Citrobacter rodentium Induces Tissue-Resident Memory CD4
            <sup>+</sup>
            T Cells

Bishu, Shrinivas; Hou, Guoqing; Zaatari, Mohammed El; Popke, Donald; Zhang, M.; Grasberger, Helmut; Zou, Wei; Stidham, Ryan W.; Higgins, Peter; Spence, Jason R.; Kamada, Nobuhiko; Kao, John Y.

doi:10.1128/iai.00295-19

Cited by 15 publications

(20 citation statements)

References 38 publications

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“…A protective role for CD4 + T RM at mucosal surfaces has recently been described for a number of bacterial pathogens of public health significance. 1,2,[28][29][30][31][32][33][34] Exposure to live pneumococcus in the nasopharynx protects mice against subsequent homologous or heterologous pneumococcal challenge. 21,22 Hence, we hypothesized that I.N.…”

Section: Resultsmentioning

confidence: 99%

Generation of protective pneumococcal-specific nasal resident memory CD4+ T cells via parenteral immunization

et al. 2020

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The generation of tissue-resident memory T cells (T RM ) is an essential aspect of immunity at mucosal surfaces, and it has been suggested that preferential generation of T RM is one of the principal advantages of mucosally administered vaccines. We have previously shown that antigen-specific, IL-17-producing CD4 + T cells can provide capsular antibody-independent protection against nasal carriage of Streptococcus pneumoniae; but whether pneumococcus-responsive T RM are localized within the nasal mucosa and are sufficient for protection from carriage has not been determined. Here, we show that intranasal administration of live or killed pneumococci to mice generates pneumococcus-responsive IL-17A-producing CD4 + mucosal T RM. Furthermore, we show that these cells are sufficient to mediate long-lived, neutrophil-dependent protection against subsequent pneumococcal nasal challenge. Unexpectedly, and in contrast with the prevailing paradigm, we found that parenteral administration of killed pneumococci also generates protective IL-17A + CD4 + T RM in the nasal mucosa. These results demonstrate a critical and sufficient role of T RM in prevention of pneumococcal colonization, and further that these cells can be generated by parenteral immunization. Our findings therefore have important implications regarding the generation of immune protection at mucosal surfaces by vaccination.Mucosal Immunology (2020) 13:172-182; https://doi.

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Section: Resultsmentioning

confidence: 99%

Generation of protective pneumococcal-specific nasal resident memory CD4+ T cells via parenteral immunization

et al. 2020

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“…However, CD4 + T RM cells lack, or possess low levels of, CD103 and can depend on receiving different signals (e.g., antigen), even in the same anatomical site [ 135 , 136 , 137 , 138 ]. Research in the past decade determined that CD4 + T RM cells are induced at various mucosal sites to mediate protective immunity against an array of bacterial pathogens, including M. tuberculosis [ 139 ], B. pertussis [ 140 ], S. pneumoniae [ 141 ], L. monocytogenes [ 142 ], C. rodentium [ 143 ], and Chlamydia trachomatis [ 144 ]. Despite this, less is known about CD4 + T RM cells in infection settings, in comparison to their CD8 + T RM cell counterparts, or whether CD4 + T RM cells form effector T H cell subtypes, such as T H 1, T H 2, and T H 17, or even T FH cells.…”

Section: How T Cells Fight Bacteriamentioning

confidence: 99%

T Cell Immunity to Bacterial Pathogens: Mechanisms of Immune Control and Bacterial Evasion

Shepherd

McLaren

2020

IJMS

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The human body frequently encounters harmful bacterial pathogens and employs immune defense mechanisms designed to counteract such pathogenic assault. In the adaptive immune system, major histocompatibility complex (MHC)-restricted αβ T cells, along with unconventional αβ or γδ T cells, respond to bacterial antigens to orchestrate persisting protective immune responses and generate immunological memory. Research in the past ten years accelerated our knowledge of how T cells recognize bacterial antigens and how many bacterial species have evolved mechanisms to evade host antimicrobial immune responses. Such escape mechanisms act to corrupt the crosstalk between innate and adaptive immunity, potentially tipping the balance of host immune responses toward pathological rather than protective. This review examines the latest developments in our knowledge of how T cell immunity responds to bacterial pathogens and evaluates some of the mechanisms that pathogenic bacteria use to evade such T cell immunosurveillance, to promote virulence and survival in the host.

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“…We and others have identified an increased frequency of CD4 þ TRM T cells with a proinflammatory Th17 phenotype in biopsy samples from active CD and ulcerative colitis patients compared with healthy control patients. 17,18,57,58 Furthermore, increased levels of CD69 þ CD103 þ CD4 þ TRM T cells have been associated with clinical flares. 18 Previous reports identified a link between CD4 þ TRM IL17A þ T cells and CD by using biopsy specimens from CD patients undergoing surgery for severe, chronically active, or complicated disease.…”

Section: Discussionmentioning

confidence: 99%

PIR-B Regulates CD4+ IL17a+ T-Cell Survival and Restricts T-Cell–Dependent Intestinal Inflammatory Responses

Uddin¹,

Tomar²,

Sharma³

et al. 2021

Cellular and Molecular Gastroenterology and Hepatology

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The inhibitory receptor paired immunoglobulin-like receptor B regulates CD4 þ T-helper 17 cell-dependent chronic intestinal inflammatory responses by tempering mammalian target of rapamycin complex Q8 1 signaling and enhancing CD4 þ interleukin 17a þ T-cell survival and regulates the outgrowth and maintenance of tissue resident memory CD4 þ interleukin 17a þ T cells.BACKGROUND & AIMS: CD4 þ T cells are regulated by activating and inhibitory cues, and dysregulation of these proper regulatory inputs predisposes these cells Q9 to aberrant inflammation and exacerbation of disease. We investigated the role of the inhibitory receptor paired immunoglobulin-like receptor B (PIR-B) in the regulation of the CD4 þ T-cell inflammatory response and exacerbation of the colitic phenotype. METHODS:We used Il10 -/spontaneous and CD4 þ CD45RB hi Tcell transfer models of colitis with PIR-B-deficient (Pirb -/-) mice. Flow cytometry, Western blot, and RNA sequencing analysis was performed on wild-type and Pirb -/-CD4 þ T cells. In silico analyses were performed on RNA sequencing data set of ileal biopsy samples from pediatric CD and non-inflammatory bowel disease patients and sorted human memory CD4 þ T cells. RESULTS:We identified PIR-B expression on memory CD4 þ interleukin (IL)17a þ cells. We show that PIR-B regulates CD4 þ T-helper 17 cell (Th17)-dependent chronic intestinal inflammatory responses and the development of colitis. Mechanistically, we show that the PIR-B-SHP Q10 -1/2 axis tempers mammalian Q11 target of rapamycin complex 1 signaling and

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Citrobacter rodentium Induces Tissue-Resident Memory CD4 ⁺ T Cells

Cited by 15 publications

References 38 publications

Generation of protective pneumococcal-specific nasal resident memory CD4+ T cells via parenteral immunization

Generation of protective pneumococcal-specific nasal resident memory CD4+ T cells via parenteral immunization

T Cell Immunity to Bacterial Pathogens: Mechanisms of Immune Control and Bacterial Evasion

PIR-B Regulates CD4+ IL17a+ T-Cell Survival and Restricts T-Cell–Dependent Intestinal Inflammatory Responses

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Citrobacter rodentium Induces Tissue-Resident Memory CD4 + T Cells

Cited by 15 publications

References 38 publications

Generation of protective pneumococcal-specific nasal resident memory CD4+ T cells via parenteral immunization

Generation of protective pneumococcal-specific nasal resident memory CD4+ T cells via parenteral immunization

T Cell Immunity to Bacterial Pathogens: Mechanisms of Immune Control and Bacterial Evasion

PIR-B Regulates CD4+ IL17a+ T-Cell Survival and Restricts T-Cell–Dependent Intestinal Inflammatory Responses

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Citrobacter rodentium Induces Tissue-Resident Memory CD4 ⁺ T Cells