FANCC Dutch founder mutation in a Mennonite family from Tamaulipas, México

Benilde García‐de Teresa; Sara Frias; Bertha Molina; María Teresa Villarreal; Alfredo Rodriguez; Alessandra Carnevale; Gerardo López‐Hernández; Lilia Vollbrechtshausen; Alberto Olaya‐Vargas; Leda Torres

doi:10.1002/mgg3.710

Molecular Genetics & Genomic Medicine (Jun 2019)

FANCC Dutch founder mutation in a Mennonite family from Tamaulipas, México

Benilde García‐de Teresa,
Sara Frias,
Bertha Molina,
María Teresa Villarreal,
Alfredo Rodriguez,
Alessandra Carnevale,
Gerardo López‐Hernández,
Lilia Vollbrechtshausen,
Alberto Olaya‐Vargas,
Leda Torres

Affiliations

Benilde García‐de Teresa: Laboratorio de Citogenética Instituto Nacional de Pediatría Ciudad de México México
Sara Frias: Laboratorio de Citogenética Instituto Nacional de Pediatría Ciudad de México México
Bertha Molina: Laboratorio de Citogenética Instituto Nacional de Pediatría Ciudad de México México
María Teresa Villarreal: Laboratorio de Enfermedades Cardiovasculares Instituto Nacional de Medicina Genómica Ciudad de México México
Alfredo Rodriguez: Laboratorio de Citogenética Instituto Nacional de Pediatría Ciudad de México México
Alessandra Carnevale: Laboratorio de Enfermedades Mendelianas Instituto Nacional de Medicina Genómica Ciudad de México México
Gerardo López‐Hernández: Servicio de Trasplante de Células Progenitoras Hematopoyéticas Instituto Nacional de Pediatría Ciudad de México México
Lilia Vollbrechtshausen: Servicio de Oncología Hospital Infantil de Tamaulipas Ciudad Victoria, Tamaulipas México
Alberto Olaya‐Vargas: Servicio de Trasplante de Células Progenitoras Hematopoyéticas Instituto Nacional de Pediatría Ciudad de México México
Leda Torres: Laboratorio de Citogenética Instituto Nacional de Pediatría Ciudad de México México

DOI: https://doi.org/10.1002/mgg3.710
Journal volume & issue: Vol. 7, no. 6
pp. n/a – n/a

Abstract

Read online

Abstract Background Fanconi anemia (FA) (OMIM #227650) is a rare hereditary disease characterized by genomic instability. The clinical phenotype involves malformations, bone marrow failure, and cancer predisposition. Genetic heterogeneity is a remarkable feature of FA; at least 22 FANC genes are known to cooperate in a unique FA/BRCA repair pathway. A common rule on the mutations found in these genes is allelic heterogeneity, except for mutations known to have arisen from a founder effect like the FANCC c.67delG in the Dutch Mennonite Community. Here, we present an 11‐year‐old male patient, member of the Mennonite Community of Tamaulipas México, with a clinical and cytogenetic diagnosis of FA. Method Chromosome fragility test was performed in all siblings. Genomic DNA was obtained from peripheral blood samples. Sanger sequencing was used to identify the FANCC c.67delG mutation (NC_000009.11(NM_000136.2):c.67delG p.(Asp23IlefsTer23)) and its accompanying haplotype. Results The FANCC c.67delG mutation in 13 members of his family confirmed a FA diagnosis in two of his siblings and identified heterozygous carriers. Haplotype analysis supports that in this family, FA is caused by the founder mutation that initially appeared in Mennonite Dutch and followed this population's migrations through Canada and further to Mexico. Conclusion The identification of the FANCC c.67delG mutation in this family not only allows proper genetic counseling, but it also grants the possibility to raise awareness of FA risk among the Mennonite community living in Mexico.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

About the journal

Abstract

Keywords