Genetic and Functional Analyses Point to FAN1 as the Source of Multiple Huntington Disease Modifier Effects

A recent genome-wide association study of Huntington disease (HD) implicated genes involved in DNA maintenance processes as modifiers of onset, including multiple genome-wide significant signals in a chr15 region containing the DNA repair gene Fanconi-Associated Nuclease 1 (FAN1). Here, we have carried out detailed genetic, molecular, and cellular investigation of the modifiers at this locus. We find that missense changes within or near the DNA-binding domain (p.Arg507His and p.Arg377Trp) reduce FAN1's DNA-binding activity and its capacity to rescue mitomycin C-induced cytotoxicity, accounting for two infrequent onset-hastening modifier signals.

https://www.cell.com/ajhg/fulltext/S0002-9297(20)30159-2?rss=yes

Source: The American Journal of Human Genetics - June 24, 2020 Category: Genetics & Stem Cells Authors: Kyung-Hee Kim, Eun Pyo Hong, Jun Wan Shin, Michael J. Chao, Jacob Loupe, Tammy Gillis, Jayalakshmi S. Mysore, Peter Holmans, Lesley Jones, Michael Orth, Darren G. Monckton, Jeffrey D. Long, Seung Kwak, Ramee Lee, James F. Gusella, Marcy E. MacDonald, Jong Tags: Article Source Type: research

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