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Regulated expression of Mg2+ binding epitope on leukocyte integrin alpha subunits.

机译:Mg2 +结合表位在白细胞整联蛋白α亚基上的调控表达。

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摘要

The leukocyte integrins LFA-1, CR3 and p150,95 are a family of heterodimeric receptors that mediate divalent cation-dependent cellular adhesion reactions. In this study we describe a novel antibody-defined epitope present on the leukocyte integrin alpha subunits indicating that the antibody recognizes a structural feature common to all three polypeptides. Antibody recognition further differs from that of previously described anti-leukocyte integrin antibodies in that it is strictly dependent upon the presence of Mg2+. This suggests that the epitope is located within, or in close proximity to, the three conserved cation binding domains and is therefore a measure of Mg2+ bound to the leukocyte integrins and thus reflects functionally active molecules. The epitope can be induced on polymorphonuclear leukocytes, a subset of T cells and on monocytes but is absent or much reduced at low temperature or in the presence of metabolic inhibitors. These observations have considerable implications for the regulation of leukocyte integrin function suggesting that Mg2+ binding to the extracellular domain(s) of the alpha subunits is controlled from within the cell. We suggest that one mechanism by which ligand binding by these molecules can be 'switched' on and off in response to external signals is by regulation of Mg2+ binding to these molecules, converting from the cation-free, 'inactive' to the Mg2+-bound, 'active' form.
机译:白细胞整合素LFA-1,CR3和p150,95是异源二聚体受体家族,可介导二价阳离子依赖性细胞粘附反应。在这项研究中,我们描述了一种新的抗体定义的抗原决定簇,该抗原决定簇存在于白细胞整合素α亚基上,表明该抗体识别所有三个多肽共有的结构特征。抗体识别与先前描述的抗白细胞整合素抗体的识别进一步不同,因为它严格依赖于Mg2 +的存在。这表明该表位位于三个保守的阳离子结合结构域之内或附近,因此是与白细胞整联蛋白结合的Mg 2+的量度,因此反映了功能活性分子。可以在多形核白细胞,T细胞的一个子集和单核细胞上诱导表位,但是在低温下或在存在代谢抑制剂的情况下,该表位不存在或减少很多。这些观察结果对白细胞整合素功能的调节具有重要意义,表明Mg2 +与α亚基的胞外域的结合是从细胞内控制的。我们认为,响应外部信号,这些分子的配体结合可以被“打开”和关闭的一种机制是通过调节Mg2 +与这些分子的结合,从无阳离子的“惰性”转变为与Mg2 +结合的分子。 ,“有效”形式。

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