首页> 美国卫生研究院文献>Journal of Virology >Adoptive immunotherapy of murine cytomegalovirus adrenalitis in the immunocompromised host: CD4-helper-independent antiviral function of CD8-positive memory T lymphocytes derived from latently infected donors.
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Adoptive immunotherapy of murine cytomegalovirus adrenalitis in the immunocompromised host: CD4-helper-independent antiviral function of CD8-positive memory T lymphocytes derived from latently infected donors.

机译:在免疫功能低下的宿主中对鼠科巨细胞病毒肾上腺炎的过继免疫疗法:衍生自潜伏感染供体的CD8阳性记忆T淋巴细胞的CD4辅助独立抗病毒功能。

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摘要

The ability of memory T lymphocytes derived from latently infected mice to control murine cytomegalovirus disease in the immunocompromised host was studied by adoptive transfer experiments. At a stage of pathogenesis when virus had already colonized target tissues, a therapeutic antiviral function could be ascribed to the CD8+ subset. This in vivo function was not restricted to sites in which intravenously infused lymphocytes usually are trapped or home in, such as the lungs or the spleen, respectively, but was also evident in the adrenal glands, a site to which antiviral effector cells have to specifically migrate. Specific infiltration of adrenal gland cortical tissue by donor-derived CD8+ memory T lymphocytes was demonstrated. CD4+ memory T lymphocytes had no antiviral effect by themselves and also were not required for the function of the CD8+ effector cells in this short-term immunotherapy model. These findings should help settle the debate about which subset of T lymphocytes comprises the effector cells that can directly control cytomegalovirus infection in the murine model system.
机译:通过过继转移实验研究了潜伏感染小鼠的记忆T淋巴细胞控制免疫受损宿主中鼠巨细胞病毒疾病的能力。在病毒已经定殖于目标组织的发病机理阶段,可以将治疗性抗病毒功能归因于CD8 +亚群。这种体内功能不仅限于通常分别捕获或安置静脉内输注的淋巴细胞的部位,例如肺或脾,而且在肾上腺也很明显,抗病毒效应细胞必须专门针对该部位迁移。证明了供体来源的CD8 +记忆T淋巴细胞对肾上腺皮质组织的特异性浸润。 CD4 +记忆T淋巴细胞本身没有抗病毒作用,在这种短期免疫治疗模型中,CD8 +效应细胞的功能也不是必需的。这些发现应有助于解决关于哪些T淋巴细胞亚群包含可直接控制鼠模型系统中巨细胞病毒感染的效应细胞的争论。

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