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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Sonic hedgehog mediates a novel pathway of PDGF-BB-dependent vessel maturation
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Sonic hedgehog mediates a novel pathway of PDGF-BB-dependent vessel maturation

机译:声波刺猬介导PDGF-BB依赖血管成熟的新途径

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摘要

Recruitment of mural cells (MCs), namely pericytes and smooth muscle cells (SMCs), is essential to improve the maturation of newly formed vessels. Sonic hedgehog (Shh) has been suggested to promote the formation of larger and more muscularized vessels, but the underlying mechanisms of this process have not yet been elucidated. We first identified Shh as a target of platelet-derived growth factor BB (PDGF-BB) and found that SMCs respond to Shh by upregulating extracellular signal-regulated kinase 1/2 and Akt phosphorylation. We next showed that PDGF-BB-induced SMC migration was reduced after inhibition of Shhor its signaling pathway. Moreover, we found that PDGF-BB-induced SMC migration involves Shh-mediated motility. In vivo, in the mouse model of corneal angiogenesis, Shh is expressed by MCs of newly formed blood vessels. PDGF-BB inhibition reduced Shh expression, demonstrating that Shh is a target of PDGF-BB, confirming in vitro experiments. Finally, we found that in vivo inhibition of either PDGF-BB or Shh signaling reduces NG2(+) MC recruitment into neovessels and subsequently reduces neovessel life span. Our findings demonstrate, for the first time, that Shh is involved in PDGF-BB-induced SMC migration and recruitment of MCs into neovessels and elucidate the molecular signaling pathway involved in this process.
机译:壁细胞(MC),即周细胞和平滑肌细胞(SMC)的募集对于改善新形成的血管的成熟至关重要。有人建议使用声波刺猬(Shh)来促进更大和更肌肉化的血管的形成,但尚未阐明该过程的潜在机制。我们首先确定Shh为血小板源性生长因子BB(PDGF-BB)的靶标,并发现SMC通过上调细胞外信号调节激酶1/2和Akt磷酸化来响应Shh。接下来,我们表明抑制Shhor的信号传导途径后,PDGF-BB诱导的SMC迁移减少。此外,我们发现PDGF-BB诱导的SMC迁移涉及Shh介导的运动。在体内,在角膜血管生成的小鼠模型中,Shh由新生血管的MC表达。 PDGF-BB抑制降低了Shh表达,表明Shh是PDGF-BB的靶标,从而证实了体外实验。最后,我们发现,体内对PDGF-BB或Shh信号的抑制作用会减少NG2(+)MC募集进入新血管,从而缩短新血管的寿命。我们的发现首次证明Shh参与了PDGF-BB诱导的SMC迁移以及MC募集进入新血管,并阐明了该过程涉及的分子信号传导途径。

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