Microbiology & Immunology - Research Publications

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Start date: 1990 × Author: Carbone, Francis ×

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    Divergent molecular networks program functionally distinct CD8+ skin-resident memory T cells
    Park, SL ; Christo, SN ; Wells, AC ; Gandolfo, LC ; Zaid, A ; Alexandre, YO ; Burn, TN ; Schroeder, J ; Collins, N ; Han, S-J ; Guillaume, SM ; Evrard, M ; Castellucci, C ; Davies, B ; Osman, M ; Obers, A ; McDonald, KM ; Wang, H ; Mueller, SN ; Kannourakis, G ; Berzins, SP ; Mielke, LA ; Carbone, FR ; Kallies, A ; Speed, TP ; Belkaid, Y ; Mackay, LK (AMER ASSOC ADVANCEMENT SCIENCE, 2023-12-01)
    Skin-resident CD8+ T cells include distinct interferon-γ-producing [tissue-resident memory T type 1 (TRM1)] and interleukin-17 (IL-17)-producing (TRM17) subsets that differentially contribute to immune responses. However, whether these populations use common mechanisms to establish tissue residence is unknown. In this work, we show that TRM1 and TRM17 cells navigate divergent trajectories to acquire tissue residency in the skin. TRM1 cells depend on a T-bet-Hobit-IL-15 axis, whereas TRM17 cells develop independently of these factors. Instead, c-Maf commands a tissue-resident program in TRM17 cells parallel to that induced by Hobit in TRM1 cells, with an ICOS-c-Maf-IL-7 axis pivotal to TRM17 cell commitment. Accordingly, by targeting this pathway, skin TRM17 cells can be ablated without compromising their TRM1 counterparts. Thus, skin-resident T cells rely on distinct molecular circuitries, which can be exploited to strategically modulate local immunity.
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    Runx3 drives a CD8+ T cell tissue residency program that is absent in CD4+ T cells
    Fonseca, R ; Burn, TN ; Gandolfo, LC ; Devi, S ; Park, SL ; Obers, A ; Evrard, M ; Christo, SN ; Buquicchio, FA ; Lareau, CA ; McDonald, KM ; Sandford, SK ; Zamudio, NM ; Zanluqui, NG ; Zaid, A ; Speed, TP ; Satpathy, AT ; Mueller, SN ; Carbone, FR ; Mackay, LK (NATURE PORTFOLIO, 2022-08)
    Tissue-resident memory T cells (TRM cells) provide rapid and superior control of localized infections. While the transcription factor Runx3 is a critical regulator of CD8+ T cell tissue residency, its expression is repressed in CD4+ T cells. Here, we show that, as a direct consequence of this Runx3-deficiency, CD4+ TRM cells lacked the transforming growth factor (TGF)-β-responsive transcriptional network that underpins the tissue residency of epithelial CD8+ TRM cells. While CD4+ TRM cell formation required Runx1, this, along with the modest expression of Runx3 in CD4+ TRM cells, was insufficient to engage the TGF-β-driven residency program. Ectopic expression of Runx3 in CD4+ T cells incited this TGF-β-transcriptional network to promote prolonged survival, decreased tissue egress, a microanatomical redistribution towards epithelial layers and enhanced effector functionality. Thus, our results reveal distinct programming of tissue residency in CD8+ and CD4+ TRM cell subsets that is attributable to divergent Runx3 activity.
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    The frequency of mucosal-associated invariant T cells is selectively increased in dermatitis herpetiformis
    Li, J ; Reantragoon, R ; Kostenko, L ; Corbett, AJ ; Varigos, G ; Carbone, FR (WILEY, 2017-08)
    BACKGROUND/OBJECTIVES: Mucosal-associated invariant T (MAIT) cells are a novel subset of innate-like T-cells that are enriched in mucosal tissues. Their presence in human skin has only recently been recognised. We describe the expression of skin-tropic molecules on human skin MAIT cells at steady state and investigate their contribution to various dermatoses with known T-cell involvement. METHODS: To examine the expression of skin-tropic molecules by MAIT cells at steady state, we performed a flow cytometric analysis of blood and skin samples from healthy donors. To investigate any potential wider contribution of MAIT cells to skin disease, we examined psoriasis, alopecia areata and dermatitis herpetiformis biopsies using immunofluorescent staining to identify the proportion of T-cells expressing MAIT cell surface markers. RESULTS: We found that MAIT cells constituted a small population of T-cells in normal human skin, similar to the percentage found in peripheral blood. Like other skin T-cells, skin MAIT cells expressed high levels of the skin-associated markers, cutaneous lymphocyte antigen and CD103. In psoriasis and alopecia areata the proportion of MAIT cells was similar to that found in normal skin, but in dermatitis herpetiformis it was significantly elevated. CONCLUSIONS: The expression of skin-tropic molecules by skin MAIT cells is consistent with their resident status in normal human skin. Our results suggest that MAIT cells may play a role in the pathogenesis of dermatitis herpetiformis.
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    Discrete tissue microenvironments instruct diversity in resident memory T cell function and plasticity
    Christo, SN ; Evrard, M ; Park, SL ; Gandolfo, LC ; Burn, TN ; Fonseca, R ; Newman, DM ; Alexandre, YO ; Collins, N ; Zamudio, NM ; Souza-Fonseca-Guimaraes, F ; Pellicci, DG ; Chisanga, D ; Shi, W ; Bartholin, L ; Belz, GT ; Huntington, ND ; Lucas, A ; Lucas, M ; Mueller, SN ; Heath, WR ; Ginhoux, F ; Speed, TP ; Carbone, FR ; Kallies, A ; Mackay, LK (NATURE PORTFOLIO, 2021-09)
    Tissue-resident memory T (TRM) cells are non-recirculating cells that exist throughout the body. Although TRM cells in various organs rely on common transcriptional networks to establish tissue residency, location-specific factors adapt these cells to their tissue of lodgment. Here we analyze TRM cell heterogeneity between organs and find that the different environments in which these cells differentiate dictate TRM cell function, durability and malleability. We find that unequal responsiveness to TGFβ is a major driver of this diversity. Notably, dampened TGFβ signaling results in CD103- TRM cells with increased proliferative potential, enhanced function and reduced longevity compared with their TGFβ-responsive CD103+ TRM counterparts. Furthermore, whereas CD103- TRM cells readily modified their phenotype upon relocation, CD103+ TRM cells were comparatively resistant to transdifferentiation. Thus, despite common requirements for TRM cell development, tissue adaptation of these cells confers discrete functional properties such that TRM cells exist along a spectrum of differentiation potential that is governed by their local tissue microenvironment.
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    Nociceptive sensory neurons promote CD8 T cell responses to HSV-1 infection
    Filtjens, J ; Roger, A ; Quatrini, L ; Wieduwild, E ; Gouilly, J ; Hoeffel, G ; Rossignol, R ; Daher, C ; Debroas, G ; Henri, S ; Jones, CM ; Malissen, B ; Mackay, LK ; Moqrich, A ; Carbone, FR ; Ugolini, S (NATURE RESEARCH, 2021-05-18)
    Host protection against cutaneous herpes simplex virus 1 (HSV-1) infection relies on the induction of a robust adaptive immune response. Here, we show that Nav1.8+ sensory neurons, which are involved in pain perception, control the magnitude of CD8 T cell priming and expansion in HSV-1-infected mice. The ablation of Nav1.8-expressing sensory neurons is associated with extensive skin lesions characterized by enhanced inflammatory cytokine and chemokine production. Mechanistically, Nav1.8+ sensory neurons are required for the downregulation of neutrophil infiltration in the skin after viral clearance to limit the severity of tissue damage and restore skin homeostasis, as well as for eliciting robust CD8 T cell priming in skin-draining lymph nodes by controlling dendritic cell responses. Collectively, our data reveal an important role for the sensory nervous system in regulating both innate and adaptive immune responses to viral infection, thereby opening up possibilities for new therapeutic strategies.
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    Clone-specific T cell receptor antagonists of major histocompatibility complex class I-restricted cytotoxic T cells.
    Jameson, SC ; Carbone, FR ; Bevan, MJ (Rockefeller University Press, 1993-06-01)
    A previous report showed that the proliferative response of helper T cells to class II major histocompatibility complex (MHC)-restricted antigens can be inhibited by analogues of the antigen, which act as T cell receptor (TCR) antagonists. Here we define and analyze peptide variants that antagonize various functions of class I MHC-restricted cytotoxic T lymphocyte (CTL) clones. Of 64 variants at individual TCR contact sites of the Kb-restricted octamer peptide ovalbumin257-264 (OVAp), a very high proportion (40%) antagonized lysis by three OVAp-specific CTL clones. This effect was highly clone specific, since many antagonists for one T cell clone have differential effects on another. We show that this inhibition of CTL function is not a result of T cell-T cell interaction, precluding veto-like phenomena as a mechanism for antagonism. Moreover, we present evidence for direct interaction between the TCR and antagonist-MHC complexes. In further analysis of the T cell response, we found that serine esterase release and cytokine production are susceptible to TCR antagonism similarly to lysis. Ca2+ flux, an early event in signaling, is also inhibited by antagonists but may be more resistant to the antagonist effect than downstream responses.
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    T cell receptor (TCR) antagonism without a negative signal: evidence from T cell hybridomas expressing two independent TCRs.
    Stotz, SH ; Bolliger, L ; Carbone, FR ; Palmer, E (Rockefeller University Press, 1999-01-18)
    Antagonist peptides inhibit T cell responses by an unknown mechanism. By coexpressing two independent T cell receptors (TCRs) on a single T cell hybridoma, we addressed the question of whether antagonist ligands induce a dominant-negative signal that inhibits the function of a second, independent TCR. The two receptors, Valpha2Vbeta5 and Valpha2Vbeta10, restricted by H-2Kb and specific for the octameric peptides SIINFEKL and SSIEFARL, respectively, were coexpressed on the same cell. Agonist stimulation demonstrated that the two receptors behaved independently with regard to antigen-induced TCR downregulation and intracellular biochemical signaling. The exposure of one TCR (Valpha2Vbeta5) to antagonist peptides could not inhibit a second independent TCR (Valpha2Vbeta10) from responding to its antigen. Thus, our data clearly demonstrate that these antagonist ligands do not generate a dominant-negative signal which affects the responsiveness of the entire cell. In addition, a kinetic analysis showed that even 12 h after engagement with their cognate antigen and 10 h after reaching a steady-state of TCR internalization, T cells were fully inhibited by the addition of antagonist peptides. The window of susceptibility to antagonist ligands correlated exactly with the time required for the responding T cells to commit to interleukin 2 production. The data support a model where antagonist ligands can competitively inhibit antigenic peptides from productively engaging the TCR. This competitive inhibition is effective during the entire commitment period, where sustained TCR engagement is essential for full T cell activation.
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    Skin-resident T cells keep parasites on a Leish
    Mackay, LK ; Carbone, FR (ROCKEFELLER UNIV PRESS, 2015-08-24)
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    Organ-specific isoform selection of fatty acid-binding proteins in tissue-resident lymphocytes
    Frizzell, H ; Fonseca, R ; Christo, SN ; Evrard, M ; Cruz-Gomez, S ; Zanluqui, NG ; von Scheidt, B ; Freestone, D ; Park, SL ; McWilliam, HEG ; Villadangos, JA ; Carbone, FR ; Mackay, LK (AMER ASSOC ADVANCEMENT SCIENCE, 2020-04)
    Tissue-resident memory T (TRM) cells exist throughout the body, where they are poised to mediate local immune responses. Although studies have defined a common mechanism of residency independent of location, there is likely to be a level of specialization that adapts TRM cells to their given tissue of lodgment. It has been shown that TRM cells in the skin rely on the uptake of exogenous fatty acids for their survival and up-regulate fatty acid-binding protein 4 (FABP4) and FABP5 as part of their transcriptional program. However, FABPs exist as a larger family of isoforms, with different members selected in a tissue-specific fashion that is optimized for local fatty acid availability. Here, we show that although TRM cells in a range of tissue widely express FABPs, they are not restricted to FABP4 and FABP5. Instead, TRM cells show varying patterns of isoform usage that are determined by tissue-derived factors. These patterns are malleable because TRM cells relocated to different organs modify their FABP expression in line with their new location. As a consequence, these results argue for tissue-specific overlays to the TRM cell residency program, including FABP expression that is tailored to the particular tissue of TRM cell lodgment.
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    Tissue-resident T cells: dynamic players in skin immunity
    Mueller, SN ; Zaid, A ; Carbone, FR (FRONTIERS RESEARCH FOUNDATION, 2014-07-16)
    The skin is a large and complex organ that acts as a critical barrier protecting the body from pathogens in the environment. Numerous heterogeneous populations of immune cells are found within skin, including some that remain resident and others that can enter and exit the skin as part of their migration program. Pathogen-specific CD8(+) T cells that persist in the epidermis following infection are a unique population of memory cells with important roles in immune surveillance and protective responses to reinfection. How these tissue-resident memory T cells form in the skin, the signals controlling their persistence and behavior, and the mechanisms by which they mediate local recall responses are just beginning to be elucidated. Here, we discuss recent progress in understanding the roles of these skin-resident T cells and also highlight some of the key unanswered questions that need addressing.