A novel Fanconi anaemia subtype associated with a dominant-negative mutation in RAD51

Publication date

2015-12-18

Authors

Ameziane, Najim
May, Patrick
Haitjema, Anneke
Van De Vrugt, Henri J.
Van Rossum-Fikkert, Sari E.
Ristic, Dejan
Williams, Gareth J.
Balk, J.A.
Rockx, Davy
Li, Hong

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Article
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Abstract

Fanconi anaemia (FA) is a hereditary disease featuring hypersensitivity to DNA cross-linker-induced chromosomal instability in association with developmental abnormalities, bone marrow failure and a strong predisposition to cancer. A total of 17 FA disease genes have been reported, all of which act in a recessive mode of inheritance. Here we report on a de novo g.41022153G>A; p.Ala293Thr (NM-002875) missense mutation in one allele of the homologous recombination DNA repair gene RAD51 in an FA-like patient. This heterozygous mutation causes a novel FA subtype, 'FA-Rffrt ', which appears to be the first subtype of FA caused by a dominant-negative mutation. The patient, who features microcephaly and mental retardation, has reached adulthood without the typical bone marrow failure and paediatric cancers. Together with the recent reports on RAD51-associated congenital mirror movement disorders, our results point to an important role for RAD51-mediated homologous recombination in neurodevelopment, in addition to DNA repair and cancer susceptibility.

Keywords

General Biochemistry,Genetics and Molecular Biology, General Chemistry, General Physics and Astronomy, SDG 3 - Good Health and Well-being

Citation

Ameziane, N, May, P, Haitjema, A, Van De Vrugt, H J, Van Rossum-Fikkert, S E, Ristic, D, Williams, G J, Balk, J, Rockx, D, Li, H, Rooimans, M A, Oostra, A B, Velleuer, E, Dietrich, R, Bleijerveld, O B, Altelaar, M, Meijers-Heijboer, H, Joenje, H, Glusman, G, Roach, J, Hood, L, Galas, D, Wyman, C, Balling, R, Den Dunnen, J, De Winter, J P, Kanaar, R, Gelinas, R & Dorsman, J C 2015, 'A novel Fanconi anaemia subtype associated with a dominant-negative mutation in RAD51', Nature Communications [E], vol. 6, 8829. https://doi.org/10.1038/ncomms9829