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Initiation, extension, and termination of RNA synthesis by a paramyxovirus polymerase.

PLoS Pathog.. 2018; 
JordanPaul C,LiuCheng,RaynaudPauline,LoMichael K,SpiropoulouChristina F,SymonsJulian A,BeigelmanLeo,DevalJe
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Codon Optimization A Nanoluciferase-based NiV minigenome assay was adapted from a previously developed NiV minigenome assay [9]. Briefly, a bacteriophage T7 polymerase-based NiV minigenome was synthesized (Genscript, Piscataway, NJ) expressing a reporter fusion construct of Nanoluciferase (Promega, Madison, WI) andmNeonGreen fluorescent protein [57].The codon-optimized ORFs for the NiV L and P proteins (Bangladesh genotype, Genbank accession AY988601.1) (Genscript, Piscataway, NJ) were a gift from Michael Lo, cloned separately into pFastBac Dual expression vector. Get A Quote

摘要

Paramyxoviruses represent a family of RNA viruses causing significant human diseases. These include measles virus, the most infectious virus ever reported, in addition to parainfluenza virus, and other emerging viruses. Paramyxoviruses likely share common replication machinery but their mechanisms of RNA biosynthesis activities and details of their complex polymerase structures are unknown. Mechanistic and functional details of a paramyxovirus polymerase would have sweeping implications for understanding RNA virus replication and for the development of new antiviral medicines. To study paramyxovirus polymerase structure and function, we expressed an active recombinant Nipah virus (NiV) polymerase comple... More

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