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抗体介导破坏稳定受体-配体复合物的定向进化和结构见解。

Directed evolution of and structural insights into antibody-mediated disruption of a stable receptor-ligand complex.

机构信息

Department of Structural Biology, Stanford University School of Medicine, Stanford, CA, 94305, USA.

Progam in Immunology, Stanford University School of Medicine, Stanford, CA, 94305, USA.

出版信息

Nat Commun. 2021 Dec 3;12(1):7069. doi: 10.1038/s41467-021-27397-z.

Abstract

Antibody drugs exert therapeutic effects via a range of mechanisms, including competitive inhibition, allosteric modulation, and immune effector mechanisms. Facilitated dissociation is an additional mechanism where antibody-mediated "disruption" of stable high-affinity macromolecular complexes can potentially enhance therapeutic efficacy. However, this mechanism is not well understood or utilized therapeutically. Here, we investigate and engineer the weak disruptive activity of an existing therapeutic antibody, omalizumab, which targets IgE antibodies to block the allergic response. We develop a yeast display approach to select for and engineer antibody disruptive efficiency and generate potent omalizumab variants that dissociate receptor-bound IgE. We determine a low resolution cryo-EM structure of a transient disruption intermediate containing the IgE-Fc, its partially dissociated receptor and an antibody inhibitor. Our results provide a conceptual framework for engineering disruptive inhibitors for other targets, insights into the failure in clinical trials of the previous high affinity omalizumab HAE variant and anti-IgE antibodies that safely and rapidly disarm allergic effector cells.

摘要

抗体药物通过多种机制发挥治疗作用,包括竞争性抑制、变构调节和免疫效应机制。促进解离是一种额外的机制,其中抗体介导的稳定高亲和力大分子复合物的“破坏”可能增强治疗效果。然而,这种机制在治疗上还没有得到很好的理解或利用。在这里,我们研究和设计了一种现有的治疗性抗体奥马珠单抗的弱破坏活性,该抗体针对 IgE 抗体以阻断过敏反应。我们开发了一种酵母展示方法来选择和设计抗体破坏效率,并生成能够解离受体结合 IgE 的强效奥马珠单抗变体。我们确定了包含 IgE-Fc、部分解离受体和抗体抑制剂的瞬时破坏中间体的低分辨率冷冻电镜结构。我们的结果为针对其他靶点设计破坏抑制剂提供了一个概念框架,深入了解以前高亲和力奥马珠单抗 HAE 变体和安全快速解除过敏效应细胞武装的抗 IgE 抗体在临床试验中失败的原因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a72/8642555/7f868ce6b293/41467_2021_27397_Fig1_HTML.jpg

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