Structural Biology Laboratory, The Salk Institute for Biological Studies, La Jolla, CA 92037, USA.
Proc Natl Acad Sci U S A. 2010 Jun 15;107(24):10902-7. doi: 10.1073/pnas.1001656107. Epub 2010 May 24.
NMR structural studies of membrane proteins (MP) are hampered by complications in MP expression, technical difficulties associated with the slow process of NMR spectral peak assignment, and limited distance information obtainable for transmembrane (TM) helices. To overcome the inherent challenges in the determination of MP structures, we have developed a rapid and cost-efficient strategy that combines cell-free (CF) protein synthesis, optimized combinatorial dual-isotope labeling for nearly instant resonance assignment, and fast acquisition of long-distance information using paramagnetic probes. Here we report three backbone structures for the TM domains of the three classes of Escherichia coli histidine kinase receptors (HKRs). The ArcB and QseC TM domains are both two-helical motifs, whereas the KdpD TM domain comprises a four-helical bundle with shorter second and third helices. The interhelical distances (up to 12 A) reveal weak interactions within the TM domains of all three receptors. Determined consecutively within 8 months, these structures offer insight into the abundant and underrepresented in the Protein Data Bank class of 2-4 TM crossers and demonstrate the efficiency of our CF combinatorial dual-labeling strategy, which can be applied to solve MP structures in high numbers and at a high speed. Our results greatly expand the current knowledge of HKR structure, opening the doors to studies on their widespread and pharmaceutically important bacterial signaling mechanism.
NMR 结构研究膜蛋白(MP)受到 MP 表达的复杂性、与 NMR 谱峰分配缓慢过程相关的技术难题以及可获得的跨膜(TM)螺旋有限距离信息的阻碍。为了克服 MP 结构测定中的固有挑战,我们开发了一种快速且具有成本效益的策略,该策略结合了无细胞(CF)蛋白合成、针对几乎即时共振分配的优化组合双同位素标记以及使用顺磁探针快速获取长程信息。在这里,我们报告了三种大肠杆菌组氨酸激酶受体(HKR)三类 TM 结构域的结构。ArcB 和 QseC 的 TM 结构域都是双螺旋结构,而 KdpD 的 TM 结构域则由四个螺旋组成,第二和第三个螺旋较短。螺旋之间的距离(长达 12 A)揭示了所有三种受体 TM 结构域内的弱相互作用。这些结构在 8 个月内连续确定,为大量且在蛋白质数据库中代表性不足的 2-4 TM 交叉类提供了深入了解,并展示了我们 CF 组合双标记策略的效率,该策略可应用于以高速和大量解决 MP 结构的问题。我们的结果极大地扩展了 HKR 结构的现有知识,为研究其广泛存在且具有重要药物作用的细菌信号机制开辟了道路。