Sedlak Steffen M, Schendel Leonard C, Melo Marcelo C R, Pippig Diana A, Luthey-Schulten Zaida, Gaub Hermann E, Bernardi Rafael C
Lehrstuhl für Angewandte Physik and Center for NanoScience (CeNS) , Ludwig-Maximilians-Universität München , Amalienstrasse 54 , 80799 Munich , Germany.
Nano Lett. 2019 Jun 12;19(6):3415-3421. doi: 10.1021/acs.nanolett.8b04045. Epub 2018 Oct 26.
Novel site-specific attachment strategies combined with improvements of computational resources enable new insights into the mechanics of the monovalent biotin/streptavidin complex under load and forced us to rethink the diversity of rupture forces reported in the literature. We discovered that the mechanical stability of this complex depends strongly on the geometry in which force is applied. By atomic force microscopy-based single molecule force spectroscopy we found unbinding of biotin to occur beyond 400 pN at force loading rates of 10 nN/s when monovalent streptavidin was tethered at its C-terminus. This value is about twice as high than that for N-terminal attachment. Steered molecular dynamics simulations provided a detailed picture of the mechanics of the unbinding process in the corresponding force loading geometries. Using machine learning techniques, we connected findings from hundreds of simulations to the experimental results, identifying different force propagation pathways. Interestingly, we observed that depending on force loading geometry, partial unfolding of N-terminal region of monovalent streptavidin occurs before biotin is released from the binding pocket.
新颖的位点特异性连接策略与计算资源的改进相结合,使我们能够对负载下单价生物素/链霉亲和素复合物的力学机制有新的见解,并促使我们重新思考文献中报道的断裂力的多样性。我们发现,这种复合物的机械稳定性在很大程度上取决于施加力的几何形状。通过基于原子力显微镜的单分子力谱,我们发现当单价链霉亲和素在其C端被拴系时,在10 nN/s的力加载速率下,生物素在超过400 pN时发生解离。该值约为N端连接时的两倍。定向分子动力学模拟提供了相应力加载几何形状下解离过程力学的详细图像。使用机器学习技术,我们将数百次模拟的结果与实验结果联系起来,确定了不同的力传播途径。有趣的是,我们观察到,根据力加载几何形状的不同,在生物素从结合口袋释放之前,单价链霉亲和素N端区域会发生部分展开。
