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首页> 外文期刊>Analytical chemistry >Measuring Remodeling of the Lipid Environment Surrounding Membrane Proteins with Lipid Exchange and Native Mass Spectrometry
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Measuring Remodeling of the Lipid Environment Surrounding Membrane Proteins with Lipid Exchange and Native Mass Spectrometry

机译:用脂质交换和天然质谱法测量膜蛋白周围膜蛋白质的重塑

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摘要

Due to their crucial biochemical roles, membrane proteins are important drug targets. Although it is clear that lipids can influence membrane protein function, the chemistry of lipid binding remains difficult to study because protein-lipid interactions are polydisperse, competitive, and transient. Furthermore, detergents, which are often used to solubilize membrane proteins in micelles, may disrupt lipid interactions that occur in bilayers. Here, we present two new approaches to quantify protein-lipid interactions in bilayers and understand how membrane proteins remodel their surrounding lipid environment. First, we used mass spectrometry (MS) to measure the exchange of lipids between lipoprotein nanodiscs with and without an embedded membrane protein. Shifts in the lipid distribution toward the membrane protein nanodiscs revealed lipid binding, and titrations allowed measurement of the optimal lipid composition for the membrane protein. Second, we used native or nondenaturing MS to ionize membrane protein nanodiscs with heterogeneous lipids. Ejecting the membrane protein complex with bound lipids in the mass spectrometer revealed enrichment of specific lipids around the membrane protein. Both new approaches showed that the E. coli ammonium transporter AmtB prefers phosphatidylglycerol lipids overall but has a minor affinity for phosphatidylcholine lipids.
机译:由于它们至关重要的生物化学作用,膜蛋白是重要的药物靶标。虽然很明显,脂质可以影响膜蛋白质功能,但脂质结合的化学仍然难以研究,因为蛋白质 - 脂质相互作用是多分散,竞争和瞬态。此外,通常用于溶解胶束中膜蛋白的洗涤剂可能破坏双层发生的脂质相互作用。在这里,我们提出了两种新方法来量化双层蛋白 - 脂质相互作用,并了解膜蛋白如何改造它们周围的脂质环境。首先,我们使用质谱(MS)测量脂蛋白纳米蛋白与嵌入膜蛋白的脂蛋白纳米蛋白之间的脂质交换。在膜蛋白纳米乳蛋白纳米蛋白的脂质分布中的偏移显示脂质结合,滴定允许测量膜蛋白的最佳脂质组合物。其次,我们使用本机或非生物的MS与非均相脂质电离膜蛋白纳米蛋白。用质谱仪中的结合脂质喷射膜蛋白络合物,揭示了膜蛋白周围的特异性脂质的富集。这两种新方法都表明,大肠杆菌铵转运蛋白AMTB整体地优先磷酸三甘油脂质,但对磷脂酰胆碱脂质具有微小的亲和力。

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