Assessing pathogenicity of mismatch repair variants of uncertain significance by molecular tumor analysis

IF 2.8 4区医学 Q2 PATHOLOGY Experimental and molecular pathology Pub Date : 2024-10-21 DOI:10.1016/j.yexmp.2024.104940

Anne-Sophie van der Werf't Lam , Noah C. Helderman , Arnoud Boot , Diantha Terlouw , Hans Morreau , Hailian Mei , Rebecca E.E. Esveldt-van Lange , Inge M.M. Lakeman , Christi J. van Asperen , Emmelien Aten , Nandy Hofland , Pia A.M. de Koning Gans , Emily Rayner , Carli Tops , Niels de Wind , Tom van Wezel , Maartje Nielsen

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Abstract

Functional analyses are the main method to classify mismatch repair (MMR) gene variants of uncertain significance (VUSs). However, the pathogenicity remains unclear for many variants because of conflicting results between clinical, molecular, and functional data. In this study, we evaluated whether whole exome sequencing (WES) could add another layer of evidence to elucidate the pathogenicity of MMR variants with conflicting interpretations. WES was performed on formalin-fixed paraffin-embedded tumor tissue of eight patients with a constitutional MMR VUS (seven families), including eight colorectal and two endometrial carcinomas and one ovarian carcinoma. Cell-free CIMRA assays were performed to assign Odds of Pathogenicity to these VUSs. In four families, seven tumors showed MMR deficiency-associated mutational signatures, supporting the pathogenicity of the VUS. Moreover, somatic (second) MMR hits identified in the WES data were found to explain MMR staining patterns when the MMR staining was discordant with the reported germline MMR gene variant. In conclusion, WES did not significantly reclassify VUS in these cases but clarified some phenotypic aspects such as age of onset and explanations in case of discordant MMR stainings.

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通过肿瘤分子分析评估意义不明的错配修复变体的致病性。

功能分析是对意义不确定的错配修复（MMR）基因变异进行分类的主要方法。然而，由于临床、分子和功能数据之间的结果相互矛盾，许多变异的致病性仍不明确。在本研究中，我们评估了全外显子组测序（WES）能否为阐明存在解释冲突的 MMR 变异的致病性提供另一层证据。我们对八名MMR VUS患者（七个家族）的福尔马林固定石蜡包埋肿瘤组织进行了全外显子组测序，其中包括八例结直肠癌、两例子宫内膜癌和一例卵巢癌。进行了无细胞 CIMRA 检测，以确定这些 VUS 的致病几率。在四个家族中，七个肿瘤显示出与 MMR 缺乏相关的突变特征，支持了 VUS 的致病性。此外，当MMR染色与报告的种系MMR基因变异不一致时，WES数据中发现的体细胞（第二）MMR命中可解释MMR染色模式。总之，在这些病例中，WES 并没有对 VUS 进行明显的重新分类，但澄清了一些表型方面的问题，如发病年龄和 MMR 染色不一致时的解释。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Experimental and molecular pathology 医学-病理学

CiteScore

8.90

自引率

0.00%

发文量

审稿时长

11.5 weeks

期刊介绍： Under new editorial leadership, Experimental and Molecular Pathology presents original articles on disease processes in relation to structural and biochemical alterations in mammalian tissues and fluids and on the application of newer techniques of molecular biology to problems of pathology in humans and other animals. The journal also publishes selected interpretive synthesis reviews by bench level investigators working at the "cutting edge" of contemporary research in pathology. In addition, special thematic issues present original research reports that unravel some of Nature''s most jealously guarded secrets on the pathologic basis of disease. Research Areas include: Stem cells; Neoangiogenesis; Molecular diagnostics; Polymerase chain reaction; In situ hybridization; DNA sequencing; Cell receptors; Carcinogenesis; Pathobiology of neoplasia; Complex infectious diseases; Transplantation; Cytokines; Flow cytomeric analysis; Inflammation; Cellular injury; Immunology and hypersensitivity; Athersclerosis.