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Generation of anti-Notch antibodies and their application in blocking Notch signalling in neural stem cells

机译:Notch抗体的产生及其在阻断神经干细胞中Notch信号传导中的应用

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Notch signalling occurs via direct cell–cell interactions and plays an important role in linking the fates of neighbouring cells. There are four different mammalian Notch receptors that can be activated by five cell surface ligands. The ability to inhibit specific Notch receptors would help identify the roles of individual family members and potentially provide a means to study and control cell differentiation. Anti-Notch antibodies in the form of single chain Fvs were generated from an antibody phage display library by selection on either the ligand binding domain or the negative regulatory region (NRR) of Notch1 and Notch2. Six antibodies targeting the NRR of Notch1 and four antibodies recognising the NRR of Notch2 were found to prevent receptor activation in cell-based luciferase reporter assays. These antibodies were potent, highly specific inhibitors of individual Notch receptors and interfered with endogenous signalling in stem cell systems of both human and mouse origin. Antibody-mediated inhibition of Notch efficiently down-regulated transcription of the immediate Notch target gene hairy and enhancer of split 5 (Hes5) in both mouse and human neural stem cells and revealed a redundant regulation of Hes5 in these cells as complete down-regulation was seen only after simultaneous blocking of Notch1 and Notch2. In addition, these antibodies promoted differentiation of neural stem cells towards a neuronal fate. In contrast to the widely used small molecule γ-secretase inhibitors, which block all 4 Notch receptors (and a multitude of other signalling pathways), antibodies allow blockade of individual Notch family members in a highly specific way. Specific inhibition will allow examination of the effect of individual Notch receptors in complex differentiation schemes regulated by the co-ordinated action of multiple signalling pathways.
机译:Notch信号通过直接的细胞间相互作用而发生,并且在联系相邻细胞的命运方面起着重要作用。有四种不同的哺乳动物Notch受体可以被五个细胞表面配体激活。抑制特定Notch受体的能力将有助于确定单个家族成员的作用,并可能提供研究和控制细胞分化的手段。通过在Notch1和Notch2的配体结合域或负调控区(NRR)上进行选择,从抗体噬菌体展示文库中生成单链Fv形式的抗Notch抗体。在基于细胞的荧光素酶报告基因检测中,发现六种靶向Notch1的NRR的抗体和四种识别Notch2的NRR的抗体可以阻止受体激活。这些抗体是单个Notch受体的有效,高度特异性抑制剂,可干扰人类和小鼠来源的干细胞系统中的内源性信号传导。抗体介导的Notch抑制有效地下调了小鼠和人类神经干细胞中即时Notch靶基因的毛状和5分裂增强子(Hes5)的转录,并揭示了这些细胞中Hes5的冗余调节,因为完全下调是仅在同时阻止Notch1和Notch2之后才能看到。另外,这些抗体促进神经干细胞向神经元命运的分化。与广泛使用的小分子γ-分泌酶抑制剂会阻断所有4种Notch受体(以及许多其他信号传导途径)相反,抗体可以高度特异性地阻断单个Notch家族成员。特异性抑制将允许在复杂的分化方案中检查单个Notch受体的作用,该方案由多个信号通路的协同作用调节。

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