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甲硫氨酸对大肠杆菌MetNIQ ABC转运蛋白-底物结合蛋白复合物稳定性的贡献。

The contribution of methionine to the stability of the Escherichia coli MetNIQ ABC transporter-substrate binding protein complex.

作者信息

Nguyen Phong T, Li Qi Wen, Kadaba Neena S, Lai Jeffrey Y, Yang Janet G, Rees Douglas C

出版信息

Biol Chem. 2015 Sep;396(9-10):1127-34. doi: 10.1515/hsz-2015-0131.

Abstract

Despite the ubiquitous role of ATP-binding cassette (ABC) importers in nutrient uptake, only the Escherichia coli maltose and vitamin B12 ABC transporters have been structurally characterized in multiple conformations relevant to the alternating access transport mechanism. To complement our previous structure determination of the E. coli MetNI methionine importer in the inward facing conformation (Kadaba et al. (2008) Science 321, 250-253), we have explored conditions stabilizing the outward facing conformation. Using two variants, the Walker B E166Q mutation with ATP+EDTA to stabilize MetNI in the ATP-bound conformation and the N229A variant of the binding protein MetQ, shown in this work to disrupt methionine binding, a high affinity MetNIQ complex was formed with a dissociation constant measured to be 27 nm. Using wild type MetQ containing a co-purified methionine (for which the crystal structure is reported at 1.6 Å resolution), the dissociation constant for complex formation with MetNI is measured to be ∼40-fold weaker, indicating that complex formation lowers the affinity of MetQ for methionine by this amount. Preparation of a stable MetNIQ complex is an essential step towards the crystallographic analysis of the outward facing conformation, a key intermediate in the uptake of methionine by this transport system.

摘要

尽管ATP结合盒(ABC)转运体在营养物质摄取中具有普遍作用,但只有大肠杆菌麦芽糖和维生素B12 ABC转运体在与交替通路转运机制相关的多种构象上进行了结构表征。为补充我们之前对内向构象的大肠杆菌MetNI甲硫氨酸转运体的结构测定(Kadaba等人,(2008年)《科学》321卷,250 - 253页),我们探索了稳定外向构象的条件。使用两种变体,即带有ATP + EDTA的沃克B E166Q突变以将MetNI稳定在ATP结合构象,以及结合蛋白MetQ的N229A变体(在本研究中显示其破坏甲硫氨酸结合),形成了一种高亲和力的MetNIQ复合物,其解离常数经测定为27 nM。使用含有共纯化甲硫氨酸的野生型MetQ(其晶体结构已在1.6 Å分辨率下报道),与MetNI形成复合物的解离常数经测定弱约40倍,这表明复合物的形成使MetQ对甲硫氨酸的亲和力降低了这个数量。制备稳定的MetNIQ复合物是对外向构象进行晶体学分析的关键步骤,外向构象是该转运系统摄取甲硫氨酸过程中的关键中间体。

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