Replication and single-cycle delivery of SARS-CoV-2 replicons

SARS-CoV-2复制子的复制和单周期递送

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作者：Ricardo-Lax,Inna,Luna,Joseph M,Thao,Tran Thi Nhu,Le Pen,Jérémie,Yu,Yingpu,Hoffmann,H-Heinrich,Schneider,William M,Razooky,Brandon S,Fernandez-Martinez,Javier,Schmidt,Fabian,Weisblum,Yiska,Trüeb,Bettina Salome,Berenguer Veiga,Inês,Schmied,Kimberly,Ebert,Nadine,Michailidis,Eleftherios,Peace,Avery,Sánchez-Rivera,Francisco J,Lowe,Scott W,Rout,Michael P,Hatziioannou,Theodora,Bieniasz,Paul D,Poirier,John T,MacDonald,Margaret R,Thiel,Volker,Rice,Charles M

期刊：	Science	影响因子：	45.800
时间：	2021	起止号：	2021 Nov 26;374(6571):1099-1106
doi：	10.1126/science.abj8430	靶点：	SARS-CoV-2

Abstract

Molecular virology tools are critical for basic studies of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and for developing new therapeutics. Experimental systems that do not rely on viruses capable of spread are needed for potential use in lower-containment settings. In this work, we use a yeast-based reverse genetics system to develop spike-deleted SARS-CoV-2 self-replicating RNAs. These noninfectious self-replicating RNAs, or replicons, can be trans-complemented with viral glycoproteins to generate replicon delivery particles for single-cycle delivery into a range of cell types. This SARS-CoV-2 replicon system represents a convenient and versatile platform for antiviral drug screening, neutralization assays, host factor validation, and viral variant characterization.

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