首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >PDGF-BB modulates endothelial proliferation and angiogenesis in vitro via PDGF beta-receptors
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PDGF-BB modulates endothelial proliferation and angiogenesis in vitro via PDGF beta-receptors

机译:PDGF-BB通过PDGFβ受体在体外调节内皮细胞增殖和血管生成

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摘要

To delineate potential angiogenic roles of platelet-derived growth factor (PDGF), we have investigated PDGF and its receptors on bovine aortic endothelial cells that exhibit spontaneous angiogenesis in vitro (angiogenic endothelial cells). Initiation of cord/tube formation by angiogenic endothelial cells required bovine or human serum. Neutralization of PDGF-BB in human serum with a monoclonal anti-PDGF-BB antibody reduced cord/tube formation by 37 +/- 10%, whereas neutralizing anti-PDGF-AA and an IgG isotype-matched control antibody had no effect. DNA synthesis in response to PDGF-BB increased as the cords and tubes developed; furthermore, PDGF-BB induced the incorporation of BrdU in the nuclei of cells associated with these structures. PDGF beta-receptor (PDGF-beta) mRNA increased concomitantly with cord/tube formation, and PDGFR-beta were specifically localized by immunocytochemistry to developing and mature cords and tubes. However, PDGFR-beta transcripts and protein were undetectable in nonangiogenic endothelial cells, and PDGF alpha-receptor mRNA was not expressed in either endothelial cell strain. In contrast to nonangiogenic endothelial cells, angiogenic endothelial cells did not express the PDGF B-chain, the required ligand for the PDGFR-beta. We conclude that (a) PDGF-BB can contribute to angiogenesis in vitro, (b) PDGFR-beta are specific for cord/tube-forming endothelial cells and mediate endothelial proliferation and cord/tube formation, and (c) in angiogenic and nonangiogenic endothelial cells, the expression of PDGFR- beta and PDGF B-chain is inversely correlated. We therefore suggest that paracrine PDGF might amplify angiogenesis via direct action on endothelially expressed PDGFR-beta.
机译:为了描述血小板源性生长因子(PDGF)的潜在血管生成作用,我们研究了PDGF及其在牛主动脉内皮细胞上的受体,这些受体在体外表现出自发性血管生成(血管生成内皮细胞)。由血管生成内皮细胞启动脐带/管形成需要牛或人血清。用单克隆抗PDGF-BB抗体中和人血清中的PDGF-BB可使脐带/管形成减少37 +/- 10%,而中和抗PDGF-AA和IgG同型匹配的对照抗体则无效。随着脐带和管的发育,对PDGF-BB的DNA合成增加;此外,PDGF-BB诱导了BrdU掺入与这些结构相关的细胞核中。 PDGFβ受体(PDGF-beta)mRNA随着脐带/管的形成而增加,并且PDGFR-beta通过免疫细胞化学特异地定位在发育中的和成熟的脐带和管中。但是,在非血管生成内皮细胞中检测不到PDGFR-beta转录本和蛋白质,并且在任一内皮细胞株中均未表达PDGFα-受体mRNA。与非血管生成内皮细胞相比,血管生成内皮细胞不表达PDGF B-链,PDGF B-链是必需的配体。我们得出的结论是:(a)PDGF-BB可以促进体外血管生成,(b)PDGFR-β对形成脐带/管的内皮细胞具有特异性,并介导内皮增殖和脐带/管的形成,以及(c)在血管生成和非血管生成中在内皮细胞中,PDGFR-β和PDGF B链的表达呈负相关。因此,我们建议旁分泌PDGF可能通过对内皮表达的PDGFR-β的直接作用来放大血管生成。

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