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葡萄球菌粘附素SpsD与弹性蛋白之间分子复合物的纳米力学

Nanomechanics of the molecular complex between staphylococcal adhesin SpsD and elastin.

作者信息

Mathelié-Guinlet Marion, Chantraine Constance, Viela Felipe, Pietrocola Giampiero, Speziale Pietro, Dufrêne Yves F

机构信息

Louvain Institute of Biomolecular Science and Technology, UCLouvain, Croix du Sud, 4-5, bte L7.07.07, B-1348 Louvain-la-Neuve, Belgium.

出版信息

Nanoscale. 2020 Jul 14;12(26):13996-14003. doi: 10.1039/d0nr02745f. Epub 2020 Jun 24.

DOI:10.1039/d0nr02745f
PMID:32578656
Abstract

Staphylococcus pseudintermedius surface protein SpsD binds to extracellular matrix proteins to invade canine epithelial cells. Using single-molecule experiments, we show that SpsD engages in two modes of interaction with elastin that are tightly controlled by physical stress. Binding is weak (∼100 pN) at low tensile force (i.e. loading rate), but is dramatically enhanced (up to ∼1500 pN) by mechanical tension. Consistent with a "dock, lock, and latch" (DLL) mechanism, this force represents among the highest mechanical strengths known for a non-covalent biological interaction. The transition from weak to strong binding correlates with an increase in molecular stiffness but, surprisingly, with a decrease in molecular extension. This unanticipated mechanical behavior indicates that the adhesin is engaged in two distinct interaction mechanisms. Our results emphasize the crucial role of protein nanomechanics in the adhesion of staphylococci, and illustrate their wide diversity of force-dependent ligand-binding activities. These single-molecule mechanical experiments may contribute to the development of antiadhesion approaches to treat infections caused by S. pseudintermedius and other bacterial pathogens engaged in DLL interactions.

摘要

中间型假丝酵母表面蛋白SpsD与细胞外基质蛋白结合以侵入犬上皮细胞。通过单分子实验,我们发现SpsD与弹性蛋白存在两种相互作用模式,这两种模式受物理应力严格控制。在低拉伸力(即加载速率)下,结合力较弱(约100 pN),但通过机械张力可显著增强(高达约1500 pN)。与“对接、锁定和闩锁”(DLL)机制一致,这种力代表了已知非共价生物相互作用中最高的机械强度之一。从弱结合到强结合的转变与分子刚度的增加相关,但令人惊讶的是,与分子伸展的减少相关。这种意外的机械行为表明粘附素参与了两种不同的相互作用机制。我们的结果强调了蛋白质纳米力学在葡萄球菌粘附中的关键作用,并说明了它们在力依赖配体结合活性方面的广泛多样性。这些单分子力学实验可能有助于开发抗粘附方法,以治疗由中间型假丝酵母和其他参与DLL相互作用的细菌病原体引起的感染。

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