Novel Candidate loci and Pathogenic Germline Variants Involved in Familial Hematological Malignancies Revealed by Whole-Exome Sequencing

Author:

Andrés-Zayas Cristina12,Suárez-González Julia12,Chicano-Lavilla María23,Bastos Oreiro Mariana23ORCID,Rodríguez-Macías Gabriela3ORCID,Font López Patricia3,Osorio Prendes Santiago3,Oarbeascoa Royuela Gillen23,García Ramírez Patricia4ORCID,Nieves Salgado Rocío5,Gómez-Centurión Ignacio23,Carbonell Muñoz Diego23ORCID,Muñiz Paula23ORCID,Kwon Mi23ORCID,Díez-Martín José Luis236,Buño Ismael1237ORCID,Martínez-Laperche Carolina23

Affiliation:

1. Genomics Unit, Gregorio Marañón General University Hospital, Gregorio Marañón Health Research Institute (IiSGM), 28009 Madrid, Spain

2. Gregorio Marañón Health Research Institute (IiSGM), 28009 Madrid, Spain

3. Department of Hematology, Gregorio Marañón General University Hospital, 28007 Madrid, Spain

4. Department of Hematology, Hospital Universitario Príncipe de Asturias, 28802 Madrid, Spain

5. Department of Hematology, Hospital Universitario Fundación Jiménez Díaz, 28040 Madrid, Spain

6. Department of Medicine, School of Medicine, Complutense University of Madrid, 28040 Madrid, Spain

7. Department of Cell Biology, School of Medicine, Complutense University of Madrid, 28040 Madrid, Spain

Abstract

The familial occurrence of hematological malignancies has been underappreciated. Recent studies suggest that up to 15% of adults with myeloid neoplasms carry germline pathogenic variants in cancer-predisposing genes. This study aimed to identify the underlying germline predisposition variant in patients with a strong family or personal onco-hematological history using whole exome sequencing on sixteen uncharacterized individuals. It was carried out in two groups of patients, one with samples available from two affected relatives (Cohort A) and one with available samples from the index case (Cohort B). In Cohort A, six families were characterized. Two families shared variants in genes associated with DNA damage response and involved in cancer development (CHEK2 and RAD54L). Pathogenic or likely pathogenic germline variants were also found in novel candidate genes (NFATC2 and TC2N). In two families, any relevant pathogenic or likely pathogenic genomic variants were identified. In Cohort B, four additional index cases were analyzed. Three of them harbor clinically relevant variants in genes with a probable role in the development of inherited forms of hematological malignancies (GATA1, MSH4 and PRF1). Overall, whole exome sequencing is a useful approach to achieve a further characterization of these patients and their mutational spectra. Moreover, further investigations may help improve optimization for disease management of affected patients and their families.

Funder

Ministry of Economy and Competitiveness

European Commission

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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