首页> 外文期刊>Microvascular Research: An International Journal >Extracellular angio-associated migratory cell protein plays a positive role in angiogenesis and is regulated by astrocytes in coculture.
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Extracellular angio-associated migratory cell protein plays a positive role in angiogenesis and is regulated by astrocytes in coculture.

机译:细胞外血管相关迁移细胞蛋白在血管生成中发挥积极作用,并在共培养中受到星形胶质细胞的调节。

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The extracellular form of angio-associated migratory cell protein (AAMP), a recently discovered protein, plays a positive role in angiogenesis and can be regulated by astrocytes. Angiogenic activities are inhibited by an affinity-purified, polyclonal antibody generated to recombinant AAMP. Inhibition of endothelial cell tube formation was previously shown and now endothelial cell migration assays using this antibody show dose-dependent inhibition (75%) of endothelial cell migration. Also, antisense inhibition has been used to determine the effects of reducing total AAMP (extracellular and intracellular forms). An AAMP-specific antisense oligonucleotide that targets a region near its amino terminus, anti-MES, inhibits (45%) total AAMP production by bovine aortic endothelial cells (BAECs), compared to a negative control oligonucleotide. Paradoxically, comparable use of antisense-MES results in a 27% increase in BAEC motility. Decreased cellular production of total AAMP (via antisense) that results in an increase of endothelial migration contrasts with antibody inhibition of extracellular AAMP that decreases migration. This indicates compartment-specific roles for AAMP in angiogenesis. Transwell cocultures of human astrocytes and BAECs increase (53%) the amount of extracellular AAMP found associated with endothelial cells. Therefore, regulation of extracellular AAMP by astrocytes is hypothesized to aid in angiogenesis of the nervous system. Extracellular AAMP's positive role may be either as a promoter or as a permissive protein in this process. (c)2002 Elsevier Science (USA).
机译:血管相关迁移细胞蛋白(AAMP)的细胞外形式是一种最近发现的蛋白,在血管生成中发挥积极作用,并可以由星形胶质细胞调节。通过重组AAMP产生的亲和纯化多克隆抗体抑制血管生成活性。先前已显示出对内皮细胞管形成的抑制作用,现在使用该抗体的内皮细胞迁移测定法显示出内皮细胞迁移的剂量依赖性抑制作用(75%)。而且,反义抑制已被用于确定降低总AAMP(细胞外和细胞内形式)的作用。与阴性对照寡核苷酸相比,靶向AAMP特异性反义寡核苷酸的氨基末端抗MES区域抑制了牛主动脉内皮细胞(BAEC)产生的AAMP总产量(45%)。矛盾的是,反义MES的可比使用导致BAEC活力增加了27%。降低总AAMP的细胞产量(通过反义)导致内皮迁移增加,而抗体对细胞外AAMP的抑制则降低了迁移。这表明AAMP在血管生成中的区室特异性作用。人星形胶质细胞和BAEC的Transwell共培养增加了与内皮细胞相关的细胞外AAMP的量(53%)。因此,假设星形胶质细胞对细胞外AAMP的调节有助于神经系统的血管生成。在此过程中,细胞外AAMP的积极作用可能是作为启动子或作为允许的蛋白质。 (c)2002 Elsevier Science(美国)。

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