Artículo
MLH1 intronic variants mapping to + 5 position of splice donor sites lead to deleterious effects on RNA splicing
Piñero, Tamara Alejandra
; Soukarieh, Omar; Rolain, Marion; Alvarez, Karin; López Köstner, Francisco; Torrezan, Giovana Tardin; Carraro, Dirce Maria; De Oliveira Nascimento, Ivana Lucia; Bomfim, Thaís Ferreira; Machado-Lopes, Taísa Manuela Bonfim; Freitas, Juliana Côrtes; Toralles, Maria Betânia; Sandes, Kiyoko Abe; Rossi, Benedito Mauro; Junior, Samuel Aguiar; Meira, Joanna; Dominguez-Valentin, Mev; Møller, Pål; Vaccaro, Carlos Alberto; Martins, Alexandra; Pavicic, Walter Hernan
Fecha de publicación:
10/2020
Editorial:
Springer
Revista:
Familial Cancer
ISSN:
1389-9600
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
Germline pathogenic variants in the DNA mismatch repair genes (MMR): MLH1, MSH2, MSH6, and PMS2, are causative of Lynch syndrome (LS). However, many of the variants mapping outside the invariant splice site positions (IVS ± 1, IVS ± 2) are classified as variants of unknown significance (VUS). Three such variants (MLH1 c.588+5G'C, c.588+5G'T and c.677+5G'A) were identified in 8 unrelated LS families from Argentina, Brazil and Chile. Herein, we collected clinical information on these families and performed segregation analysis and RNA splicing studies to assess the implication of these VUS in LS etiology. Pedigrees showed a clear pattern of variant co-segregation with colorectal cancer and/or other LS-associated malignancies. Tumors presented deficient expression of MLH1-PMS2 proteins in 7/7 of the LS families, and MSI-high status in 3/3 cases. Moreover, RNA analyses revealed that c.588+5G'C and c.588+5G'T induce skipping of exon 7 whereas c.677+5G'A causes skipping of exon 8. In sum, we report that the combined clinical findings in the families and the molecular studies provided the evidences needed to demonstrate that the three MLH1 variants are causative of LS and to classify c.588+5G'C and c.677+5G'A as class 5 (pathogenic), and c.588+5G'T as class 4 (likely-pathogenic). Our findings underline the importance of performing clinical and family analyses, as well as RNA splicing assays in order to determine the clinical significance of intronic variants, and contribute to the genetic counseling and clinical management of patients and their relatives.
Archivos asociados
Licencia
Identificadores
Colecciones
Articulos (IMTIB)
Articulos de INSTITUTO DE MEDICINA TRASLACIONAL E INGENIERIA BIOMEDICA
Articulos de INSTITUTO DE MEDICINA TRASLACIONAL E INGENIERIA BIOMEDICA
Citación
Piñero, Tamara Alejandra; Soukarieh, Omar; Rolain, Marion; Alvarez, Karin; López Köstner, Francisco; et al.; MLH1 intronic variants mapping to + 5 position of splice donor sites lead to deleterious effects on RNA splicing; Springer; Familial Cancer; 19; 4; 10-2020; 323-336
Compartir
Altmétricas