Linker domain function predicts pathogenic MLH1 missense variants.

James London Juana Martín-López Inho YangJiaquan LiuJong-Bong LeeRichard Fishel

Published in: Proceedings of the National Academy of Sciences of the United States of America (2021)

The pathogenic consequences of 369 unique human HsMLH1 missense variants has been hampered by the lack of a detailed function in mismatch repair (MMR). Here single-molecule images show that HsMSH2-HsMSH6 provides a platform for HsMLH1-HsPMS2 to form a stable sliding clamp on mismatched DNA. The mechanics of sliding clamp progression solves a significant operational puzzle in MMR and provides explicit predictions for the distribution of clinically relevant HsMLH1 missense mutations.

Keyphrases

single molecule
intellectual disability
copy number
atomic force microscopy

living cells
endothelial cells
deep learning
autism spectrum disorder

high throughput
circulating tumor
induced pluripotent stem cells

cell free
genome wide
high speed