Department of Molecular and Cellular Biology, Arizona Cancer Center, Tucson, Arizona 85724, USA.
J Biol Chem. 2010 Jan 15;285(3):1841-9. doi: 10.1074/jbc.M109.057349. Epub 2009 Nov 16.
Integrin alphaIIbbeta3 affinity regulation by talin binding to the cytoplasmic tail of beta3 is a generally accepted model for explaining activation of this integrin in Chinese hamster ovary cells and human platelets. Most of the evidence for this model comes from the use of multivalent ligands. This raises the possibility that the activation being measured is that of increased clustering of the integrin rather than affinity. Using a newly developed assay that probes integrins on the surface of cells with only monovalent ligands prior to fixation, I do not find increases in affinity of alphaIIbbeta3 integrins by talin head fragments in Chinese hamster ovary cells, nor do I observe affinity increases in human platelets stimulated with thrombin. Binding to a multivalent ligand does increase in both of these cases. This assay does report affinity increases induced by either Mn(2+), a cytoplasmic domain mutant (D723R) in the cytoplasmic domain of beta3, or preincubation with a peptide ligand. These results reconcile the previously observed differences between talin effects on integrin activation in Drosophila and vertebrate systems and suggest new models for talin regulation of integrin activity in human platelets.
整合素 αIIbbeta3 通过与β3 胞质尾部结合来调节其亲和力,这是解释该整合素在中华仓鼠卵巢细胞和人血小板中激活的公认模型。该模型的大部分证据来自于多价配体的使用。这就提出了这样一种可能性,即所测量的激活是整合素聚类增加,而不是亲和力增加。使用一种新开发的测定法,在固定之前用单价配体探测细胞表面上的整合素,我没有发现 talin 头部片段在中华仓鼠卵巢细胞中增加 αIIbbeta3 整合素的亲和力,也没有观察到凝血酶刺激的人血小板中亲和力增加。在这两种情况下,与多价配体的结合都增加了。该测定法确实报告了由 Mn(2+)、β3 胞质结构域中的突变体(D723R)或与肽配体预孵育诱导的亲和力增加。这些结果调和了以前在果蝇和脊椎动物系统中观察到的 talin 对整合素激活的影响之间的差异,并为 talin 调节人血小板中整合素活性提出了新的模型。
