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

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

doi:10.3390/genes13081355

Cited by 2 publications

(4 citation statements)

References 79 publications

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“…This in-frame deletion is located in the exon 4 of CHEK2 gene and predicted to lead to the loss of two amino acids, Among the selected variants, c.728G>A in MSH2 gene was identified in one breast cancer case with a family history of ovarian, gastric and lung cancers. Interestingly, this same variant was recently described in a Tunisian patient with gastric cancer that has a family history of breast, ovarian, and colon cancers (Kabbage et al, 2022). In this same study, structural bioinformatics analyses revealed that this variant is involved in the MSH2-MLH1 complex stability and may impact on the binding of MSH2 protein with MLH1 by disrupting the electrostatic potential which is suggestive of a pathogenic effect.…”

Section: Genotype Phenotype Correlation and Segregation Analysissupporting

confidence: 61%

“…Indeed, this variant, which was described in a gastric cancer patient, appears to affect the MSH2-MLH1 complex as well as DNAcomplex stability. Interestingly, both cases carrying this variant (current report & Kabbage et al, 2022) showed family history of cancer suggestive of lynch syndrome involving breast, gastric and ovarian malignancies which in turn may support the pathogenicity of the c.728G>A variant. In addition to MMR genes, we have identified a likely pathogenic splicing variant in RAD50 gene that was predicted to lead to exon skipping (c.3036+5G>A).…”

Section: Discussionsupporting

confidence: 51%

“…Nevertheless, family history of both probands were consistent with lynch syndrome tumor spectrum which in turn may support the pathogenicity of the identified variants. Among the other MMR genes, we have identified a missense variant, c.728G>A in MSH2 gene that seems to be likely pathogenic based on the findings of Kabbage et al (2022). Indeed, this variant, which was described in a gastric cancer patient, appears to affect the MSH2-MLH1 complex as well as DNAcomplex stability.…”

Section: Discussionmentioning

confidence: 95%

“…For the missense variant identified within the MSH2 gene, no further investigations were performed, as findings of the study of Kabbage et al (2022) are suggestive of a likely pathogenic effect.…”

Section: In-silico Functional Analysesmentioning

confidence: 99%

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Uncovering the clinical relevance of unclassified variants in DNA repair genes: a focus on BRCA negative Tunisian cancer families

Boujemaa,

Nouira,

Jandoubi

et al. 2024

Front. Genet.

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Introduction: Recent advances in sequencing technologies have significantly increased our capability to acquire large amounts of genetic data. However, the clinical relevance of the generated data continues to be challenging particularly with the identification of Variants of Uncertain Significance (VUSs) whose pathogenicity remains unclear. In the current report, we aim to evaluate the clinical relevance and the pathogenicity of VUSs in DNA repair genes among Tunisian breast cancer families.Methods: A total of 67 unsolved breast cancer cases have been investigated. The pathogenicity of VUSs identified within 26 DNA repair genes was assessed using different in silico prediction tools including SIFT, PolyPhen2, Align-GVGD and VarSEAK. Effects on the 3D structure were evaluated using the stability predictor DynaMut and molecular dynamics simulation with NAMD. Family segregation analysis was also performed.Results: Among a total of 37 VUSs identified, 11 variants are likely deleterious affecting ATM, BLM, CHEK2, ERCC3, FANCC, FANCG, MSH2, PMS2 and RAD50 genes. The BLM variant, c.3254dupT, is novel and seems to be associated with increased risk of breast, endometrial and colon cancer. Moreover, c.6115G>A in ATM and c.592+3A>T in CHEK2 were of keen interest identified in families with multiple breast cancer cases and their familial cosegregation with disease has been also confirmed. In addition, functional in silico analyses revealed that the ATM variant may lead to protein immobilization and rigidification thus decreasing its activity. We have also shown that FANCC and FANCG variants may lead to protein destabilization and alteration of the structure compactness which may affect FANCC and FANCG protein activity.Conclusion: Our findings revealed that VUSs in DNA repair genes might be associated with increased cancer risk and highlight the need for variant reclassification for better disease management. This will help to improve the genetic diagnosis and therapeutic strategies of cancer patients not only in Tunisia but also in neighboring countries.

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Section: Genotype Phenotype Correlation and Segregation Analysissupporting

confidence: 61%

Section: Discussionsupporting

confidence: 51%

Section: Discussionmentioning

confidence: 95%

Section: In-silico Functional Analysesmentioning

confidence: 99%

See 2 more Smart Citations

Uncovering the clinical relevance of unclassified variants in DNA repair genes: a focus on BRCA negative Tunisian cancer families

Boujemaa,

Nouira,

Jandoubi

et al. 2024

Front. Genet.

Self Cite

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In Silico Deciphering of the Potential Impact of Variants of Uncertain Significance in Hereditary Colorectal Cancer Syndromes

Fasano,

Lepore Signorile,

De Marco

et al. 2024

Cells

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Colorectal cancer (CRC) ranks third in terms of cancer incidence worldwide and is responsible for 8% of all deaths globally. Approximately 10% of CRC cases are caused by inherited pathogenic mutations in driver genes involved in pathways that are crucial for CRC tumorigenesis and progression. These hereditary mutations significantly increase the risk of initial benign polyps or adenomas developing into cancer. In recent years, the rapid and accurate sequencing of CRC-specific multigene panels by next-generation sequencing (NGS) technologies has enabled the identification of several recurrent pathogenic variants with established functional consequences. In parallel, rare genetic variants that are not characterized and are, therefore, called variants of uncertain significance (VUSs) have also been detected. The classification of VUSs is a challenging task because each amino acid has specific biochemical properties and uniquely contributes to the structural stability and functional activity of proteins. In this scenario, the ability to computationally predict the effect of a VUS is crucial. In particular, in silico prediction methods can provide useful insights to assess the potential impact of a VUS and support additional clinical evaluation. This approach can further benefit from recent advances in artificial intelligence-based technologies. In this review, we describe the main in silico prediction tools that can be used to evaluate the structural and functional impact of VUSs and provide examples of their application in the analysis of gene variants involved in hereditary CRC syndromes.

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

Cited by 2 publications

References 79 publications

Uncovering the clinical relevance of unclassified variants in DNA repair genes: a focus on BRCA negative Tunisian cancer families

Uncovering the clinical relevance of unclassified variants in DNA repair genes: a focus on BRCA negative Tunisian cancer families

In Silico Deciphering of the Potential Impact of Variants of Uncertain Significance in Hereditary Colorectal Cancer Syndromes

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