Non-selective antagonists acting at a stable cell-cell interface have the potential to induce signaling

John, Proudfoot
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Abstract

A model, based on receptor occupancy theory, for signaling due to receptor A and co-receptor B colocalization in the presence of a stable cell-cell interface reveals that a non-selective antagonist of receptor A with affinity for a receptor C on the trans-cell can induce as well as inhibit the signal due to A. As a result, assertion of selectivity for agents acting in such a system should be supported by measurement of signal when the co-receptor B is absent. For conditions where the co-receptor B is non-functional, the model reveals the potential to rescue function through bifunctional ligands, such as bispecific antibodies, antibody conjugates or even bifunctional tethered small molecules.
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在稳定的细胞-细胞界面上发挥作用的非选择性拮抗剂有可能诱导信号传导
根据受体占位理论建立的受体 A 和共受体 B 共定位在稳定的细胞-细胞界面上产生信号的模型显示,对跨细胞上的受体 C 具有亲和力的受体 A 非选择性拮抗剂既能诱导也能抑制 A 产生的信号。对于共受体 B 无功能的情况,该模型揭示了通过双功能配体(如双特异性抗体、抗体共轭物或甚至双功能系链小分子)挽救功能的潜力。
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