Goold, R; Hamilton, J; Menneteau, T; Flower, M; Bunting, EL; Aldous, SG; Porro, A; ... Tabrizi, SJ; + view all Goold, R; Hamilton, J; Menneteau, T; Flower, M; Bunting, EL; Aldous, SG; Porro, A; Vicente, JR; Allen, ND; Wilkinson, H; Bates, GP; Sartori, AA; Thalassinos, K; Balmus, G; Tabrizi, SJ; - view fewer (2021) FAN1 controls mismatch repair complex assembly via MLH1 retention to stabilize CAG repeat expansion in Huntington's disease. Cell Reports , 36 (9) , Article 109649. 10.1016/j.celrep.2021.109649.

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Abstract

CAG repeat expansion in the HTT gene drives Huntington’s disease (HD) pathogenesis and is modulated by DNA damage repair pathways. In this context, the interaction between FAN1, a DNA-structure-specific nuclease, and MLH1, member of the DNA mismatch repair pathway (MMR), is not defined. Here, we identify a highly conserved SPYF motif at the N terminus of FAN1 that binds to MLH1. Our data support a model where FAN1 has two distinct functions to stabilize CAG repeats. On one hand, it binds MLH1 to restrict its recruitment by MSH3, thus inhibiting the assembly of a functional MMR complex that would otherwise promote CAG repeat expansion. On the other hand, it promotes accurate repair via its nuclease activity. These data highlight a potential avenue for HD therapeutics in attenuating somatic expansion.

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