Biallelic inactivation of REV7 is associated with Fanconi anemia
Dominique Bluteau, … , Alan D. D’Andrea, Jean Soulier
Dominique Bluteau, … , Alan D. D’Andrea, Jean Soulier
Published August 8, 2016
Citation Information: J Clin Invest. 2016;126(9):3580-3584. https://doi.org/10.1172/JCI88010.
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Brief Report Genetics Hematology

Biallelic inactivation of REV7 is associated with Fanconi anemia

Abstract

Fanconi anemia (FA) is a recessive genetic disease characterized by congenital abnormalities, chromosome instability, progressive bone marrow failure (BMF), and a strong predisposition to cancer. Twenty FA genes have been identified, and the FANC proteins they encode cooperate in a common pathway that regulates DNA crosslink repair and replication fork stability. We identified a child with severe BMF who harbored biallelic inactivating mutations of the translesion DNA synthesis (TLS) gene REV7 (also known as MAD2L2), which encodes the mutant REV7 protein REV7-V85E. Patient-derived cells demonstrated an extended FA phenotype, which included increased chromosome breaks and G2/M accumulation upon exposure to DNA crosslinking agents, γH2AX and 53BP1 foci accumulation, and enhanced p53/p21 activation relative to cells derived from healthy patients. Expression of WT REV7 restored normal cellular and functional phenotypes in the patient’s cells, and CRISPR/Cas9 inactivation of REV7 in a non-FA human cell line produced an FA phenotype. Finally, silencing Rev7 in primary hematopoietic cells impaired progenitor function, suggesting that the DNA repair defect underlies the development of BMF in FA. Taken together, our genetic and functional analyses identified REV7 as a previously undescribed FA gene, which we term FANCV.

Authors

Dominique Bluteau, Julien Masliah-Planchon, Connor Clairmont, Alix Rousseau, Raphael Ceccaldi, Catherine Dubois d’Enghien, Olivier Bluteau, Wendy Cuccuini, Stéphanie Gachet, Régis Peffault de Latour, Thierry Leblanc, Gérard Socié, André Baruchel, Dominique Stoppa-Lyonnet, Alan D. D’Andrea, Jean Soulier

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Figure 3

CRISPR/Cas9 knockout of REV7 recapitulates the FA phenotype.

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CRISPR/Cas9 knockout of REV7 recapitulates the FA phenotype. (A) Western...
(A) Western blot of whole cell lysates shows no detectable REV7 protein in the REV7–/– line. FANCD2 is still efficiently monoubiquitylated in response to 100 ng/ml MMC. (B) Western blot showing reconstitution of WT REV7 expression in REV7–/– cells. (CD) Increase in chromosome aberrations (left graph) and radials (right) after 48-hour treatment with 20 ng/ml MMC as compared with cells complemented with WT REV7 cDNA. Original magnification, ×1,000. (E) Increase in G2/M arrest with and without MMC treatment (20 ng/ml). (F) Impaired clonogenic capacity of REV7–/– cells over 10-day treatment with MMC. (G) REV7 is required for normal hematopoiesis; CFU scoring of bone marrow Lin cells after lentiviral silencing using REV7 or scramble (scr) shRNAs. Fancg-/- cells are used as FA cell control. CFUs were numbered after 7 days on methylcellulose; 2 passages (P1 and P2) were performed. (H) Cell population percentages in CFUs after 7 days of culture.