Development and Homeostasis of T Cell Memory in Rhesus Macaque

生物 免疫学 人口 CD28 效应器 T细胞 恒河猴 CD8型 免疫系统 记忆T细胞 细胞毒性T细胞 存储单元 细胞生物学 遗传学 体外 医学 环境卫生 物理 量子力学 电压 晶体管
作者
Christine J. Pitcher,Shoko I. Hagen,Joshua M. Walker,Richard Lum,Bridget L. Mitchell,Vernon C. Maino,Michael K. Axthelm,Louis J. Picker
出处
期刊:Journal of Immunology [American Association of Immunologists]
卷期号:168 (1): 29-43 被引量:466
标识
DOI:10.4049/jimmunol.168.1.29
摘要

Abstract The rhesus macaque (RM) is a critical animal model for studies of viral pathogenesis and immunity, yet fundamental aspects of their cellular immune response remain poorly defined. One such deficiency is the lack of validated phenotypic signatures for their naive and memory T cell subsets, and the resultant unavailability of accurate information on their memory T cell development, homeostasis, and function. In this study, we report a phenotypic paradigm allowing definitive characterization of these subsets and their comprehensive functional analysis. Naive T cells are optimally delineated by their homogeneous CD95lowCD28highβ7 integrinint (CD4+) or CD95lowCD28intCD11alow (CD8+) phenotypes. This subset 1) was present in blood and secondary lymph tissues, but not effector sites; 2) vastly predominated in the fetal/neonatal immune system, but rapidly diminished with postnatal age; 3) lacked IFN-γ production capability, and specific responses to RM CMV; and 4) demonstrated low in vivo proliferative activity. CD4+ and CD8+ memory subsets were CD95high, but otherwise phenotypically heterogeneous and included all IFN-γ production, RM CMV-specific responses, effector site T cells, and demonstrated high in vivo proliferative activity (∼10 times the naive subset). These analyses also revealed the RM “effector memory” subset within the overall memory population. This population, best defined by lack of CD28 expression, contained the majority of RM CMV-specific cells, was highly enriched in extralymphoid effector sites, and comprised an increasing proportion of total memory cells with age. The effector memory subset demonstrated similar in vivo proliferative activity and survival as CD28+ “central memory” T cells, consistent with independent homeostatic regulation.
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