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Fig. 1. Working models for the role of class 3 semaphorins in mouse vascular
development. (A) NRP1 contains several distinct structural domains
that cooperate to mediate binding of class 3 semaphorins and VEGF164; the a1
domain is crucial for binding the SEMA domain, the b1 domain for VEGF164
binding. (B) Based on tissue culture models, it has been suggested that
SEMA3A modulates VEGF signalling by competing with VEGF164 for binding to
NRP1. (C) SEMA3A may signal directly through complexes containing NRP1
and A-type plexins in endothelial cells, as observed in neurons. SEMA3E and
possibly other class 3 semaphorins may influence vascular development by
signalling through plexin D1-NRP1 complexes (D) and/or through plexin
D1 in a mechanism that does not require NRP1 (E). (F) VEGF164
has been implicated as a modifier of neuronal growth and axon guidance based
on its ability to compete with SEMA3A for NRP1 binding in a neuronal
progenitor cell line in vitro.
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