Merck
CN

Chemical tagging of a drug target using 5-sulfonyl tetrazole.

Bioorganic & medicinal chemistry letters (2013-02-19)
Satsuki Otsuki, Shinichi Nishimura, Hisae Takabatake, Kozue Nakajima, Yasuaki Takasu, Toru Yagura, Yuki Sakai, Akira Hattori, Hideaki Kakeya
摘要

Irreversible modification is one of the most promising strategies to identify cellular receptors of bioactive small molecules. Here we report that receptor proteins can be chemically tagged using a 5-sulfonyl tetrazole probe. 5-Sulfonyl tetrazole easily accepted nucleophilic attack of thiol groups, while 5-sulfinyl tetrazole did not. These functional groups were introduced into probe molecules of a natural product. Cyclosporine A, an immunosuppressant produced by a microbe, was derivatized to possess 5-sulfonyl tetrazole and a tag group, which enabled chemical tagging of cyclophilin A, the cellular receptor of cyclosporine A. Cyclosporine A derivative possessing 5-sulfinyl tetrazole could not tag cyclophilin A. This technique will allow efficient identification of cellular receptors of bioactive small molecules.

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Sigma-Aldrich
四唑 溶液, suitable for DNA synthesis, filtered through a 1 μm filter, ~0.45 M in acetonitrile