Cascio Graciela, Martín-Cófreces Noa B, Rodríguez-Frade José Miguel, López-Cotarelo Pilar, Criado Gabriel, Pablos José L, Rodríguez-Fernández José Luis, Sánchez-Madrid Francisco, Mellado Mario
Departamento de Inmunología y Oncología, Centro Nacional de Biotecnología/Consejo Superior de Investigaciones Cientificas, E-28049 Madrid, Spain;
Servicio de Inmunología, Instituto de Investigación Sanitaria Hospital Universitario de la Princesa, Universidad Autónoma de Madrid, E-28006 Madrid, Spain;
J Immunol. 2015 Jun 1;194(11):5509-19. doi: 10.4049/jimmunol.1402419. Epub 2015 Apr 27.
The adaptive immune response requires interaction between T cells and APC to form a specialized structure termed the immune synapse (IS). Although the TCR is essential for IS organization, other factors such as chemokines participate in this process. In this study, we show that the chemokine CXCL12-mediated signaling contributes to correct IS organization and therefore influences T cell activation. CXCR4 downregulation or blockade on T cells caused defective actin polymerization at the contact site with APC, altered microtubule-organizing center polarization and the IS structure, and reduced T cell/APC contact duration. T cell activation was thus inhibited, as shown by reduced expression of CD25 and CD69 markers and of IL-2 mRNA levels. The results indicate that, through Gi and JAK1 and 2 kinases activation, CXCL12 signaling cooperates to build the IS and to maintain adhesive contacts between APC and T cells, required for continuous TCR signaling.
适应性免疫反应需要T细胞与抗原呈递细胞(APC)相互作用,以形成一种称为免疫突触(IS)的特殊结构。虽然T细胞受体(TCR)对于免疫突触的形成至关重要,但其他因素如趋化因子也参与了这一过程。在本研究中,我们发现趋化因子CXCL12介导的信号传导有助于免疫突触的正确形成,从而影响T细胞的激活。T细胞上CXCR4的下调或阻断会导致与APC接触部位的肌动蛋白聚合缺陷,改变微管组织中心的极化和免疫突触结构,并缩短T细胞/APC的接触持续时间。如CD25和CD69标志物表达降低以及IL-2 mRNA水平降低所示,T细胞激活因此受到抑制。结果表明,通过激活Gi以及JAK1和JAK2激酶,CXCL12信号传导协同构建免疫突触,并维持APC与T细胞之间的粘附接触,这是持续TCR信号传导所必需的。
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