假肽HB-19与细胞表面核仁蛋白结合,抑制血管生成。

Q4 Neuroscience
Charalampos Birmpas, Jean Paul Briand, Josẻ Courty, Panagiotis Katsoris
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引用次数: 19

摘要

背景:核仁蛋白是肿瘤和内皮细胞表面过表达的一种蛋白。近年来的研究强调了细胞表面核蛋白在肿瘤生长和血管生成中的作用。这种细胞表面分子作为多种配体的受体,参与病理生理过程,如生长因子、细胞粘附分子如整合素、选择素或层粘连蛋白-1、脂蛋白和病毒(HIV和柯萨奇B)。HB-19是一种合成的多聚假肽,结合细胞表面表达的核蛋白,抑制肿瘤生长和血管生成。方法/主要发现:在本工作中,我们进一步研究了假肽HB-19对HUVECs的生物学作用。在之前的研究中,我们已经在鸡胚CAM实验中证明了HB-19抑制体内血管生成。我们现在提供的证据表明,HB-19在不诱导HUVECs凋亡的情况下抑制HUVECs的体外粘附、迁移和增殖。上述生物学作用似乎受到SRC、ERK1/2、AKT和FAK激酶的调控,因为我们发现HB-19在HUVECs中抑制了它们的激活。基质金属蛋白酶(Matrix metalloproteinases, MMPs)在肿瘤生长和血管生成中起着至关重要的作用,因此我们研究了HB-19对MMP-2表达的影响,发现HB-19在HUVECs中下调MMP-2的表达。最后,使用siRNA下调核仁蛋白证实了核仁蛋白在这些肽的生物学作用中的意义。结论/意义:综上所述,这些结果表明HB-19可能成为靶向细胞表面核蛋白的肿瘤治疗策略的有趣工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The pseudopeptide HB-19 binds to cell surface nucleolin and inhibits angiogenesis.

The pseudopeptide HB-19 binds to cell surface nucleolin and inhibits angiogenesis.

The pseudopeptide HB-19 binds to cell surface nucleolin and inhibits angiogenesis.

The pseudopeptide HB-19 binds to cell surface nucleolin and inhibits angiogenesis.

Background: Nucleolin is a protein over-expressed on the surface of tumor and endothelial cells. Recent studies have underlined the involvement of cell surface nucleolin in tumor growth and angiogenesis. This cell surface molecule serves as a receptor for various ligands implicated in pathophysiological processes such as growth factors, cell adhesion molecules like integrins, selectins or laminin-1, lipoproteins and viruses (HIV and coxsackie B). HB-19 is a synthetic multimeric pseudopeptide that binds cell surface expressed nucleolin and inhibits both tumor growth and angiogenesis.

Methodology/principal findings: In the present work, we further investigated the biological actions of pseudopeptide HB-19 on HUVECs. In a previous work, we have shown that HB-19 inhibits the in vivo angiogenesis on the chicken embryo CAM assay. We now provide evidence that HB-19 inhibits the in vitro adhesion, migration and proliferation of HUVECs without inducing their apoptosis. The above biological actions seem to be regulated by SRC, ERK1/2, AKT and FAK kinases as we found that HB-19 inhibits their activation in HUVECs. Matrix metalloproteinases (MMPs) play crucial roles in tumor growth and angiogenesis, so we investigated the effect of HB-19 on the expression of MMP-2 and we found that HB-19 downregulates MMP-2 in HUVECs. Finally, down regulation of nucleolin using siRNA confirmed the implication of nucleolin in the biological actions of these peptides.

Conclusions/significance: Taken together, these results indicate that HB-19 could constitute an interesting tool for tumor therapy strategy, targeting cell surface nucleolin.

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来源期刊
Vascular Cell
Vascular Cell Neuroscience-Neurology
CiteScore
0.70
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