| Literature DB >> 30682372 |
Bing Zhang1, Jun Li2, Xiaolin Yang1, Lijie Wu3, Jia Zhang4, Yang Yang5, Yao Zhao1, Lu Zhang6, Xiuna Yang4, Xiaobao Yang4, Xi Cheng7, Zhijie Liu3, Biao Jiang4, Hualiang Jiang7, Luke W Guddat8, Haitao Yang9, Zihe Rao10.
Abstract
Despite intensive efforts to discover highly effective treatments to eradicate tuberculosis (TB), it remains as a major threat to global human health. For this reason, new TB drugs directed toward new targets are highly coveted. MmpLs (Mycobacterial membrane proteins Large), which play crucial roles in transporting lipids, polymers and immunomodulators and which also extrude therapeutic drugs, are among the most important therapeutic drug targets to emerge in recent times. Here, crystal structures of mycobacterial MmpL3 alone and in complex with four TB drug candidates, including SQ109 (in Phase 2b-3 clinical trials), are reported. MmpL3 consists of a periplasmic pore domain and a twelve-helix transmembrane domain. Two Asp-Tyr pairs centrally located in this domain appear to be key facilitators of proton-translocation. SQ109, AU1235, ICA38, and rimonabant bind inside the transmembrane region and disrupt these Asp-Tyr pairs. This structural data will greatly advance the development of MmpL3 inhibitors as new TB drugs.Entities:
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Year: 2019 PMID: 30682372 DOI: 10.1016/j.cell.2019.01.003
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582