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The nucleotide addition cycle of the SARS-CoV-2 polymerase

Cell Rep. 2021-08; 
Subhas Chandra Bera, Mona Seifert, Robert N Kirchdoerfer, Pauline van Nies, Yibulayin Wubulikasimu, Salina Quack, Flávia S Papini, Jamie J Arnold, Bruno Canard, Craig E Cameron, Martin Depken, David Dulin
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Codon Optimization The SARS-CoV-2?nsp12 gene was codon optimized and cloned into pFastBac with C-terminal additions of a TEV site and strep tag (Genscript) Get A Quote

摘要

Coronaviruses have evolved elaborate multisubunit machines to replicate and transcribe their genomes. Central to these machines are the RNA-dependent RNA polymerase subunit (nsp12) and its intimately associated cofactors (nsp7 and nsp8). We use a high-throughput magnetic-tweezers approach to develop a mechanochemical description of this core polymerase. The core polymerase exists in at least three catalytically distinct conformations, one being kinetically consistent with incorporation of incorrect nucleotides. We provide evidence that the RNA-dependent RNA polymerase (RdRp) uses a thermal ratchet instead of a power stroke to transition from the pre- to post-translocated state. Ultra-stable magnetic tweezers en... More

關鍵詞

SARS-CoV-2 polymerase, backtracking, high-throughput/ultra-stable magnetic tweezers, nucleotide addition cycle, polymerase mechanochemistry, single-molecule biophysics
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