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β整合素样蛋白介导的黏附及其在特罗斯ulus贻贝细胞培养过程中的干扰。

β Integrin-like protein-mediated adhesion and its disturbances during cell cultivation of the mussel Mytilus trossulus.

作者信息

Maiorova Mariia A, Odintsova Nelly A

机构信息

A. V. Zhirmunsky Institute of Marine Biology, Far Eastern Branch of the Russian Academy of Sciences, Palchevsky Str. 17, 690041, Vladivostok, Russia.

出版信息

Cell Tissue Res. 2015 Aug;361(2):581-92. doi: 10.1007/s00441-015-2122-y. Epub 2015 Feb 13.

Abstract

In this study, we focus on the specific contribution of β integrin-like protein to adhesion-mediated events in molluscan larval cells in culture that could not have been investigated within the whole animal. An analysis of disturbances to cell-substratum adhesion, caused by the integrin receptor inhibiting Arg-Gly-Asp-Ser (RGDS)-peptide, the Ca(2+)/Mg(2+)-chelators and the stress influence of freezing-thawing, reveals that all these factors resulted in the partial destruction of the integrin-extracellular matrix (ECM) interaction in culture and, in particular, changes in the distribution and relative abundance of β integrin-positive cells. The experiments, carried out on selected substrates, found that β integrin-positive cells demonstrate different affinities for the substrates. This finding further supports the assumption that epithelial differentiation in cultivated cells of larval Mytilus may be mediated by β integrin-like proteins via binding to laminin; direct binding to other components of the ECM could not be demonstrated. The mussel β integrin-positive cells are not involved in myogenic or neuronal differentiation on any of the substrates but part of them has tubulin-positive cilia, forming some epithelia-like structures. Our data indicate that β integrin-positive cells are able to proliferate in vitro which suggests that they could participate in renewing the digestive epithelium in larvae. The findings provide evidence that the distribution pattern of β integrin-like protein depends on the cell type and the factors influencing the adhesion.

摘要

在本研究中,我们聚焦于β整合素样蛋白对培养的软体动物幼虫细胞中黏附介导事件的特定贡献,而这在完整动物体内无法进行研究。对整合素受体抑制性精氨酸 - 甘氨酸 - 天冬氨酸 - 丝氨酸(RGDS)肽、钙/镁螯合剂以及冻融应激影响所导致的细胞与基质黏附干扰进行分析后发现,所有这些因素都会导致培养物中整合素 - 细胞外基质(ECM)相互作用的部分破坏,尤其是β整合素阳性细胞的分布和相对丰度发生变化。在选定基质上进行的实验发现,β整合素阳性细胞对不同基质表现出不同的亲和力。这一发现进一步支持了这样一种假设,即幼虫贻贝培养细胞中的上皮分化可能由β整合素样蛋白通过与层粘连蛋白结合介导;但未能证明其与ECM其他成分的直接结合。贻贝β整合素阳性细胞在任何基质上都不参与肌源性或神经源性分化,但其中一部分具有微管蛋白阳性的纤毛,形成一些上皮样结构。我们的数据表明,β整合素阳性细胞能够在体外增殖,这表明它们可能参与幼虫消化上皮的更新。这些发现提供了证据,表明β整合素样蛋白的分布模式取决于细胞类型和影响黏附的因素。

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