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葡萄球菌主要自溶素的重复结构对于与人类血小板反应蛋白 1 和玻连蛋白的相互作用是必不可少的。

Repeating structures of the major staphylococcal autolysin are essential for the interaction with human thrombospondin 1 and vitronectin.

机构信息

From the Department of Genetics of Microorganisms and.

出版信息

J Biol Chem. 2014 Feb 14;289(7):4070-82. doi: 10.1074/jbc.M113.521229. Epub 2013 Dec 26.

Abstract

Human thrombospondin 1 (hTSP-1) is a matricellular glycoprotein facilitating bacterial adherence to and invasion into eukaryotic cells. However, the bacterial adhesin(s) remain elusive. In this study, we show a dose-dependent binding of soluble hTSP-1 to Gram-positive but not Gram-negative bacteria. Diminished binding of soluble hTSP-1 to proteolytically pretreated staphylococci suggested a proteinaceous nature of potential bacterial adhesin(s) for hTSP-1. A combination of separation of staphylococcal surface proteins by two-dimensional gel electrophoresis with a ligand overlay assay with hTSP-1 and identification of the target protein by mass spectrometry revealed the major staphylococcal autolysin Atl as a bacterial binding protein for hTSP-1. Binding experiments with heterologously expressed repeats of the AtlE amidase from Staphylococcus epidermidis suggest that the repeating sequences (R1ab-R2ab) of the N-acetyl-muramoyl-L-alanine amidase of Atl are essential for binding of hTSP-1. Atl has also been identified previously as a staphylococcal vitronectin (Vn)-binding protein. Similar to the interaction with hTSP-1, the R1ab-R2ab repeats of Atl are shown here to be crucial for the interaction of Atl with the complement inhibition and matrix protein Vn. Competition assays with hTSP-1 and Vn revealed the R1ab-R2ab repeats of AtlE as the common binding domain for both host proteins. Furthermore, Vn competes with hTSP-1 for binding to Atl repeats and vice versa. In conclusion, this study identifies the Atl repeats as bacterial adhesive structures interacting with the human glycoproteins hTSP-1 and Vn. Finally, this study provides insight into the molecular interplay between hTSP-1 and Vn, respectively, and a bacterial autolysin.

摘要

人血栓反应蛋白 1(hTSP-1)是一种基质细胞糖蛋白,可促进细菌黏附并侵入真核细胞。然而,细菌黏附素仍未被发现。在这项研究中,我们发现可溶性 hTSP-1 与革兰氏阳性菌呈剂量依赖性结合,但与革兰氏阴性菌不结合。可溶性 hTSP-1 与经蛋白水解预处理的葡萄球菌结合减少表明潜在的细菌黏附素(s)具有蛋白质性质。通过二维凝胶电泳分离葡萄球菌表面蛋白与 hTSP-1 的配体覆盖测定相结合,并用质谱法鉴定靶蛋白,发现主要的葡萄球菌自溶素 Atl 是 hTSP-1 的细菌结合蛋白。与表皮葡萄球菌 AtlE 酰胺酶的异源表达重复进行的结合实验表明,Atl 的 N-乙酰基-胞壁酰-L-丙氨酸酰胺酶的重复序列(R1ab-R2ab)对于结合 hTSP-1 是必需的。Atl 也以前被鉴定为葡萄球菌纤连蛋白(Vn)结合蛋白。与与 hTSP-1 的相互作用类似,Atl 的 R1ab-R2ab 重复序列在此显示对于 Atl 与补体抑制和基质蛋白 Vn 的相互作用至关重要。用 hTSP-1 和 Vn 进行竞争实验表明,AtlE 的 R1ab-R2ab 重复序列是两种宿主蛋白的共同结合域。此外,Vn 与 hTSP-1 竞争结合 Atl 重复序列,反之亦然。总之,这项研究确定了 Atl 重复序列作为与人类糖蛋白 hTSP-1 和 Vn 相互作用的细菌黏附结构。最后,这项研究为 hTSP-1 和 Vn 分别与细菌自溶素之间的分子相互作用提供了新的认识。

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