Structural basis of noscapine activation for tubulin binding

doi:10.1021/acs.jmedchem.0c00855

Published August 13, 2020 | Version peer review

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Structural basis of noscapine activation for tubulin binding

Noscapine is a natural alkaloid that is used as an antitussive medicine. However, it also acts as a weak anticancer agent in certain in vivo models through amechanism that is largely unknown. Here, we performed structural studies and show that the cytotoxic agent 7A-O-demethoxy-amino-noscapine (7A-aminonoscapine) binds to the colchicine site of tubulin. We suggest that the 7A-methoxy group of noscapine prevents binding to tubulin due to a stericclash of the compound with the T5-loop of a-tubulin. We further propose that the anticancer activity of noscapine arises from a bioactive metabolite thatbinds to the colchicine site of tubu- lin to induce mitotic arrest through a microtubule cytoskeleton-based mechanism.

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Journal article

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Zenodo

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English

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Created: December 7, 2020
Modified: September 30, 2021

Structural basis of noscapine activation for tubulin binding

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