Targeted Gene Panel Sequencing Unveiled New Pathogenic Mutations in Patients With Breast Cancer

Souad Kartti; El Mehdi Bouricha; Oumaima Zarrik; Youssef Aghlallou; Chaimaa Mounjid; Rachid ELJaoudi; Lahcen Belyamani; Azeddine Ibrahimi; Basma EL khannoussi

doi:10.1177/11779322231182054

Bioinformatics and Biology Insights (Jun 2023)

Targeted Gene Panel Sequencing Unveiled New Pathogenic Mutations in Patients With Breast Cancer

Souad Kartti,
El Mehdi Bouricha,
Oumaima Zarrik,
Youssef Aghlallou,
Chaimaa Mounjid,
Rachid ELJaoudi,
Lahcen Belyamani,
Azeddine Ibrahimi,
Basma EL khannoussi

Affiliations

Souad Kartti: Mohammed VI Center for Research and Innovation, Rabat, Morocco
El Mehdi Bouricha: Mohammed VI Center for Research and Innovation, Rabat, Morocco
Oumaima Zarrik: Biotechnology Lab (MedBiotech), Bioinova Research Center, Rabat Medical & Pharmacy School, Mohammed V University in Rabat, Rabat, Morocco
Youssef Aghlallou: Institute for Research in Cancer, Fes, Morocco
Chaimaa Mounjid: Pathology Department, Oncology National Institute, Rabat Medical and Pharmacy School, Mohammed V University in Rabat, Rabat, Morocco
Rachid ELJaoudi: Emergency Department, Military Hospital Mohammed V, Rabat, Morocco
Lahcen Belyamani: Mohammed VI University of Health Sciences, Casablanca, Morocco
Azeddine Ibrahimi: Mohammed VI University of Health Sciences, Casablanca, Morocco
Basma EL khannoussi: Pathology Department, Oncology National Institute, Rabat Medical and Pharmacy School, Mohammed V University in Rabat, Rabat, Morocco

DOI: https://doi.org/10.1177/11779322231182054
Journal volume & issue: Vol. 17

Abstract

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The increasing commercialization of new gene panels based on next-generation sequencing for clinical research has significantly improved our understanding of breast cancer genetics and has led to the discovery of new mutation variants. The study included 16 unselected Moroccan breast cancer patients tested with multi-gene panel (HEVA screen panel) using Illumina Miseq, followed by Sanger sequencing to validate the most relevant mutation. Mutational analysis revealed the presence of 13 mutations (11 single-nucleotide polymorphisms [SNPs] and 2 indels), and 6 of 11 identified SNPs were predicted as pathogenic. One of the 6 pathogenic mutations was c.7874G>C, a heterozygous SNP in HD-OB domain of BRCA2 gene, which led to the arginine to threonine change at codon 2625 of the protein. This work describes the first case of a patient with breast cancer harboring this pathogenic variant and analyzes its functional impact using molecular docking and molecular dynamics simulation. Further experimental investigations are needed to validate its pathogenicity and to verify its association with breast cancer.

Published in Bioinformatics and Biology Insights

ISSN: 1177-9322 (Online)
Publisher: SAGE Publishing
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General)
Website: https://journals.sagepub.com/home/bbi

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