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Role of the neuropilin ligands VEGF164 and SEMA3A in neuronal and vascular patterning in the mouse

机译:神经毛素配体VEGF164和SEMA3A在小鼠中神经元和血管图案中的作用

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Blood vessels and neurons use similar guidance cues to control their behaviour during embryogenesis. The semaphorin SEMA3A was originally identified as a repulsive cue for developing axons that acts by signalling through receptor complexes containing NRP1 and A-type plexins. SEMA3A also competes with the VEGF164 isoform.of vascular endothelial growth factor for binding to NRP1 to modulate the migration of endothelial cells in vitro. Surprisingly, we have found that SEMA3A and semaphorin signalling through NRP1 were not required for blood vessel development in the mouse. Moreover, we found that there was no genetic interaction between SEMA3A and VEGF164 during vasculogenesis or angiogenesis. Our observations suggest that in vivo vascular NRP1 preferentially confers VEGF164 signals, whilst axonal NRP1 preferentially transmits SEMA3A signals.
机译:血管和神经元使用类似的指导提示来控制胚胎发生期间的行为。 Semaphorin Sema3a最初被识别为驱动提示,用于开发通过通过含有NRP1和α型红色的受体复合物发出信号传递的轴突。 SEMA3A还与VEGF164同种族竞争。血管内皮生长因子,用于结合NRP1来调节体外内皮细胞的迁移。令人惊讶的是,我们发现血管在小鼠中的血管发育不需要通过NRP1的Sema3a和信号素信号传导。此外,我们发现在血管生成或血管生成期间Sema3a和Vegf164之间没有遗传相互作用。我们的观察结果表明,在体内血管NRP1中优先赋予VEGF164信号,而轴突NRP1优先发送SEMA3A信号。

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