Robert Botea, Madalina Piron-Dumitrascu, Tiberiu Augustin Georgescu, Camil Laurentiu Bohiltea, Silviu Cristian Voinea, Valentin Nicolae Varlas, Simona Raluca Iacoban, Nicolae Suciu
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This study aims to fill this gap by performing a detailed comparative analysis of germline and somatic mutations in endometrial cancer within the context of Lynch syndrome.</p><p><strong>Methods: </strong>We conducted whole exome sequencing on matched germline and somatic DNA from 13 patients diagnosed with Lynch syndrome-associated endometrial cancer. High-depth sequencing was performed, followed by rigorous bioinformatics analysis to identify and annotate variants, focusing on their potential pathogenicity and relevance to both endometrial and colorectal cancer.</p><p><strong>Results: </strong>Our analysis revealed 1,118 germline and 14,051 somatic variants, with 493 variants common to both. Recurrent pathogenic mutations in MLH1, MSH2, and MSH6 were confirmed, highlighting their critical role in Lynch syndrome. Notably, frequent somatic mutations in the PIK3CA and PTEN genes were identified, implicating the PI3K/AKT/mTOR pathway as a key oncogenic driver in these cancers. Additionally, novel somatic mutations in genes related to the extracellular matrix such as FBN1 and SPARC were uncovered, suggesting a possible unique role in endometrial tumor progression.</p><p><strong>Conclusions: </strong>This study provides new insights into the molecular basis of Lynch syndrome-associated endometrial cancer, emphasizing the overlap in oncogenic pathways with colorectal cancer. The discovery of shared and unique genetic mutations highlights the importance of developing combined treatment strategies and suggests that targeting these specific mutations could improve therapy for patients with Lynch syndrome-associated cancers.</p>","PeriodicalId":94081,"journal":{"name":"Journal of gastrointestinal and liver diseases : JGLD","volume":" ","pages":"339-347"},"PeriodicalIF":0.0000,"publicationDate":"2024-09-29","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Lynch Syndrome-associated Genomic Variants.\",\"authors\":\"Robert Botea, Madalina Piron-Dumitrascu, Tiberiu Augustin Georgescu, Camil Laurentiu Bohiltea, Silviu Cristian Voinea, Valentin Nicolae Varlas, Simona Raluca Iacoban, Nicolae Suciu\",\"doi\":\"10.15403/jgld-5856\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background and aims: </strong>Lynch Syndrome, a hereditary disorder characterized by germline mutations in mismatch repair (MMR) genes, is a major contributor to colorectal cancers. 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引用次数: 0
摘要
背景和目的:林奇综合征是一种以错配修复(MMR)基因的种系突变为特征的遗传性疾病,是结直肠癌的主要诱因。在子宫内膜癌中也发现了这种疾病。尽管已确定 MMR 缺陷在肿瘤发生中的作用,但驱动林奇综合征相关子宫内膜癌的特定基因组改变及其与结肠直肠癌的重叠仍不完全清楚。本研究旨在通过对林奇综合征背景下子宫内膜癌的种系突变和体细胞突变进行详细的比较分析来填补这一空白:方法:我们对 13 名被诊断为林奇综合征相关子宫内膜癌患者的匹配种系和体细胞 DNA 进行了全外显子测序。我们进行了高深度测序,随后进行了严格的生物信息学分析,以识别和注释变异,重点关注其潜在的致病性以及与子宫内膜癌和结肠直肠癌的相关性:我们的分析发现了1,118个种系变异和14,051个体细胞变异,其中493个变异在两种情况下都存在。MLH1、MSH2和MSH6的致病突变得到证实,突显了它们在林奇综合征中的关键作用。值得注意的是,在PIK3CA和PTEN基因中发现了频繁的体细胞突变,这表明PI3K/AKT/mTOR通路是这些癌症的关键致癌驱动因素。此外,还发现了FBN1和SPARC等与细胞外基质相关的基因发生了新的体细胞突变,这表明它们在子宫内膜肿瘤的发展过程中可能起着独特的作用:本研究为林奇综合征相关子宫内膜癌的分子基础提供了新的见解,强调了其与结直肠癌在致癌途径上的重叠。共同和独特基因突变的发现凸显了制定联合治疗策略的重要性,并表明针对这些特定突变可以改善林奇综合征相关癌症患者的治疗。
Background and aims: Lynch Syndrome, a hereditary disorder characterized by germline mutations in mismatch repair (MMR) genes, is a major contributor to colorectal cancers. It has also been identified in endometrial cancer. Despite the established role of MMR deficiency in tumorigenesis, the specific genomic alterations driving Lynch syndrome-associated endometrial cancer, and their overlap with colorectal cancer, remain incompletely understood. This study aims to fill this gap by performing a detailed comparative analysis of germline and somatic mutations in endometrial cancer within the context of Lynch syndrome.
Methods: We conducted whole exome sequencing on matched germline and somatic DNA from 13 patients diagnosed with Lynch syndrome-associated endometrial cancer. High-depth sequencing was performed, followed by rigorous bioinformatics analysis to identify and annotate variants, focusing on their potential pathogenicity and relevance to both endometrial and colorectal cancer.
Results: Our analysis revealed 1,118 germline and 14,051 somatic variants, with 493 variants common to both. Recurrent pathogenic mutations in MLH1, MSH2, and MSH6 were confirmed, highlighting their critical role in Lynch syndrome. Notably, frequent somatic mutations in the PIK3CA and PTEN genes were identified, implicating the PI3K/AKT/mTOR pathway as a key oncogenic driver in these cancers. Additionally, novel somatic mutations in genes related to the extracellular matrix such as FBN1 and SPARC were uncovered, suggesting a possible unique role in endometrial tumor progression.
Conclusions: This study provides new insights into the molecular basis of Lynch syndrome-associated endometrial cancer, emphasizing the overlap in oncogenic pathways with colorectal cancer. The discovery of shared and unique genetic mutations highlights the importance of developing combined treatment strategies and suggests that targeting these specific mutations could improve therapy for patients with Lynch syndrome-associated cancers.
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