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去甲氧基姜黄素是来自不同生命王国的P型ATP酶的有效抑制剂。

Demethoxycurcumin Is A Potent Inhibitor of P-Type ATPases from Diverse Kingdoms of Life.

作者信息

Dao Trong Tuan, Sehgal Pankaj, Tung Truong Thanh, Møller Jesper Vuust, Nielsen John, Palmgren Michael, Christensen Søren Brøgger, Fuglsang Anja Thoe

机构信息

Department of Plant and Environmental Sciences, University of Copenhagen, Copenhagen, Denmark.

Department of Drug Design and Pharmacology, University of Copenhagen, Copenhagen, Denmark.

出版信息

PLoS One. 2016 Sep 19;11(9):e0163260. doi: 10.1371/journal.pone.0163260. eCollection 2016.

Abstract

P-type ATPases catalyze the active transport of cations and phospholipids across biological membranes. Members of this large family are involved in a range of fundamental cellular processes. To date, a substantial number of P-type ATPase inhibitors have been characterized, some of which are used as drugs. In this work a library of natural compounds was screened and we first identified curcuminoids as plasma membrane H+-ATPases inhibitors in plant and fungal cells. We also found that some of the commercial curcumins contain several curcuminoids. Three of these were purified and, among the curcuminoids, demethoxycurcumin was the most potent inhibitor of all tested P-type ATPases from fungal (Pma1p; H+-ATPase), plant (AHA2; H+-ATPase) and animal (SERCA; Ca2+-ATPase) cells. All three curcuminoids acted as non-competitive antagonist to ATP and hence may bind to a highly conserved allosteric site of these pumps. Future research on biological effects of commercial preparations of curcumin should consider the heterogeneity of the material.

摘要

P型ATP酶催化阳离子和磷脂跨生物膜的主动运输。这个大家族的成员参与了一系列基本的细胞过程。迄今为止,大量的P型ATP酶抑制剂已被鉴定,其中一些被用作药物。在这项工作中,我们筛选了一个天然化合物库,并首次鉴定出姜黄素类化合物是植物和真菌细胞中质膜H⁺-ATP酶的抑制剂。我们还发现一些市售姜黄素含有多种姜黄素类化合物。其中三种被纯化,在所有测试的姜黄素类化合物中,去甲氧基姜黄素是真菌(Pma1p;H⁺-ATP酶)、植物(AHA2;H⁺-ATP酶)和动物(SERCA;Ca²⁺-ATP酶)细胞中所有测试的P型ATP酶最有效的抑制剂。所有三种姜黄素类化合物对ATP都起非竞争性拮抗剂的作用,因此可能与这些泵的高度保守的变构位点结合。未来关于姜黄素商业制剂生物学效应的研究应考虑该物质的异质性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22f2/5028038/f9375816230b/pone.0163260.g001.jpg

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