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RIPLET, and not TRIM25, is required for endogenous RIG‐I‐dependent antiviral responses

Immunology & Cell Biology. 2019-07; 
Thomas J Hayman Alan C Hsu Tatiana B Kolesnik Laura F Dagley Joschka Willemsen Michelle D Tate Paul J Baker Nadia J Kershaw Lukasz Kedzierski Andrew I Webb Peter A Wark Katherine Kedzierska Seth L Masters Gabrielle T Belz Marco Binder Philip M Hansbro Nicos A Nicola Sandra E Nicholson
Products/Services Used Details Operation
Custom Vector Construction … The construct encoding TRIM25 with an N- terminal Flag epitope tag (DYKDDDDK) has been described previously35.The Flag-tagged human Riplet construct was obtained from GenScript in a pcDNA 3.1 expression vector. Constructs for … Get A Quote

摘要

The innate immune system is our first line of defense against viral pathogens. Host cell pattern recognition receptors sense viral components and initiate immune signaling cascades that result in the production of an array of cytokines to combat infection. Retinoic acid–inducible gene‐I (RIG‐I) is a pattern recognition receptor that recognizes viral RNA and, when activated, results in the production of type I and III interferons (IFNs) and the upregulation of IFN‐stimulated genes. Ubiquitination of RIG‐I by the E3 ligases tripartite motif‐containing 25 (TRIM25) and Riplet is thought to be requisite for RIG‐I activation; however, recent studies have questioned the relative importance of these two e... More

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