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CD56brightCD16− Killer Ig-Like Receptor− NK Cells Display Longer Telomeres and Acquire Features of CD56dim NK Cells upon Activation

CD16 生物 细胞生物学 白细胞介素12 白细胞介素21 Janus激酶3 NK-92 淋巴因子激活杀伤细胞 淋巴结 受体 流式细胞术 免疫学 免疫系统 细胞毒性T细胞 CD3型 T细胞 体外 CD8型 生物化学
作者
Chiara Romagnani,Kerstin Juelke,Michela Falco,Barbara Morandi,Antonella D’Agostino,Roberta Costa,G. B. Ratto,Giuseppe Forte,Paolo Carrega,Gabrielle Lui,Romana Conte,Till Strowig,Alessandro Moretta,Christian Münz,Andreas Thiel,Lorenzo Moretta,Guido Ferlazzo
出处
期刊:Journal of Immunology [The American Association of Immunologists]
卷期号:178 (8): 4947-4955 被引量:430
标识
DOI:10.4049/jimmunol.178.8.4947
摘要

Abstract Human NK cells can be divided into CD56dimCD16+ killer Ig-like receptors (KIR)+/− and CD56brightCD16− KIR− subsets that have been characterized extensively regarding their different functions, phenotype, and tissue localization. Nonetheless, the developmental relationship between these two NK cell subsets remains controversial. We report that, upon cytokine activation, peripheral blood (PB)-CD56bright NK cells mainly gain the signature of CD56dim NK cells. Remarkably, KIR can be induced not only on CD56bright, but also on CD56dim KIR− NK cells, and their expression correlates with lower proliferative response. In addition, we demonstrate for the first time that PB-CD56dim display shorter telomeres than PB- and lymph node (LN)-derived CD56bright NK cells. Along this line, although human NK cells collected from nonreactive LN display almost no KIR and CD16 expression, NK cells derived from highly reactive LN, efferent lymph, and PB express significant amounts of KIR and CD16, implying that CD56bright NK cells could acquire these molecules in the LN during inflammation and then circulate through the efferent lymph into PB as KIR+CD16+ NK cells. Altogether, our results suggest that CD56brightCD16− KIR− and CD56dimCD16+KIR+/− NK cells correspond to sequential steps of differentiation and support the hypothesis that secondary lymphoid organs can be sites of NK cell final maturation and self-tolerance acquisition during immune reaction.
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