 26.32% (26.32%-84.21%) STR alternation. The cutoff with 26.32% of the STR alternations covered all 15 MSI cases and suggested that it might be a potential threshold. Given the similar mechanism of the mutations of MSI and forensic STR, the widely used forensic identifier STR kit might provide potential usage for identifying hypermutational status in GI cancers.

摘要

越来越多的证据表明,体细胞超突变状态和程序性细胞死亡-1 过表达是潜在的预测生物标志物,表明免疫检查点抑制剂免疫治疗的获益。然而,生物标志物匹配的试验仍然有限,许多基因组改变仍然难以靶向。为了从微卫星不稳定性低/微卫星稳定(MSI-L/MSS)病例中分离出潜在的体细胞超突变肿瘤,我们采用了两种商业试剂盒来确定 250 例胃肠道(GI)肿瘤的 MSI 和法医短串联重复(STR)改变。鉴定出三种类型的法医 STR 改变,即等位基因缺失、Aadd 和 Anew。62.4%(250/250)的 GI 患者存在 STR 改变,其中微卫星高度不稳定和 MSI-L/MSS 病例分别为 100%(15/15)和 60%(141/235)。30%(250/250)的患者存在 STR 不稳定性,其 STR 改变超过 26.32%(26.32%-84.21%)。STR 改变率为 26.32%的截断值覆盖了所有 15 例 MSI 病例,并提示这可能是一个潜在的阈值。鉴于 MSI 和法医 STR 突变的机制相似,广泛使用的法医标识符 STR 试剂盒可能为鉴定 GI 癌症中的超突变状态提供潜在用途。

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Investigation of an Alternative Marker for Hypermutability Evaluation in Different Tumors.不同肿瘤中高突变评估替代标志物的研究。
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