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Stochastic Processes and Component Plasticity Governing DNA Mismatch Repair.

Journal of molecular biology (2018-06-05)
Jiaquan Liu, Jong-Bong Lee, Richard Fishel
要旨

DNA mismatch repair (MMR) is a DNA excision-resynthesis process that principally enhances replication fidelity. Highly conserved MutS (MSH) and MutL (MLH/PMS) homologs initiate MMR and in higher eukaryotes act as DNA damage sensors that can trigger apoptosis. MSH proteins recognize mismatched nucleotides, whereas the MLH/PMS proteins mediate multiple interactions associated with downstream MMR events including strand discrimination and strand-specific excision that are initiated at a significant distance from the mismatch. Remarkably, the biophysical functions of the MLH/PMS proteins have been elusive for decades. Here we consider recent observations that have helped to define the mechanics of MLH/PMS proteins and their role in choreographing MMR. We highlight the stochastic nature of DNA interactions that have been visualized by single-molecule analysis and the plasticity of protein complexes that employ thermal diffusion to complete the progressions of MMR.

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Sigma-Aldrich
フェニルメチルスルホニルフルオリド, ≥98.5% (GC)
Sigma-Aldrich
ペプスタチンA, microbial, ≥90% (HPLC)
Sigma-Aldrich
Nα-p-トシル-L-アルギニンメチルエステル 塩酸塩
Sigma-Aldrich
セルリティック エクスプレス
Sigma-Aldrich
シス-11-メチル-2-ドデセン酸, ≥90.0% (HPLC)