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Chemokine Receptor–Dependent Control of Skin Tissue–Resident Memory T Cell Formation

机译:趋化因子受体依赖性的皮肤组织控制-常驻记忆T细胞形成

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Infection or inflammation of the skin recruits effector CD8+ T cells that enter the epidermis and form populations of long-lived tissue-resident memory T (TRM) cells. These skin TRM cells migrate within the constrained epidermal environment by extending multiple dynamic dendritic projections and squeezing between keratinocytes to survey the tissue for pathogens. In this study, we examined the signals required for this distinctive mode of T cell migration by inhibiting key cytoskeletal components and performing intravital two-photon microscopy to visualize TRM cell behavior. We found that TRM cell motility and dendrite formation required an intact actomyosin cytoskeleton and the Rho-associated coiled-coil containing kinases. We also identified an essential role for microtubules for maintaining skin TRM cell shape and cellular integrity. We reveal a role for pertussis toxin–sensitive signaling for TRM cell dendritic morphology and migration that is independent of CXCR3 or CXCR6, or the skin-selective chemokine receptors CCR10 and CCR8. However, we found that CXCR6 and CCR10 expression by CD8+ T cells was required for the optimal formation of memory T cell populations, in particular TRM cell populations in the skin.
机译:皮肤的感染或炎症会吸收效应CD8 + T细胞,这些CD8 + T细胞进入表皮并形成长寿的组织驻留记忆T(TRM)细胞。这些皮肤TRM细胞通过扩展多个动态树突状突起并挤压角质形成细胞之间以调查组织中的病原体,从而在受限的表皮环境中迁移。在这项研究中,我们通过抑制关键的细胞骨架成分并进行活体双光子显微镜观察TRM细胞行为,检查了T细胞迁移这种独特模式所需的信号。我们发现TRM细胞运动性和树突形成需要完整的放线菌素细胞骨架和与Rho相关的卷曲螺旋激酶。我们还确定了微管在维持皮肤TRM细胞形状和细胞完整性方面的重要作用。我们揭示了百日咳毒素敏感信号传导对TRM细胞树突形态和迁移的作用,其独立于CXCR3或CXCR6或皮肤选择性趋化因子受体CCR10和CCR8。但是,我们发现CD8 + T细胞表达CXCR6和CCR10是记忆T细胞群体(尤其是皮肤中的TRM细胞群体)最佳形成所必需的。

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