Kamil Nosol scite author profile

ABCB1 detoxifies cells by exporting diverse xenobiotic compounds, thereby limiting drug disposition and contributing to multidrug resistance in cancer cells. Multiple small-molecule inhibitors and inhibitory antibodies have been developed for therapeutic applications, but the structural basis of their activity is insufficiently understood. We determined cryo-EM structures of nanodisc-reconstituted, human ABCB1 in complex with the Fab fragment of the inhibitory, monoclonal antibody MRK16 and bound to a substrate (the antitumor drug vincristine) or to the potent inhibitors elacridar, tariquidar, or zosuquidar. We found that inhibitors bound in pairs, with one molecule lodged in the central drug-binding pocket and a second extending into a phenylalanine-rich cavity that we termed the “access tunnel.” This finding explains how inhibitors can act as substrates at low concentration, but interfere with the early steps of the peristaltic extrusion mechanism at higher concentration. Our structural data will also help the development of more potent and selective ABCB1 inhibitors.

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Structure and drug resistance of the Plasmodium falciparum transporter PfCRT

Kim

Tan

Wicht

et al. 2019

Nature

153

203

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Structure and mechanism of the ER-based glucosyltransferase ALG6

Bloch

Pesciullesi

Boilevin

et al. 2020

Nature

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Structure of human NTCP reveals the basis of recognition and sodium-driven transport of bile salts into the liver

et al. 2022

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Kamil Nosol

Cryo-EM structures reveal distinct mechanisms of inhibition of the human multidrug transporter ABCB1

Structure and drug resistance of the Plasmodium falciparum transporter PfCRT

Structure and mechanism of the ER-based glucosyltransferase ALG6

Structure of human NTCP reveals the basis of recognition and sodium-driven transport of bile salts into the liver

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