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α-和β-木糖苷对体外内皮细胞形态发生相互作用的抑制作用。

Inhibition of endothelial cell morphogenetic interactions in vitro by alpha- and beta-xylosides.

作者信息

Schor A M, Schor S L

机构信息

CRC Department of Medical Oncology, Christie Hospital, Manchester, England.

出版信息

In Vitro Cell Dev Biol. 1988 Jul;24(7):659-68. doi: 10.1007/BF02623603.

DOI:10.1007/BF02623603
PMID:3397367
Abstract

Bovine aortic endothelial cells retain the ability to undergo histiotypic morphogenetic interactions in vitro as evidenced by a) the reversible expression of a sprouting cell phenotype and b) the patterned self-association of these sprouting cells into three-dimensional meshworks and tubule-like structures. These morphogenetic events are inhibited by xylosides in a dose-dependent manner. Two types of beta-xylosides (p-nitrophenyl-beta-D-xylopyranoside and 4-methylumbelliferyl-beta-D-xylopyranoside) and one alpha-xyloside (p-nitrophenyl-alpha-D-xylopyranoside) were tested. beta-xylosides are well characterized acceptors of glycosaminoglycan chains, whereas alpha-xylosides do not function in this capacity and have been extensively used as negative controls when studying the effects of beta-xylosides. Both alpha- and beta-xylosides inhibited endothelial morphogenetic interactions. This inhibition was slowly reversed during the 6- to 7-d period following removal of the xyloside. Inhibition of morphogenetic interactions by xylosides occurred at concentrations (0.5 to 2.0 mM) that had no demonstrable effects on cell proliferation, migration, or adhesion to 2-D plastic or collagen substrata. The xylosides seemed to inhibit cell spreading on a 3-D environment, they also inhibited the incorporation of [3H]-proline and Na2 35SO4 into the extracellular matrix deposited by the cells, suggesting that the inhibition of morphogenesis may be related to the inhibition of matrix deposition. Endothelial morphogenetic interactions were not inhibited by the extracellular matrix or by the conditioned medium produced by cells cultured in the presence of xylosides.

摘要

牛主动脉内皮细胞在体外仍保留进行组织型形态发生相互作用的能力,这表现为:a) 发芽细胞表型的可逆表达;b) 这些发芽细胞以模式化方式自组装成三维网络和管状结构。这些形态发生事件受到木糖苷的剂量依赖性抑制。测试了两种类型的β-木糖苷(对硝基苯基-β-D-吡喃木糖苷和4-甲基伞形酮基-β-D-吡喃木糖苷)和一种α-木糖苷(对硝基苯基-α-D-吡喃木糖苷)。β-木糖苷是糖胺聚糖链的特征明确的受体,而α-木糖苷不具备此功能,在研究β-木糖苷的作用时已被广泛用作阴性对照。α-木糖苷和β-木糖苷均抑制内皮细胞的形态发生相互作用。在去除木糖苷后的6至7天内,这种抑制作用会缓慢逆转。木糖苷对形态发生相互作用的抑制发生在对细胞增殖、迁移或对二维塑料或胶原蛋白基质的黏附没有明显影响的浓度(0.5至2.0 mM)下。木糖苷似乎抑制细胞在三维环境中的铺展,它们还抑制细胞将[3H]-脯氨酸和Na2 35SO4掺入细胞沉积的细胞外基质中,这表明形态发生的抑制可能与基质沉积的抑制有关。细胞外基质或在木糖苷存在下培养的细胞产生的条件培养基均未抑制内皮细胞的形态发生相互作用。

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本文引用的文献

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Cell proliferation and migration on collagen substrata in vitro.体外胶原蛋白基质上的细胞增殖与迁移。
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Abnormal overgrowth of chick embryos treated with p-nitrophenyl beta-D-xyloside at early stages of development.在发育早期用对硝基苯基β-D-木糖苷处理的鸡胚胎出现异常过度生长。
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Phospholipase C release of basic fibroblast growth factor from human bone marrow cultures as a biologically active complex with a phosphatidylinositol-anchored heparan sulfate proteoglycan.磷脂酶C从人骨髓培养物中释放碱性成纤维细胞生长因子,该因子以与磷脂酰肌醇锚定的硫酸乙酰肝素蛋白聚糖形成的生物活性复合物形式存在。
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Inhibition of branching morphogenesis and alteration of glycosaminoglycan biosynthesis in salivary glands treated with beta-D-xyloside.用β-D-木糖苷处理唾液腺后对分支形态发生的抑制及糖胺聚糖生物合成的改变。
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Regulation of haemopoiesis in long-term bone marrow cultures. IV. Glycosaminoglycan synthesis and the stimulation of haemopoiesis by beta-D-xylosides.长期骨髓培养中造血作用的调节。IV. 糖胺聚糖合成与β-D-木糖苷对造血作用的刺激
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Effect of p-nitrophenyl-beta-D-xyloside on proteoglycan synthesis and extracellular matrix formation by bovine corneal endothelial cell cultures.对硝基苯基-β-D-木糖苷对牛角膜内皮细胞培养物中蛋白聚糖合成及细胞外基质形成的影响
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In vitro rapid organization of endothelial cells into capillary-like networks is promoted by collagen matrices.胶原蛋白基质可促进体外内皮细胞快速组织形成毛细血管样网络。
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