Abstract
It remains undefined whether a subset of CD4+ T cells can function as fast-acting cells to control Mycobacterium tuberculosis (Mtb) infection. Here we show that the primary CD4+CD161+ T-cell subset, not CD4+CD161-, in unexposed healthy humans fast acted as unconventional T cells capable of inhibiting intracellular Mtb and BCG growth upon exposure to infected autologous and allogeneic macrophages or lung epithelial A549 cells. Such inhibition coincided with the ability of primary CD4+CD161+ T cells to rapidly express/secrete anti-TB cytokines including IFN-γ, TNF-α, IL-17, and perforin upon exposure to Mtb. Mechanistically, blockades of CD161 pathway, perforin or IFN-γ by blocking mAbs abrogated the ability of CD4+CD161+ T cells to inhibit intracellular mycobacterial growth. Pre-treatment of infected macrophages with inhibitors of autophagy also blocked the CD4+CD161+ T cell-mediated growth inhibition of mycobacteria. Furthermore, adoptive transfer of human CD4+CD161+ T cells conferred protective immunity against mycobacterial infection in SCID mice. Surprisingly, CD4+CD161+ T cells in TB patients exhibited a loss or reduction of their capabilities to produce perforin/IFN-γ and to inhibit intracellular growth of mycobacteria in infected macrophages. These immune dysfunctions were consistent with PD1/Tim3 up-regulation on CD4+CD161+ T cells in active tuberculosis patients, and the blockade of PD1/Tim3 on this subset cells enhanced the inhibition of intracellular mycobacteria survival. Thus, these findings suggest that a fast-acting primary CD4+CD161+T-cell subset in unexposed humans employs the CD161 pathway, perforin, and IFN-γ/autophagy to inhibit the growth of intracellular mycobacteria, thereby distinguishing them from the slow adaptive responses of conventional CD4+ T cells. The presence of fast-acting CD4+CD161+ T-cell that inhibit mycobacterial growth in unexposed humans but not TB patients also implicates the role of these cells in protective immunity against initial Mtb infection.
Highlights
Tuberculosis (TB), caused by Mycobacterium tuberculosis (Mtb), remains the top killer among infectious diseases largely due to epidemics of human immunodeficiency virus (HIV)/AIDS and drug resistance [1]
Since nonhuman primates (NHP) closely resemble humans, we hypothesized that human CD4+CD161+ T cells may represent the fast-acting CD4+ T-cell subset required to control early Mtb dissemination after pulmonary infection in NHPs [19]
Since CD4+CD161+ T cells were derived from healthy donors express potential MHC II different from THP-1 or A549 target cells, such mismatches implicate that CD4+ CD161+ T-cell inhibition of intracellular mycobacteria does not likely require MHC II-restricted antigen recognition
Summary
Tuberculosis (TB), caused by Mycobacterium tuberculosis (Mtb), remains the top killer among infectious diseases largely due to epidemics of HIV/AIDS and drug resistance [1]. Protective immune mechanisms against TB infection remain largely undefined [5]. Studies in mice indicate that CD4+ T cells are required for immunity against high-dose Mtb infection [9,10,11]. CD4+ T cells can evolve into Th1 effector cells producing IFN-g/TNF-a for macrophage activation and subsequent control of TB infection [12]. Ag-activated CD4+ T effector cells generated from exposed or infected individuals can function as cytotoxic T cells producing cytotoxic granules or inhibiting of intracellular Mtb bacilli [17, 18]. The phenotypes and functional mechanisms of CTL-like CD4+ T-cell immunity are unclear
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