TP53 mutation status and consensus molecular subtypes of colorectal cancer in patients from Rwanda.

IF 3.4 2区医学 Q2 ONCOLOGY BMC Cancer Pub Date : 2024-10-11 DOI:10.1186/s12885-024-13009-8

Augustin Nzitakera, Delphine Uwamariya, Hisami Kato, Jean Bosco Surwumwe, André Mbonigaba, Ella Larissa Ndoricyimpaye, Schifra Uwamungu, Felix Manirakiza, Marie Claire Ndayisaba, Gervais Ntakirutimana, Benoit Seminega, Vincent Dusabejambo, Eric Rutaganda, Placide Kamali, François Ngabonziza, Rei Ishikawa, Hirofumi Watanabe, Belson Rugwizangoga, Satoshi Baba, Hidetaka Yamada, Katsuhiro Yoshimura, Yasuhiro Sakai, Haruhiko Sugimura, Kazuya Shinmura

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Abstract

Background: Mutations in the TP53 tumor suppressor gene are well-established drivers of colorectal cancer (CRC) development. However, data on the prevalence of TP53 variants and their association with consensus molecular subtype (CMS) classification in patients with CRC from Rwanda are currently lacking. This study addressed this knowledge gap by investigating TP53 mutation status concerning CMS classification in a CRC cohort from Rwanda.

Methods: Formalin-fixed paraffin-embedded (FFPE) tissue blocks were obtained from 51 patients with CRC at the University Teaching Hospital of Kigali, Rwanda. Exons 4 to 11 and their flanking intron-exon boundaries in the TP53 gene were sequenced using Sanger sequencing to identify potential variants. The recently established immunohistochemistry-based classifier was employed to determine the CMS of each tumor.

Results: Sequencing analysis of cancerous tissue DNA revealed TP53 pathogenic variants in 23 of 51 (45.1%) patients from Rwanda. These variants were predominantly missense types (18/23, 78.3%). The most frequent were c.455dup (p.P153Afs*28), c.524G > A (p.R175H), and c.733G > A (p.G245S), each identified in three tumors. Trinucleotide sequence context analysis of the 23 mutations (20 of which were single-base substitutions) revealed a predominance of the [C > N] pattern among single-base substitutions (SBSs) (18/20; 90.0%), with C[C > T]G being the most frequent mutation (5/18, 27.8%). Furthermore, pyrimidine bases (C and T) were preferentially found at the 5' flanking position of the mutated cytosine (13/18; 72.2%). Analysis of CMS subtypes revealed the following distribution: CMS1 (microsatellite instability-immune) (6/51, 11.8%), CMS2 (canonical) (28/51, 54.9%), CMS3 (metabolic) (9/51, 17.6%), and CMS4 (mesenchymal) (8/51, 15.7%). Interestingly, the majority of TP53 variants were in the CMS2 subgroup (14/23; 60.1%).

Conclusion: Our findings indicate a high frequency of TP53 variants in CRC patients from Rwanda. Importantly, these variants are enriched in the CMS2 subtype. This study, representing the second investigation into molecular alterations in patients with CRC from Rwanda and the first to explore TP53 mutations and CMS classification, provides valuable insights into the molecular landscape of CRC in this understudied population.

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卢旺达结直肠癌患者的 TP53 基因突变状态和分子亚型共识。

背景：TP53 抑癌基因的突变是结直肠癌（CRC）发病的公认驱动因素。然而，目前尚缺乏有关卢旺达 CRC 患者中 TP53 变异的发生率及其与共识分子亚型（CMS）分类的关系的数据。本研究通过调查卢旺达 CRC 队列中与 CMS 分类相关的 TP53 突变状态，填补了这一知识空白：方法：从卢旺达基加利大学教学医院的 51 名 CRC 患者身上获得了福尔马林固定石蜡包埋（FFPE）组织块。采用桑格测序法对 TP53 基因的第 4 至 11 号外显子及其侧翼的内含子-外显子边界进行了测序，以确定潜在的变异。采用最近建立的基于免疫组化的分类器来确定每个肿瘤的 CMS：癌症组织 DNA 的测序分析显示，卢旺达 51 名患者中有 23 人（45.1%）存在 TP53 致病变异。这些变异主要是错义类型（18/23，78.3%）。最常见的变异是 c.455dup (p.P153Afs*28)、c.524G > A (p.R175H) 和 c.733G > A (p.G245S)，每个变异都在三个肿瘤中发现。对 23 个突变（其中 20 个为单碱基置换）的三核苷酸序列上下文分析表明，在单碱基置换（SBS）中，[C > N]模式占主导地位（18/20；90.0%），C[C > T]G 是最常见的突变（5/18，27.8%）。此外，嘧啶碱基（C 和 T）优先出现在突变胞嘧啶的 5' 侧翼位置（13/18；72.2%）。对 CMS 亚型的分析显示了以下分布情况：CMS1（微卫星不稳定性-免疫）（6/51，11.8%）、CMS2（典型）（28/51，54.9%）、CMS3（代谢）（9/51，17.6%）和CMS4（间质）（8/51，15.7%）。有趣的是，大多数 TP53 变体出现在 CMS2 亚组（14/23；60.1%）：我们的研究结果表明，卢旺达的 CRC 患者中 TP53 变异的频率很高。结论：我们的研究结果表明，卢旺达的 CRC 患者中 TP53 变异的频率很高，重要的是，这些变异富集在 CMS2 亚型中。这项研究是对卢旺达 CRC 患者分子改变的第二次调查，也是对 TP53 变异和 CMS 分类的首次探索，为了解这一研究不足人群的 CRC 分子状况提供了有价值的见解。

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

BMC Cancer 医学-肿瘤学

CiteScore

6.00

自引率

2.60%

发文量

1204

审稿时长

6.8 months

期刊介绍： BMC Cancer is an open access, peer-reviewed journal that considers articles on all aspects of cancer research, including the pathophysiology, prevention, diagnosis and treatment of cancers. The journal welcomes submissions concerning molecular and cellular biology, genetics, epidemiology, and clinical trials.