首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Beta 1D integrin displaces the beta 1A isoform in striated muscles: localization at junctional structures and signaling potential in nonmuscle cells
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Beta 1D integrin displaces the beta 1A isoform in striated muscles: localization at junctional structures and signaling potential in nonmuscle cells

机译:Beta 1D整联蛋白取代了横纹肌中的beta 1A亚型:位于结点结构和非肌肉细胞中的信号传导潜力

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摘要

The cytoplasmic domains of integrins provide attachment of these extracellular matrix receptors to the cytoskeleton and play a critical role in integrin-mediated signal transduction. In this report we describe the identification, expression, localization, and initial functional characterization of a novel form of beta 1 integrin, termed beta 1D. This isoform contains a unique alternatively spliced cytoplasmic domain of 50 amino acids, with the last 24 amino acids encoded by an additional exon. Of these 24 amino acids, 11 are conserved when compared to the beta 1A isoform, but 13 are unique (Zhidkova, N. I., A. M. Belkin, and R. Mayne. 1995. Biochem. Biophys. Res. Commun. 214:279-285; van der Flier, A., I. Kuikman, C. Baudoin, R, van der Neuf, and A. Sonnenberg. 1995. FEBS Lett. 369:340-344). Using an anti-peptide antibody against the beta 1D integrin subunit, we demonstrated that the beta 1D isoform is synthesized only in skeletal and cardiac muscles, while very low amounts of beta 1A were detected by immunoblot in striated muscles. Whereas beta 1A could not be detected in adult skeletal muscle fibers and cardiomyocytes by immunofluorescence, beta 1D was localized to the sarcolemma of both cell types. In skeletal muscle, beta 1D was concentrated in costameres, myotendinous, and neuromuscular junctions. In cardiac muscle this beta 1 isoform was found in costamers and intercalated discs. beta 1D was associated with alpha 7A and alpha 7B in adult skeletal muscle. In cardiomyocytes of adult heart, alpha 7B was the major partner for the beta 1D isoform. beta 1D could not be detected in proliferating C2C12 myoblasts, but it appeared immediately after myoblast fusion and its amount continued to rise during myotube growth and maturation. In contrast, expression of the beta 1A isoform was downregulated during myodifferentiation in culture and it was completely displaced by beta 1D in mature differentiated myotubes. We also analyzed some functional properties of the beta 1D integrin subunit. Expression of human beta 1D in CHO cells led to its localization at focal adhesions. Clustering of this integrin isoform on the cell surface stimulated tyrosine phosphorylation of pp125FAK (focal adhesion kinase) and caused transient activation of mitogen-activated protein (MAP) kinases. These data indicate that beta 1D and beta 1A integrin isoforms are functionally similar with regard to integrin-mediated signaling.
机译:整联蛋白的胞质结构域使这些细胞外基质受体与细胞骨架结合,并在整联蛋白介导的信号转导中起关键作用。在本报告中,我们描述了称为β1D的新型β1整联蛋白的鉴定,表达,定位和初始功能表征。该同工型包含独特的50个氨基酸的可变剪接胞质结构域,最后24个氨基酸由另一个外显子编码。与β1A同工型相比,这24个氨基酸中有11个是保守的,但13个是独特的(Zhidkova,NI,AM Belkin和R. Mayne。1995. Biochem。Biophys。Res。Commun。214:279-285; van der Flier,A.,I.Kuikman,C.Baudoin,R,van der Neuf,和A.Sonnenberg.1995.FEBS Lett.369:340-344)。使用针对β1D整联蛋白亚基的抗肽抗体,我们证明了β1D同工型仅在骨骼肌和心肌中合成,而通过横纹肌中的免疫印迹检测到非常少量的β1A。 β1A在成人骨骼肌纤维和心肌细胞中无法通过免疫荧光检测到,而β1D则定位于两种细胞类型的肌膜。在骨骼肌中,β1D集中在肋骨,肌腱和神经肌肉接头中。在心肌中,在肋骨和插入椎间盘中发现了这种β1亚型。 beta 1D与成人骨骼肌中的alpha 7A和alpha 7B相关。在成年心脏的心肌细胞中,alpha 7B是beta 1D亚型的主要伴侣。在增生的C2C12成肌细胞中未检测到beta 1D,但它在成肌细胞融合后立即出现,并且其数量在成肌细胞生长和成熟期间持续增加。相反,β1A亚型的表达在培养中的肌无分化过程中被下调,并且在成熟分化的肌管中被β1D完全取代。我们还分析了1D整合素亚基的一些功能特性。人β1D在CHO细胞中的表达导致其定位在粘着斑处。这种整合素同工型在细胞表面上的聚集刺激了pp125FAK(局灶性粘附激酶)的酪氨酸磷酸化,并导致有丝分裂原活化蛋白(MAP)激酶的瞬时活化。这些数据表明,关于整合素介导的信号传导,β1D和β1A整合素同工型在功能上相似。

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