The spectrum of TP53 mutations in Rwandan patients with gastric cancer

Augustin Nzitakera; Jean Bosco Surwumwe; Ella Larissa Ndoricyimpaye; Schifra Uwamungu; Delphine Uwamariya; Felix Manirakiza; Marie Claire Ndayisaba; Gervais Ntakirutimana; Benoit Seminega; Vincent Dusabejambo; Eric Rutaganda; Placide Kamali; François Ngabonziza; Rei Ishikawa; Belson Rugwizangoga; Yuji Iwashita; Hidetaka Yamada; Kimio Yoshimura; Haruhiko Sugimura; Kazuya Shinmura

doi:10.1186/s41021-024-00302-y

Genes and Environment (Mar 2024)

The spectrum of TP53 mutations in Rwandan patients with gastric cancer

Augustin Nzitakera,
Jean Bosco Surwumwe,
Ella Larissa Ndoricyimpaye,
Schifra Uwamungu,
Delphine Uwamariya,
Felix Manirakiza,
Marie Claire Ndayisaba,
Gervais Ntakirutimana,
Benoit Seminega,
Vincent Dusabejambo,
Eric Rutaganda,
Placide Kamali,
François Ngabonziza,
Rei Ishikawa,
Belson Rugwizangoga,
Yuji Iwashita,
Hidetaka Yamada,
Kimio Yoshimura,
Haruhiko Sugimura,
Kazuya Shinmura

Affiliations

Augustin Nzitakera: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)
Jean Bosco Surwumwe: Department of Pathology, University Teaching Hospital of Kigali
Ella Larissa Ndoricyimpaye: Department of Biomedical Laboratory Sciences, School of Health Sciences, College of Medicine and Health Sciences, University of Rwanda
Schifra Uwamungu: Department of Biomedical Laboratory Sciences, School of Health Sciences, College of Medicine and Health Sciences, University of Rwanda
Delphine Uwamariya: Department of Biomedical Laboratory Sciences, School of Health Sciences, College of Medicine and Health Sciences, University of Rwanda
Felix Manirakiza: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)
Marie Claire Ndayisaba: Department of Pathology, University Teaching Hospital of Kigali
Gervais Ntakirutimana: Department of Pathology, University Teaching Hospital of Kigali
Benoit Seminega: Department of Pathology, School of Medicine and Pharmacy, College of Medicine and Health Sciences, University of Rwanda
Vincent Dusabejambo: Department of Pathology, School of Medicine and Pharmacy, College of Medicine and Health Sciences, University of Rwanda
Eric Rutaganda: Department of Pathology, School of Medicine and Pharmacy, College of Medicine and Health Sciences, University of Rwanda
Placide Kamali: Department of Pathology, School of Medicine and Pharmacy, College of Medicine and Health Sciences, University of Rwanda
François Ngabonziza: Department of Pathology, School of Medicine and Pharmacy, College of Medicine and Health Sciences, University of Rwanda
Rei Ishikawa: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)
Belson Rugwizangoga: Department of Pathology, University Teaching Hospital of Kigali
Yuji Iwashita: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)
Hidetaka Yamada: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)
Kimio Yoshimura: Department of Health Policy and Management, Keio University School of Medicine
Haruhiko Sugimura: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)
Kazuya Shinmura: Department of Tumor Pathology, Hamamatsu University School of Medicine (HUSM)

DOI: https://doi.org/10.1186/s41021-024-00302-y
Journal volume & issue: Vol. 46, no. 1
pp. 1 – 16

Abstract

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Abstract Background Gastric cancer is the sixth most frequently diagnosed cancer and third in causing cancer-related death globally. The most frequently mutated gene in human cancers is TP53, which plays a pivotal role in cancer initiation and progression. In Africa, particularly in Rwanda, data on TP53 mutations are lacking. Therefore, this study intended to obtain TP53 mutation status in Rwandan patients with gastric cancer. Results Formalin-fixed paraffin-embedded tissue blocks of 95 Rwandan patients with histopathologically proven gastric carcinoma were obtained from the University Teaching Hospital of Kigali. After DNA extraction, all coding regions of the TP53 gene and the exon–intron boundary region of TP53 were sequenced using the Sanger sequencing. Mutated TP53 were observed in 24 (25.3%) of the 95 cases, and a total of 29 mutations were identified. These TP53 mutations were distributed between exon 4 and 8 and most of them were missense mutations (19/29; 65.5%). Immunohistochemical analysis for TP53 revealed that most of the TP53 missense mutations were associated with TP53 protein accumulation. Among the 29 mutations, one was novel (c.459_477delCGGCACCCGCGTCCGCGCC). This 19-bp deletion mutation in exon 5 caused the production of truncated TP53 protein (p.G154Wfs*10). Regarding the spectrum of TP53 mutations, G:C > A:T at CpG sites was the most prevalent (10/29; 34.5%) and G:C > T:A was the second most prevalent (7/29; 24.1%). Interestingly, when the mutation spectrum of TP53 was compared to three previous TP53 mutational studies on non-Rwandan patients with gastric cancer, G:C > T:A mutations were significantly more frequent in this study than in our previous study (p = 0.013), the TCGA database (p = 0.017), and a previous study on patients from Hong Kong (p = 0.006). Even after correcting for false discovery, statistical significance was observed. Conclusions Our results suggested that TP53 G:C > T:A transversion mutation in Rwandan patients with gastric cancer is more frequent than in non-Rwandan patients with gastric cancer, indicating at an alternative etiological and carcinogenic progression of gastric cancer in Rwanda.

Published in Genes and Environment

ISSN: 1880-7062 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General): Ecology; Science: Biology (General): Genetics
Website: https://genesenvironment.biomedcentral.com/

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