Interchangeable alpha chain cytoplasmic domains play a positive role in control of cell adhesion mediated by VLA-4, a beta 1 integrin.

P D Kassner; M E Hemler

首页> 外文期刊>The Journal of Experomental Medicine >Interchangeable alpha chain cytoplasmic domains play a positive role in control of cell adhesion mediated by VLA-4, a beta 1 integrin.

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Interchangeable alpha chain cytoplasmic domains play a positive role in control of cell adhesion mediated by VLA-4, a beta 1 integrin.

机译：可互换的α链胞质域在控制VLA-4（β1整联蛋白）介导的细胞粘附中发挥积极作用。

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Integrins can exist in a range of functional states, depending on the cell type and its state of activation. Although the mechanism that controls activity is unknown, it has been suggested that for some integrins, alpha chain cytoplasmic domains may exert either a negative effect or no effect on adhesion function. To address this issue for VLA-4 (an alpha 4 beta 1 heterodimer), we constructed an alpha 4 cytoplasmic deletion mutant and chimeric alpha chains composed of the extracellular domains of alpha 4 and the cytoplasmic domains of alpha 2, alpha 4, or alpha 5. Upon stable transfection of wild-type alpha 4, VLA-4 heterodimer was obtained that mediated (a) poor adhesion to CS1 peptide, fibronectin, or vascular cell adhesion molecule 1 (VCAM-1) (in K562 cells); (b) poor adhesion to CS1 peptide but moderate adhesion to VCAM-1 (in MIP101 cells); and (c) moderate adhesion to both CS1 peptide and VCAM-1 (in PMWK cells). Chimeric alpha 4 constructs and wild-type alpha 4 yielded similar results in these cell lines. In contrast, truncation of the alpha 4 cytoplasmic domain (after the conserved GFFKR motif) caused an almost complete loss of adhesive activity in all three cell lines. Thus, several interchangeable alpha chain cytoplasmic domains play a fundamentally positive role in determining the state of constitutive activity for VLA-4. The alpha chain cytoplasmic domain is also required for agonist-stimulated adhesion, since phorbol ester stimulated the cell adhesion mediated by wild-type and chimeric alpha chains, but not by the cytoplasmic deletion mutant. The inactivity of both wild-type VLA-4 (in K562 cells), and truncated VLA-4 (in all three cell lines) was overcome by the addition of a stimulatory anti-beta 1 monoclonal antibody. Thus, the alpha cytoplasmic domain-dependent cellular mechanism controlling both constitutive and agonist-stimulated VLA-4 activity could be bypassed by external manipulation of the integrin.

机译：整联蛋白可以以多种功能状态存在，这取决于细胞类型及其激活状态。尽管控制活性的机制尚不清楚，但有人建议对于某些整联蛋白，α链胞质结构域可能对粘附功能起负面作用，也可能不起作用。为了解决VLA-4（α4β1异源二聚体）的问题，我们构建了一个α4细胞质缺失突变体和由α4的胞外域和α2，α4或α的胞质域组成的嵌合α链。 5.稳定转染野生型α4后，获得VLA-4异二聚体，其介导（a）对CS1肽，纤连蛋白或血管细胞粘附分子1（VCAM-1）的粘附性差（在K562细胞中）; （b）对CS1肽的粘附力较弱，但对VCAM-1的粘附力中等（在MIP101细胞中）; （c）对CS1肽和VCAM-1均具有中等粘附力（在PMWK细胞中）。在这些细胞系中，嵌合的α4构建体和野生型α4产生了相似的结果。相反，α4细胞质结构域的截短（在保守的GFFKR基序之后）在所有三个细胞系中几乎完全丧失了粘附活性。因此，几个可互换的α链胞质结构域在确定VLA-4的组成活性状态中起根本上的积极作用。激动剂刺激的粘附也需要α链胞质域，因为佛波酯可刺激野生型和嵌合α链而不是胞质缺失突变体介导的细胞粘附。通过添加刺激性抗β1单克隆抗体，可以克服野生型VLA-4（在K562细胞中）和截短的VLA-4（在所有三个细胞系中）的无活性。因此，通过整联蛋白的外部操作可以绕过控制组成型和激动剂刺激的VLA-4活性的α细胞质结构域依赖性细胞机制。

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《The Journal of Experomental Medicine》 |1993年第2期|共12页
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P D Kassner; M E Hemler;
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Interchangeable alpha chain cytoplasmic domains play a positive role in control of cell adhesion mediated by VLA-4, a beta 1 integrin.

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