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Cell-type specific potent Wnt signaling blockade by bispecific antibody

机译:细胞型特异性强效Wnt信号传导通过双特异性抗体阻断

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Cell signaling pathways are often shared between normal and diseased cells. How to achieve cell type-specific, potent inhibition of signaling pathways is a major challenge with implications for therapeutic development. Using the Wnt/β-catenin signaling pathway as a model system, we report here a novel and generally applicable method to achieve cell type-selective signaling blockade. We constructed a bispecific antibody targeting the Wnt co-receptor LRP6 (the effector antigen) and a cell type-associated antigen (the guide antigen) that provides the targeting specificity. We found that the bispecific antibody inhibits Wnt-induced reporter activities with over one hundred-fold enhancement in potency, and in a cell type-selective manner. Potency enhancement is dependent on the expression level of the guide antigen on the target cell surface and the apparent affinity of the anti-guide antibody. Both internalizing and non-internalizing guide antigens can be used, with internalizing bispecific antibody being able to block signaling by all ligands binding to the target receptor due to its removal from the cell surface. It is thus feasible to develop bispecific-based therapeutic strategies that potently and selectively inhibit signaling pathways in a cell type-selective manner, creating opportunity for therapeutic targeting.
机译:细胞信号传导途径通常在正常和患病细胞之间共享。如何实现细胞类型特异性,对信号通路的有效抑制是对治疗发育的影响的主要挑战。使用WNT /β-Catenin信号传导路径作为模型系统,我们在此报告了一种新颖的和一般适用的方法来实现细胞类型选择性信号封锁。我们构建了靶向WNT共受体LRP6(效应抗原)的双特异性抗体和提供靶向特异性的细胞类型相关抗原(引导抗原)。我们发现双特异性抗体抑制WNT诱导的报告活动,其效力百倍增加,并以细胞类型选择性方式。效力增强取决于靶细胞表面上的引导抗原的表达水平和抗引导抗体的表观亲和力。可以使用内化和非内化指导抗原,其中内化双特异性抗体能够通过从细胞表面的去除而通过与靶受体结合的所有配体阻断信号传导。因此,可以以细胞类型选择性方式效果和选择性地抑制信号传导途径,为治疗靶向产生机会,因此可行的基于双特异性的治疗策略是可行的。

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