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A genome-wide screen for human salicylic acid (SA)-binding proteins reveals targets through which SA may influence development of various diseases.

Sci Rep. 2019; 
Choi HW,, Wang L, Powell AF, Strickler SR, Wang D,, Dempsey DA, Schroeder FC, Klessig DF.
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Proteins, Expression, Isolation and Analysis The samples were then pre-cleaned with protein G agarose resin (GenScript) with rotation for 1 hr at 4 °C to remove any proteins that non-specifically bound to this resin. Get A Quote

摘要

Salicylic acid (SA) is the major metabolite and active ingredient of aspirin; both compounds reduce pain, fever, and inflammation. Despite over a century of research, aspirin/SA's mechanism(s) of action is still only partially understood. Here we report the results of a genome-wide, high-throughput screen to identify potential SA-binding proteins (SABPs) in human HEK293 cells. Following photo-affinity crosslinking to 4-azidoSA and immuno-selection with an anti-SA antibody, approximately 2,000 proteins were identified. Among these, 95 were enriched more than 10-fold. Pathway enrichment analysis with these 95 candidate SABPs (cSABPs) revealed possible involvement of SA in multiple biological pathways, including (... More

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