A Rare <em>MSH2</em> Variant as a Candidate Marker for Lynch Syndrome II Screening in Tunisia: A Case of Diffuse Gastric Carcinoma

Maria Kabbage; Jihenne Ben Aissa-Haj; Houcemeddine Othman; Amira Jaballah-Gabteni; Sarra Laarayedh; Sahar Elouej; Mouna Medhioub; Haifa Tounsi Kettiti; Amal Khsiba; Moufida Mahmoudi; Houda BelFekih; Afifa Maaloul; Hassen Touinsi; Lamine Hamzaoui; Emna Chelbi; Sonia Abdelhak; Mohamed Samir Boubaker; Mohamed Mousaddak Azzouz

doi:10.3390/genes13081355

Genes (Jul 2022)

A Rare <em>MSH2</em> Variant as a Candidate Marker for Lynch Syndrome II Screening in Tunisia: A Case of Diffuse Gastric Carcinoma

Maria Kabbage,
Jihenne Ben Aissa-Haj,
Houcemeddine Othman,
Amira Jaballah-Gabteni,
Sarra Laarayedh,
Sahar Elouej,
Mouna Medhioub,
Haifa Tounsi Kettiti,
Amal Khsiba,
Moufida Mahmoudi,
Houda BelFekih,
Afifa Maaloul,
Hassen Touinsi,
Lamine Hamzaoui,
Emna Chelbi,
Sonia Abdelhak,
Mohamed Samir Boubaker,
Mohamed Mousaddak Azzouz

Affiliations

Maria Kabbage: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Jihenne Ben Aissa-Haj: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Houcemeddine Othman: Sydney Brenner Institute for Molecular Bioscience, University of the Witwatersrand, Johannesburg 2000, South Africa
Amira Jaballah-Gabteni: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Sarra Laarayedh: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Sahar Elouej: Marseille Medical Genetics, Aix Marseille University, INSERM, 13007 Marseille, France
Mouna Medhioub: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Haifa Tounsi Kettiti: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Amal Khsiba: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Moufida Mahmoudi: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Houda BelFekih: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Afifa Maaloul: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Hassen Touinsi: Department of Surgery, Mohamed Tahar Maamouri Hospital, Nabeul 8000, Tunisia
Lamine Hamzaoui: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Emna Chelbi: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Sonia Abdelhak: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia
Mohamed Samir Boubaker: Department of Human and Experimental Pathology, Institut Pasteur de Tunis, Tunis 1002, Tunisia
Mohamed Mousaddak Azzouz: Laboratory of Biomedical Genomics and Oncogenetics, Institut Pasteur de Tunis, Tunis EL Manar University, Tunis 1002, Tunisia

DOI: https://doi.org/10.3390/genes13081355
Journal volume & issue: Vol. 13, no. 8
p. 1355

Abstract

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Several syndromic forms of digestive cancers are known to predispose to early-onset gastric tumors such as Hereditary Diffuse Gastric Cancer (HDGC) and Lynch Syndrome (LS). LSII is an extracolonic cancer syndrome characterized by a tumor spectrum including gastric cancer (GC). In the current work, our main aim was to identify the mutational spectrum underlying the genetic predisposition to diffuse gastric tumors occurring in a Tunisian family suspected of both HDGC and LS II syndromes. We selected the index case “JI-021”, which was a woman diagnosed with a Diffuse Gastric Carcinoma and fulfilling the international guidelines for both HDGC and LSII syndromes. For DNA repair, a custom panel targeting 87 candidate genes recovering the four DNA repair pathways was used. Structural bioinformatics analysis was conducted to predict the effect of the revealed variants on the functional properties of the proteins. DNA repair genes panel screening identified two variants: a rare MSH2 c.728G>A classified as a variant with uncertain significance (VUS) and a novel FANCD2 variant c.1879G>T. The structural prediction model of the MSH2 variant and electrostatic potential calculation showed for the first time that MSH2 c.728G>A is likely pathogenic and is involved in the MSH2-MLH1 complex stability. It appears to affect the MSH2-MLH1 complex as well as DNA-complex stability. The c.1879G>T FANCD2 variant was predicted to destabilize the protein structure. Our results showed that the MSH2 p.R243Q variant is likely pathogenic and is involved in the MSH2-MLH1 complex stability, and molecular modeling analysis highlights a putative impact on the binding with MLH1 by disrupting the electrostatic potential, suggesting the revision of its status from VUS to likely pathogenic. This variant seems to be a shared variant in the Mediterranean region. These findings emphasize the importance of testing DNA repair genes for patients diagnosed with diffuse GC with suspicion of LSII and colorectal cancer allowing better clinical surveillance for more personalized medicine.

Published in Genes

ISSN: 2073-4425 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Biology (General): Genetics
Website: http://www.mdpi.com/journal/genes/

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