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The evolutionarily conserved SLX4 protein, a key regulator of nucleases, is critical for DNA damage response. SLX4 nuclease complexes mediate repair during replication and can also resolve Holliday junctions formed during homologous recombination. Here we describe the phenotype of the Btbd12 knockout mouse, the mouse ortholog of SLX4, which recapitulates many key features of the human genetic illness Fanconi anemia. Btbd12-deficient animals are born at sub-Mendelian ratios, have greatly reduced fertility, are developmentally compromised and are prone to blood cytopenias. Btbd12(-/-) cells prematurely senesce, spontaneously accumulate damaged chromosomes and are particularly sensitive to DNA crosslinking agents. Genetic complementation reveals a crucial requirement for Btbd12 (also known as Slx4) to interact with the structure-specific endonuclease Xpf-Ercc1 to promote crosslink repair. The Btbd12 knockout mouse therefore establishes a disease model for Fanconi anemia and genetically links a regulator of nuclease incision complexes to the Fanconi anemia DNA crosslink repair pathway.

Original publication

DOI

10.1038/ng.752

Type

Journal article

Journal

Nat Genet

Publication Date

02/2011

Volume

43

Pages

147 - 152

Keywords

Animals, Cellular Senescence, Cross-Linking Reagents, DNA Damage, Fanconi Anemia, Female, Fibroblasts, Genetic Complementation Test, Hematopoietic Stem Cells, Humans, Magnetic Resonance Imaging, Male, Mice, Mice, Knockout, Recombinases