Predicting Pathogenicity of CDH1 Gene Variants in Patients with Early-onset Diffuse Gastric Cancer from Western Mexico

García-Ruvalcaba, Azaria; Rizo de la Torre, Lourdes del C.; Magaña-Torres, María T.; Prado-Montes-de-Oca, Ernesto; Ruiz-Ramírez, Andrea V.; Rangel-Villalobos, Héctor; Aguilar-Velázquez, José A.; García-Muro, Andrea M.; Sánchez-López, Josefina Y.

doi:10.24875/ric.20000470

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Revista de investigación clínica

versión On-line ISSN 2564-8896versión impresa ISSN 0034-8376

Resumen

GARCIA-RUVALCABA, Azaria et al. Predicting Pathogenicity of CDH1 Gene Variants in Patients with Early-onset Diffuse Gastric Cancer from Western Mexico. Rev. invest. clín. [online]. 2021, vol.73, n.3, pp.172-181. Epub 23-Jun-2021. ISSN 2564-8896. https://doi.org/10.24875/ric.20000470.

Background:

Early-onset diffuse gastric cancer (EODGC) occurs at or before 50 years of age. Pathogenic mutations and germline deletions in the CDH1 gene (E-cadherin) are well-documented genetic factors associated with the causes of EODGC.

Objective:

The objective of the study was to study CDH1 germline variants and their potential functional impact in patients with EODGC in a Mexican population.

Methods:

We studied seven EODGC patients from a biomedical research center in western Mexico. Variants were identified by Sanger sequencing and multiplex ligation-dependent probe amplification. The DeepSEA and SNPClinic v.1.0 software and the Ensembl (1000 Genomes Project, 1kGP) and ClinVar databases were used to predict functional single-nucleotide polymorphisms (SNPs). The genetic admixture of the Mexican patients was corroborated by 22 short tandem repeat loci genotyping and structure analysis.

Results:

We found 12 germline CDH1 variants in all EODGC patients, and all of them are considered as polymorphisms: rs34561447, rs5030625, rs16260, rs1330727101, rs28372783, rs942269593, rs3743674, rs1801552, rs34939176, rs33964119, rs3556654, and rs1801026. The prediction of regulatory SNPs in the promoter suggests a role for a retrovirus in EODGC that induces the transcription of interferon-related genes through toll-like receptor-interferon response factor 3 signaling, as three SNPs in the CDH1 promoter alter three binding sites for this transcription factor. In addition, SNPs rs28372783 and rs1801026 could alter upstream stimulatory factors 1 (USF1)/USF2-mediated telomerase-dependent lymphocyte activation in EODGC. Other interesting result is a CTCF-dependent shorter CDH1 isoform lacking exon 14, probably due to exon-skipping mediated by rs33964119.

Conclusions:

Classical pathogenic germline mutations in the CDH1 gene were not found in these 7 EODGC patients. However, the in silico approaches revealed the possible involvement of a retrovirus and a shorter E-cadherin isoform in EODGC. Nevertheless, further in vitro and in vivo assays are needed to confirm these predictions.

Palabras llave : Early-onset diffuse gastric cancer; CDH1 gene; E-cadherin; Gastric cancer; Variants; Bioinformatics.

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