Natural killer (NK) cells contribute to control of HIV/SIV infection. We defined macaque NK-cell subsets based on expression of CD56 and CD16 and found their distribution to be highly disparate. CD16 ؉ NK cells predominated in peripheral blood, whereas most mucosal NK cells were CD56 ؉ , and lymph nodes contained both CD56 ؉ and CD16 ؊ CD56 ؊ (doublenegative [DN]) subsets. Functional profiles were also distinct among subsets-CD16 ؉ NK cells expressed high levels of cytolytic molecules, and CD56 ؉ NK cells were predominantly cytokine-secreting cells, whereas DN NK possessed both functions. In macaques chronically infected with SIV, circulating CD16 ؉ and DN NK cells were expanded in number and, although markers of cytoxicity increased, cytokine secretion decreased. Notably, CD56 ؉ NK cells in SIV-infected animals up-regulated perforin, granzyme B, and CD107a. In contrast, the lymph nodehoming molecules CD62 ligand (CD62L) and C-C chemokine receptor type 7 (CCR7), which are expressed primarily on CD56 ؉ and DN NK cells, were significantly down-regulated on NK cells from infected animals. These data demonstrate that SIV infection drives a shift in NK-cell function characterized by decreased cytokine production, expanded cytotoxicity, and trafficking away from secondary lymphoid organs, suggesting that the NK-cell repertoire is not only heterogeneous but also plastic.
IntroductionSince their discovery in the 1970s, natural killer (NK) cells have been considered the major effector cells of the innate immune system because of their ability to kill virus-infected or neoplastic cells. Although NK cell-mediated killing does not require prior antigen sensitization, cell-to-cell contact between NK and target T cells occurs through a complex array of inhibitory and activating receptors. In humans, NK cells express both killer-cell immunoglobulin-like receptors (KIRs), which interact with major histocompatibility complex (MHC) class I molecules and can be either inhibitory or activating, and receptors belonging to the C-type lectin family such as natural killer group 2A (NKG2A), an inhibitory receptor that recognizes HLA-E and NKG2D, which recognizes the stress-induced ligands MHC class I chain-related gene A and B (MICA/MICB) and members of the ULBP family. 1 Human NK cells also express various natural cytotoxicity receptors including NKp46, NKp30, and NKp44, for which the ligands remain incompletely characterized. 2,3 However, increasing evidence suggests that the complexity of NK-cell function has been underappreciated and that in addition to cytolysis of aberrant T cells, NK cells also produce a wide array of cytokines, mediate tolerance to self-antigens, and regulate dendritic cell functions. 4 Most recently, murine studies have suggested that NK cells may even display characteristics of adaptive immune responses. 5 In humans, 2 primary phenotypically defined subsets of NK cells have been described, cytolytic CD56 dim CD16 ϩ and cytokinesecreting CD56 bright CD16 Ϫ subsets, of which the CD56 dim CD16 ϩ subset predomina...
