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通过化学生物学基因组学鉴定 ABCB/P-糖蛋白特异性生长素运输抑制剂。

Identification of an ABCB/P-glycoprotein-specific inhibitor of auxin transport by chemical genomics.

机构信息

Laboratory of Plant Systems Bio-Dynamics, Pohang University of Science and Technology, 790-784 Pohang, Korea.

出版信息

J Biol Chem. 2010 Jul 23;285(30):23309-17. doi: 10.1074/jbc.M110.105981. Epub 2010 May 14.

Abstract

Plant development and physiology are widely determined by the polar transport of the signaling molecule auxin. This process is controlled on the cellular efflux level catalyzed by members of the PIN (pin-formed) and ABCB (ATP-binding cassette protein subfamily B)/P-glycoprotein family that can function independently and coordinately. In this study, we have identified by means of chemical genomics a novel auxin transport inhibitor (ATI), BUM (2-[4-(diethylamino)-2-hydroxybenzoyl]benzoic acid), that efficiently blocks auxin-regulated plant physiology and development. In many respects, BUM resembles the functionality of the diagnostic ATI, 1-N-naphtylphtalamic acid (NPA), but it has an IC(50) value that is roughly a factor 30 lower. Physiological analysis and binding assays identified ABCBs, primarily ABCB1, as key targets of BUM and NPA, whereas PIN proteins are apparently not directly affected. BUM is complementary to NPA by having distinct ABCB target spectra and impacts on basipetal polar auxin transport in the shoot and root. In comparison with the recently identified ATI, gravacin, it lacks interference with ABCB membrane trafficking. Individual modes or targets of action compared with NPA are reflected by apically shifted root influx maxima that might be the result of altered BUM binding preferences or affinities to the ABCB nucleotide binding folds. This qualifies BUM as a valuable tool for auxin research, allowing differentiation between ABCB- and PIN-mediated efflux systems. Besides its obvious application as a powerful weed herbicide, BUM is a bona fide human ABCB inhibitor with the potential to restrict multidrug resistance during chemotherapy.

摘要

植物的发育和生理机能在很大程度上取决于信号分子生长素的极性运输。这一过程受到 PIN(形成针状)和 ABCB(ATP 结合盒蛋白亚家族 B)/P-糖蛋白家族成员的细胞外排水平的控制,这些成员可以独立和协调地发挥作用。在这项研究中,我们通过化学基因组学手段鉴定了一种新型生长素运输抑制剂(ATI),BUM(2-[4-(二乙氨基)-2-羟基苯甲酰]苯甲酸),它能有效地阻断生长素调节的植物生理和发育。在许多方面,BUM 类似于诊断性 ATI,1-N-萘基邻苯二甲酸(NPA),但它的 IC50 值大约低 30 倍。生理分析和结合测定将 ABCB 鉴定为 BUM 和 NPA 的关键靶点,主要是 ABCB1,而 PIN 蛋白显然没有直接受到影响。BUM 通过具有不同的 ABCB 靶标谱和对茎和根中底极性生长素运输的影响与 NPA 互补。与最近鉴定的 ATI,gravacin 相比,它缺乏对 ABCB 膜运输的干扰。与 NPA 相比,单独的作用模式或靶点表现在根的入流最大值向根尖转移,这可能是由于 BUM 结合偏好或对 ABCB 核苷酸结合折叠的亲和力发生改变所致。这使 BUM 成为生长素研究的有价值工具,允许区分 ABCB 和 PIN 介导的外排系统。除了作为一种强大的除草剂的明显应用外,BUM 还是一种真正的人类 ABCB 抑制剂,具有在化疗期间限制多药耐药的潜力。

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