Snapshots of ligand entry, malleable binding and induced helical movement in P-glycoprotein

Author:

Szewczyk Paul,Tao Houchao,McGrath Aaron P.,Villaluz Mark,Rees Steven D.,Lee Sung Chang,Doshi Rupak,Urbatsch Ina L.,Zhang Qinghai,Chang Geoffrey

Abstract

P-glycoprotein (P-gp) is a transporter of great clinical and pharmacological significance. Several structural studies of P-gp and its homologs have provided insights into its transport cycle, but questions remain regarding how P-gp recognizes diverse substrates and how substrate binding is coupled to ATP hydrolysis. Here, four new P-gp co-crystal structures with a series of rationally designed ligands are presented. It is observed that the binding of certain ligands, including an ATP-hydrolysis stimulator, produces a large conformational change in the fourth transmembrane helix, which is positioned to potentially transmit a signal to the nucleotide-binding domains. A new ligand-binding site on the surface of P-gp facing the inner leaflet of the membrane is also described, providing vital insights regarding the entry mechanism of hydrophobic drugs and lipids into P-gp. These results represent significant advances in the understanding of how P-gp and related transporters bind and export a plethora of metabolites, antibiotics and clinically approved and pipeline drugs.

Publisher

International Union of Crystallography (IUCr)

Subject

General Medicine,Structural Biology

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