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Metal Dependence and Functional Diversity of Type I Cas3 Nucleases

Biochemistry. 2022-02; 
Sining Sun, Zunyu He, Paul Jiang, Rishika Baral, Maria-Eirini Pandelia
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Codon Optimization … thioreducens (Tt) (Uniprot ID: A0A0Q2RFE4) were synthesized, codon optimized for expression in Ec, and inserted into pET26b(+) via NdeI and XhoI by GenScript (Piscataway, NJ)?… Get A Quote

摘要

Type I CRISPR-Cas systems provide prokaryotes with protection from parasitic genetic elements by cleaving foreign DNA. In addition, they impact bacterial physiology by regulating pathogenicity and virulence, making them key players in adaptability and evolution. The signature nuclease Cas3 is a phosphodiesterase belonging to the HD-domain metalloprotein superfamily. By directing specific metal incorporation, we map a promiscuous metal ion cofactor profile for Cas3 from (). Cas3 affords significant ssDNA cleavage with four homo-dimetal centers (Fe, Co, Mn, and Ni), while the diferrous form is the most active and likely biologically relevant in vivo. Electron paramagnetic resonance (EPR) spectroscopy and M?ssb... More

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