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Interaction between the Rev1 C-Terminal Domain and the PolD3 Subunit of Polζ Suggests a Mechanism of Polymerase Exchange upon Rev1/Polζ-Dependent Translesion Synthesis.

Biochemistry.. 2016-04; 
Pustovalova Y, Magalhães MT, D'Souza S, Rizzo AA, Korza G, Walker GC, Korzhnev DM.
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Peptide Synthesis ... sodium phosphate buffer, 100 mM NaCl, 0.5 mM EDTA, 2 mM DTT, 0.05% NaN3, 10% D2O, pH 7.0. A custom-synthesized peptide (GenScript) including the predicted RIR motif from human PolD3 (PolD3-RIR; residues 231-246; KGNMMSNFFGKAAMNK) has low solubility at ... Get A Quote

摘要

Translesion synthesis (TLS) is a mutagenic branch of cellular DNA damage tolerance that enables bypass replication over DNA lesions carried out by specialized low-fidelity DNA polymerases. The replicative bypass of most types of DNA damage is performed in a two-step process of Rev1/Polζ-dependent TLS. In the first step, a Y-family TLS enzyme, typically Polη, Polι, or Polκ, inserts a nucleotide across a DNA lesion. In the second step, a four-subunit B-family DNA polymerase Polζ (Rev3/Rev7/PolD2/PolD3 complex) extends the distorted DNA primer-template. The coordinated action of error-prone TLS enzymes is regulated through their interactions with the two scaffold proteins, the sliding clamp PCNA and the TLS p... More

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