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IgGs are made for walking on bacterial and viral surfaces

机译:IgG用于在细菌和病毒表面行走

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Binding of antibodies to their cognate antigens is fundamental for adaptive immunity. Molecular engineering of antibodies for therapeutic and diagnostic purposes emerges to be one of the major technologies in combating many human diseases. Despite its importance, a detailed description of the nanomechanical process of antibody-antigen binding and dissociation on the molecular level is lacking. Here we utilize high-speed atomic force microscopy to examine the dynamics of antibody recognition and uncover a principle; antibodies do not remain stationary on surfaces of regularly spaced epitopes; they rather exhibit 'bipedal' stochastic walking. As monovalent Fab fragments do not move, steric strain is identified as the origin of short-lived bivalent binding. Walking antibodies gather in transient clusters that might serve as docking sites for the complement system and/or phagocytes. Our findings could inspire the rational design of antibodies and multivalent receptors to exploit/inhibit steric strain-induced dynamic effects.
机译:抗体与其同源抗原的结合是适应性免疫的基础。用于治疗和诊断目的的抗体分子工程学已成为对抗许多人类疾病的主要技术之一。尽管它的重要性,但缺乏在分子水平上抗体-抗原结合和解离的纳米机械过程的详细描述。在这里,我们利用高速原子力显微镜检查抗体识别的动力学并揭示原理。抗体在规则间隔的表位表面不能保持静止;他们宁愿表现出“两足动物”的随机行走。由于单价Fab片段不移动,因此将空间应变确定为短暂的二价结合的起点。步行抗体聚集在可能充当补体系统和/或吞噬细胞对接位点的瞬时簇中。我们的发现可以启发抗体和多价受体的合理设计,以开发/抑制空间菌株诱导的动态效应。

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