Up-regulation of the integrin alpha 1/beta 1 in human neuroblastoma cells differentiated by retinoic acid: correlation with increased neurite outgrowth response to laminin.

P Rossino, P Defilippi, L Silengo, G Tarone
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引用次数: 99

Abstract

Retinoic acid (RA) is known to induce differentiation of neuroblastoma cells in vitro. Here we show that treatment of two human neuroblastoma cell lines, SY5Y and IMR32, with RA resulted in a fivefold increase of the integrin alpha 1/beta 1 expression. The effect was selective because expression of the alpha 3/beta 1 integrin, also present in these cells, was not increased. The up-regulation of the alpha 1/beta 1 differentiated SY5Y cells correlated with increased neurite response to laminin. In fact, RA-treated SY5Y cells elongated neurites on laminin-coated substratum more efficiently compared with untreated cells or cells treated with nerve growth factor, insulin, or phorbol 12-myristate 13-acetate. These three agents induced partial morphological differentiation but did not increase alpha 1 integrin expression. Neurite extension in RA-treated cells was more efficient on laminin than on fibronectin or collagen type I and was inhibited with beta 1 integrin antibodies on all three substrates. Affinity chromatography experiments showed that alpha 1/beta 1 is the major laminin receptor in both untreated and RA-treated SY5Y cells. These data show that RA, a naturally occurring morphogen implicated in embryonic development, can selectively regulate the expression of integrin complexes in neuronal cells and suggest an important role of the alpha 1/beta 1 laminin receptor in the morphological differentiation of nerve cells.

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视黄酸分化的人神经母细胞瘤细胞中整合素α 1/ β 1的上调:与层粘连蛋白对神经突生长反应的增加相关
已知维甲酸(RA)在体外诱导神经母细胞瘤细胞分化。在这里,我们发现用RA治疗两种人类神经母细胞瘤细胞系SY5Y和IMR32导致整合素α 1/ β 1表达增加五倍。这种效应是选择性的,因为同样存在于这些细胞中的α 3/ β 1整合素的表达没有增加。α 1/ β 1分化的SY5Y细胞的上调与神经突对层粘连蛋白的反应增加相关。事实上,与未处理的细胞或神经生长因子、胰岛素或phorbol 12-肉豆酸酯13-乙酸处理的细胞相比,ra处理的SY5Y细胞更有效地延长了层粘连蛋白包被基质上的神经突。这三种药物诱导了部分形态分化,但没有增加α 1整合素的表达。在ra处理的细胞中,神经突的延伸对层粘连蛋白比对纤维连接蛋白或I型胶原更有效,并且在所有三种底物上被β 1整合素抗体抑制。亲和层析实验表明,α 1/ β 1是未处理和ra处理的SY5Y细胞的主要层粘连蛋白受体。这些数据表明,RA是一种参与胚胎发育的自然形成的形态因子,可以选择性地调节神经元细胞中整合素复合物的表达,并提示α 1/ β 1层粘连蛋白受体在神经细胞的形态分化中起重要作用。
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