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达利珠单抗抑制免疫的结构基础。

Structural basis of immunosuppression by the therapeutic antibody daclizumab.

机构信息

State Key Laboratory of Molecular Biology and Research Center for Structural Biology, Institute of Biochemistry and Cell Biology, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, Shanghai 200031, China.

出版信息

Cell Res. 2010 Dec;20(12):1361-71. doi: 10.1038/cr.2010.130. Epub 2010 Sep 7.

DOI:10.1038/cr.2010.130
PMID:20820193
Abstract

Interleukin-2 (IL)-2 signaling plays a pivotal role in the activation of immune responses, and drugs that block this pathway have been shown to be effective for the immunosuppression in patients with organ transplantation to alleviate/eliminate allograft rejection. The first humanized monoclonal antibody (mAb) daclizumab falls into this category and shows high specificity and affinity against a key component of the IL-2 receptor complex, namely IL-2Rα. To reveal the molecular mechanism of the inhibition of the IL-2 signaling pathway by daclizumab, we determined the crystal structures of the daclizumab Fab in free form and in complex with the IL-2Rα ectodomain at 2.6 and 2.8 Å resolution, respectively. The daclizumab Fab adopts a similar conformation in the presence or absence of the IL-2Rα ectodomain. The antigen-binding site of daclizumab is mainly composed of five complementarity determining regions (CDRs) that form a large positively charged surface depression and two flanking patches that are generally hydrophobic. The conformational epitope consists of several discontinuous segments of the IL-2Rα ectodomain, a large portion of which overlaps with the regions that interact with IL-2, suggesting that the binding of daclizumab to IL-2Rα would prevent the IL-2 binding to IL-2Rα and the subsequent formation of the IL-2/IL-2Rαβγ(c) complex, and therefore block the IL-2 signaling pathway. These results also have implications for the design and development of improved mAb drugs targeting IL-2Rα.

摘要

白细胞介素-2(IL-2)信号通路在激活免疫反应中起着关键作用,已证明阻断该途径的药物可有效抑制器官移植患者的免疫抑制作用,以减轻/消除同种异体移植物排斥反应。第一种人源化单克隆抗体(mAb)达利珠单抗属于这一类,对 IL-2 受体复合物的关键组成部分,即 IL-2Rα,具有高特异性和亲和力。为了揭示达利珠单抗抑制 IL-2 信号通路的分子机制,我们分别以 2.6 和 2.8Å的分辨率确定了游离形式和与 IL-2Rα 胞外结构域复合物形式的达利珠单抗 Fab 的晶体结构。无论是否存在 IL-2Rα 胞外结构域,达利珠单抗 Fab 均采用相似的构象。达利珠单抗的抗原结合位点主要由五个互补决定区(CDRs)组成,形成一个大的正电荷凹陷和两个侧翼补丁,通常为疏水性。构象表位由 IL-2Rα 胞外结构域的几个不连续片段组成,其中大部分与与 IL-2 相互作用的区域重叠,这表明达利珠单抗与 IL-2Rα 的结合会阻止 IL-2 与 IL-2Rα 的结合,以及随后形成的 IL-2/IL-2Rαβγ(c) 复合物,从而阻断 IL-2 信号通路。这些结果也为设计和开发针对 IL-2Rα 的改良 mAb 药物提供了启示。

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Structural basis of immunosuppression by the therapeutic antibody daclizumab.达利珠单抗抑制免疫的结构基础。
Cell Res. 2010 Dec;20(12):1361-71. doi: 10.1038/cr.2010.130. Epub 2010 Sep 7.
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The fractional excretion of soluble interleukin-2 receptor-alpha is an excellent predictor of the interleukin-2 receptor-alpha status after treatment with daclizumab.可溶性白细胞介素-2受体α的分数排泄是用达利珠单抗治疗后白细胞介素-2受体α状态的极佳预测指标。
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The use of antibodies against the IL-2 receptor in transplantation.
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[Daclizumab and basiliximab: monoclonal mouse-man antibodies with effective immunosuppression without side effects].[达利珠单抗和巴利昔单抗:具有有效免疫抑制作用且无副作用的鼠-人单克隆抗体]
Ned Tijdschr Geneeskd. 2000 Dec 9;144(50):2396-400.

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