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一种伯氏疏螺旋体 LptD 同源物是通过螺旋体外膜翻转表面脂蛋白所必需的。

A Borrelia burgdorferi LptD homolog is required for flipping of surface lipoproteins through the spirochetal outer membrane.

机构信息

Department of Microbiology, Molecular Genetics and Immunology, University of Kansas School of Medicine, Kansas City, Kansas, USA.

Stowers Institute for Medical Research, Kansas City, Missouri, USA.

出版信息

Mol Microbiol. 2023 Jun;119(6):752-767. doi: 10.1111/mmi.15072. Epub 2023 May 12.

Abstract

Borrelia spirochetes are unique among diderm bacteria in their lack of lipopolysaccharide (LPS) in the outer membrane (OM) and their abundance of surface-exposed lipoproteins with major roles in transmission, virulence, and pathogenesis. Despite their importance, little is known about how surface lipoproteins are translocated through the periplasm and the OM. Here, we characterized Borrelia burgdorferi BB0838, a distant homolog of the OM LPS assembly protein LptD. Using a CRISPR interference approach, we showed that BB0838 is required for cell growth and envelope stability. Upon BB0838 knockdown, surface lipoprotein OspA was retained in the inner leaflet of the OM, as determined by its inaccessibility to in situ proteolysis but its presence in OM vesicles. The topology of the OM porin/adhesin P66 remained unaffected. Quantitative mass spectrometry of the B. burgdorferi membrane-associated proteome confirmed the selective periplasmic retention of surface lipoproteins under BB0838 knockdown conditions. Additional analysis identified a single in situ protease-accessible BB0838 peptide that mapped to a predicted β-barrel surface loop. Alphafold Multimer modeled a B. burgdorferi LptB FGCAD complex spanning the periplasm. Together, this suggests that BB0838/LptD facilitates the essential terminal step in spirochetal surface lipoprotein secretion, using an orthologous OM component of a pathway that secretes LPS in proteobacteria.

摘要

螺旋体属细菌的外膜(OM)中缺乏脂多糖(LPS),而表面暴露的脂蛋白丰富,这些脂蛋白在传播、毒力和发病机制中起主要作用,它们在厚壁菌中是独特的。尽管它们很重要,但对于表面脂蛋白如何穿过周质和 OM 进行易位知之甚少。在这里,我们对 Borrelia burgdorferi BB0838 进行了表征,它是 OM LPS 组装蛋白 LptD 的远同源物。使用 CRISPR 干扰方法,我们表明 BB0838 是细胞生长和包膜稳定性所必需的。在 BB0838 敲低后,表面脂蛋白 OspA 被保留在内膜,这是通过其不可接近原位蛋白酶解但存在于 OM 囊泡中来确定的。OM 孔蛋白/黏附素 P66 的拓扑结构不受影响。B. burgdorferi 膜相关蛋白质组的定量质谱分析证实了在 BB0838 敲低条件下表面脂蛋白的选择性周质保留。进一步的分析确定了一个单一的原位蛋白酶可及的 BB0838 肽,该肽映射到预测的β桶表面环上。Alphafold Multimer 构建了一个跨越周质的 B. burgdorferi LptB FGCAD 复合物。总的来说,这表明 BB0838/LptD 利用厚壁菌中 LPS 分泌途径的 OM 同源成分促进了螺旋体表面脂蛋白分泌的基本终末步骤。

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