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BamA 的构象特异性标记和抑制因子分析提示了大肠杆菌中β-桶组装的循环机制。

Conformation-specific labeling of BamA and suppressor analysis suggest a cyclic mechanism for β-barrel assembly in Escherichia coli.

机构信息

Department of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Mar 26;110(13):5151-6. doi: 10.1073/pnas.1302662110. Epub 2013 Mar 11.

Abstract

In gram-negative bacteria, integral outer membrane β-barrel proteins (OMPs) are assembled by the beta-barrel assembly machine (Bam) complex. The essential components of this complex are the OMP BamA [which contains a carboxyl-terminal β-barrel and an amino-terminal periplasmic module composed of five polypeptide transport associated (POTRA) domains] and the lipoprotein BamD. In Escherichia coli, the Bam complex also contains three nonessential lipoproteins (BamBCE), all of which require the barrel-proximal POTRA domain (P5) for stable interactions with BamA. We have previously reported that the BamA β-barrel assumes two different conformations. A method for conformation-specific labeling of BamA described here reveals that these conformers reflect the degree of surface exposure of the conserved sixth extracellular loop (L6). L6 is surface accessible in one conformation but not in the other, likely because it occupies the lumen of the BamA β-barrel in the latter case. A gain-of-function mutation that promotes Bam activity (bamDR197L) and a loss-of-function mutation that decreases the activity of Bam (ΔbamE) both favor surface exposure of BamA L6, suggesting that BamD and BamE normally act to control L6 exposure through opposing functions. These results, along with the synthetic lethality of the bamDR197L ΔbamE double mutant, imply a cyclic mechanism in which the Bam lipoproteins regulate the conformation of BamA during the OMP assembly reaction. Our results further suggest that BamDE controls L6 exposure via conformational signals transmitted through P5 to L6.

摘要

在革兰氏阴性菌中,完整的外膜 β-桶状蛋白(OMP)由β-桶状组装机(Bam)复合物组装。该复合物的基本组成部分是 OMP BamA[包含羧基末端 β-桶和由五个多肽转运相关(POTRA)结构域组成的氨基末端周质模块]和脂蛋白 BamD。在大肠杆菌中,Bam 复合物还包含三种非必需的脂蛋白(BamBC),所有这些脂蛋白都需要桶状近侧 POTRA 结构域(P5)才能与 BamA 稳定相互作用。我们之前曾报道过 BamA β-桶呈现出两种不同的构象。这里描述的一种构象特异性标记 BamA 的方法表明,这些构象反映了保守的第六个细胞外环(L6)的表面暴露程度。L6 在一种构象中是可接触的,但在另一种构象中则不可接触,可能是因为在后一种情况下它占据了 BamA β-桶的内腔。促进 Bam 活性的功能获得突变(bamDR197L)和降低 Bam 活性的功能丧失突变(ΔbamE)都有利于 BamA L6 的表面暴露,这表明 BamD 和 BamE 通常通过相反的功能来控制 L6 的暴露。这些结果,以及 bamDR197L ΔbamE 双突变体的合成致死性,表明 Bam 脂蛋白在 OMP 组装反应过程中通过调节 BamA 构象的循环机制。我们的结果进一步表明,BamDE 通过通过 P5 传递到 L6 的构象信号来控制 L6 的暴露。

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