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首页> 外文期刊>Journal of Molecular Biology >Hydrophobic surface patches on LolA of Pseudomonas aeruginosa are essential for lipoprotein binding.
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Hydrophobic surface patches on LolA of Pseudomonas aeruginosa are essential for lipoprotein binding.

机译:铜绿假单胞菌的LolA上的疏水表面补丁对于脂蛋白结合至关重要。

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摘要

Many lipoproteins reside in the outer membrane (OM) of Gram-negative bacteria, and their biogenesis is dependent on the Lol (localization of lipoproteins) system. The periplasmic chaperone LolA accepts OM-destined lipoproteins that are released from the inner membrane by the LolCDE complex and transfers them to the OM receptor LolB. The exact nature of the LolA-lipoprotein complex is still unknown. The crystal structure of Escherichia coli LolA features an open beta-barrel covered by alpha helices that together constitute a hydrophobic cavity, which would allow the binding of one acyl chain. However, OM lipoproteins contain three acyl chains, and the stoichiometry of the LolA-lipoprotein complex is 1:1. Here we present the crystal structure of Pseudomonas aeruginosa LolA that projects clear hydrophobic surface patches. Since these patches are large enough to accommodate acyl chains, their role in lipoprotein binding was investigated. Several LolA mutant proteins were created, and their functionality was assessed by studying their capacity to release lipoproteins produced in sphaeroplasts. Interruption of the largest hydrophobic patch completely destroyed the lipoprotein-releasing capacity of LolA, while interruption of smaller patches apparently reduced efficiency. Thus, the results show a new lipoprotein transport model that places (some of) the acyl chains on the hydrophobic surface patches.
机译:许多脂蛋白驻留在革兰氏阴性细菌的外膜(OM)中,它们的生物发生取决于Lol(脂蛋白的定位)系统。周质伴侣蛋白LolA接受由LolCDE复合物从内膜释放的OM标定的脂蛋白,并将其转移至OM受体LolB。 LolA-脂蛋白复合物的确切性质仍然未知。大肠杆菌LolA的晶体结构的特征是一个开放的β桶,被α螺旋覆盖,这些螺旋共同构成一个疏水腔,这将允许一个酰基链的结合。然而,OM脂蛋白包含三个酰基链,并且LolA-脂蛋白复合物的化学计量为1:1。在这里,我们介绍铜绿假单胞菌LolA的晶体结构,投射出清晰的疏水表面补丁。由于这些补丁足够大以容纳酰基链,因此研究了它们在脂蛋白结合中的作用。创建了几种LolA突变蛋白,并通过研究其释放在球形塑料中产生的脂蛋白的能力来评估其功能。最大疏水补丁的中断完全破坏了LolA的脂蛋白释放能力,而较小补丁的中断显然降低了效率。因此,结果显示了一种新的脂蛋白运输模型,该模型将(部分)酰基链置于疏水性表面斑上。

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