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Effects of immobilized VEGF on endothelial progenitor cells cultured on silicon substituted and nanocrystalline hydroxyapatites

机译:固定化VEGF对硅取代和纳米晶羟基磷灰石培养的内皮祖细胞的影响

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摘要

Vascular endothelial growth factor (VEGF) plays an essential role in angiogenesis and vascular homeostasis. Endothelial progenitor cells (EPCs) are primitive bone marrow cells participating in neovascularization and revascularization processes, which also promote bone regeneration. Synthetic hydroxyapatite (HA) has been widely used in bone repair and implant coatings. In HA-based materials, small levels of ionic substitution by silicon (Si) have significant effects on osteoclastic and osteoblastic responses. Moreover, nanocrystalline hydroxyapatites (nano-HA) display enhanced bioreactivity and beneficial effects in bone formation. In this work, the angiogenic potential of VEGF-121 adsorbed on crystalline and nanocrystalline HAs with different Si proportion is evaluated with endothelial-like cells derived from EPCs cultured on nano-HA, nano-SiHA0.25, nano-SiHA0.4, HA, SiHA0.25 and SiHA0.4 disks. The Si amount incorporated for x = 0.25 is enough to yield changes in the textural parameters and surface charge without decomposing the HA phase. Si substitution for x = 0.4 does not result in pure Si-substituted apatites. Si probably remains at the grain boundaries as amorphous silica in nano-SiHA0.4 and SiHA0.4 is decomposed in alpha-TCP and HA after 1150 degrees C treatment. Immobilized VEGF on nano-HA, nano-SiHA0.25, nano-SiHA0.4, HA, SiHA0.25 and SiHA0.4 maintains its function exerting a local regulation of the cell response. The crystallite size and topography of nanocrystalline HAs could produce insufficient and weak contacts with endothelial-like cells triggering anoikis. Concerning Si proportion, the best results are obtained with SiHA0.25/VEGF and nano-SiHA0.25/VEGF disks. All these results suggest the potential utility of SiHA0.25/VEGF and nano-SiHA0.25/VEGF for bone repair and tissue engineering by promoting angiogenesis.
机译:血管内皮生长因子(VEGF)在血管生成和血管稳态中起重要作用。内皮祖细胞(EPC)是参与新血管形成和血运重建过程的原始骨髓细胞,也促进骨再生。合成羟基磷灰石(HA)已广泛用于骨修复和植入涂层。在公顷的材料中,硅(Si)的少量离子取代对破骨细胞和骨细胞反应具有显着影响。此外,纳米晶羟基磷灰石(纳米HA)显示增强的生物反应性和骨形成中的有益效果。在这项工作中,用衍生在纳米-MA,纳米SiHa0.25,Nano-Siha0.4,HA培养的EPCs的内皮样细胞,评价吸附在结晶和纳米晶体上具有不同Si比例的VEGF-121的血管生成电位。 ,siha0.25和siha0.4磁盘。 X = 0.25的Si量足以产生纹理参数和表面电荷的变化,而不会分解HA相。 X = 0.4的Si取代不会导致纯Si取代的磷灰石。 Si可能仍然在谷物边界处,作为纳米SiHa0.4和SiHa0.4中的无定形二氧化硅在1150摄氏度后在α-TCP和HA中分解。固定化VEGF在纳米-A,纳米SiHa0.25,Nano-SiHa0.4,Ha,SiHa0.25和SiHa0.4上保持其施加局部调节细胞反应的功能。纳米晶体的微晶尺寸和形貌可能产生不足和弱触点与触发Anoikis的内皮样细胞。关于SI比例,用SIHA0.25 / VEGF和纳米SIHA0.25 / VEGF盘获得最佳结果。所有这些结果表明SiHa0.25 / VEGF和Nano-SiHa0.25 / VEGF通过促进血管生成的骨修复和组织工程的潜在效用。

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  • 来源
    《RSC Advances》 |2016年第95期|共10页
  • 作者单位

    Univ Complutense Madrid Fac Chem Dept Biochem &

    Mol Biol 1 E-28040 Madrid Spain;

    Hosp Nacl Paraplej Serv Salud Castilla La Mancha Toledo Spain;

    Univ Complutense Madrid Fac Chem Dept Biochem &

    Mol Biol 1 E-28040 Madrid Spain;

    Univ Complutense Madrid Fac Chem Dept Biochem &

    Mol Biol 1 E-28040 Madrid Spain;

    Univ Complutense Madrid Fac Pharm Dept Inorgan &

    Bioinorgan Chem Inst Invest Hosp Octubre I 12 12 E-28040 Madrid Spain;

    Univ Complutense Madrid Fac Pharm Dept Inorgan &

    Bioinorgan Chem Inst Invest Hosp Octubre I 12 12 E-28040 Madrid Spain;

    Univ Complutense Madrid Fac Pharm Dept Inorgan &

    Bioinorgan Chem Inst Invest Hosp Octubre I 12 12 E-28040 Madrid Spain;

    Univ Complutense Madrid Fac Chem Dept Biochem &

    Mol Biol 1 E-28040 Madrid Spain;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学;
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