Recirculating CD4 memory T cells mount rapid secondary responses without major contributions from follicular CD4 effectors and B cells

Luther, Sanjiv A.; Serre, Karine; Cunningham, Adam F.; Khan, Mahmood; Acha‐Orbea, Hans; MacLennan, Ian C. M.; Toellner, Kai‐Michael

doi:10.1002/eji.200636573

Cited by 5 publications

(7 citation statements)

References 51 publications

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“…Molecules of a similar size are able to disperse rapidly throughout the host and prime in multiple sites (43), and this explains why T cell activation and proliferation was synchronous after sFliC. In contrast, alum-precipitated proteins given s.c. tend to prime in draining LN, but not necessarily in other sites (44)(45)(46).…”

Section: Discussionmentioning

confidence: 95%

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Flores‐Langarica

Marshall

Hitchcock

et al. 2012

The Journal of Immunology

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Mucosal immunity is poorly activated after systemic immunization with protein Ags. Nevertheless, induction of mucosal immunity in such a manner would be an attractive and simple way to overcome the intrinsic difficulties in delivering Ag to such sites. Flagellin from Salmonella enterica serovar Typhimurium (FliC) can impact markedly on host immunity, in part via its recognition by TLR5. In this study, we show that systemic immunization with soluble FliC (sFliC) drives distinct immune responses concurrently in the mesenteric lymph nodes (MLN) and the spleen after i.p. and s.c. immunization. In the MLN, but not the spleen, sFliC drives a TLR5-dependent recruitment of CD103+ dendritic cells (DCs), which correlates with a diminution in CD103+ DC numbers in the lamina propria. In the MLN, CD103+ DCs carry Ag and are the major primers of endogenous and transgenic T cell priming. A key consequence of these interactions with CD103+ DCs in the MLN is an increase in local regulatory T cell differentiation. In parallel, systemic sFliC immunization results in a pronounced switching of FliC-specific B cells to IgA in the MLN but not elsewhere. Loss of TLR5 has more impact on MLN than splenic Ab responses, reflected in an ablation of IgA, but not IgG, serum Ab titers. Therefore, systemic sFliC immunization targets CD103+ DCs and drives distinct mucosal T and B cell responses. This offers a potential “Trojan horse” approach to modulate mucosal immunity by systemically immunizing with sFliC.

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Section: Discussionmentioning

confidence: 95%

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Flores‐Langarica

Marshall

Hitchcock

et al. 2012

The Journal of Immunology

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“…It promotes Th2 responses with the induction of Th2 cytokines in CD4 T cells [16] and strong antibody production associated with elevated titers of the Th2-dependent IgG1 and IgE antibodies [17]. We previously reported that several weeks after immunization with alumprecipitated Ag recirculating memory CD4 T cells are found in lymphoid organs not exposed to the Ag and mount accelerated secondary responses [18]. In the present study we questioned the precise timing of appearance and responsiveness of recirculating memory CD4 T cells in Ag-free lymphoid organs.…”

Section: Introductionmentioning

confidence: 99%

“…Importantly, these early central-memory-like cells are immediately responsive to further Ag stimulation and produce effectors more rapidly than naïve cells. In addition to early memory formation there is production of effector helpers that produce Th2 cytokines [16] and direct B cells to undergo Ig class switching and to form plasmablasts and germinal centers [17][18][19]. Finally, the effect of the initial T-cell precursor frequency has been considered, for evidence has emerged that this can influence central and effector memory commitment [20], and memory T-cell survival [21,22].…”

Section: Introductionmentioning

confidence: 99%

Early simultaneous production of intranodal CD4 Th2 effectors and recirculating rapidly responding central‐memory‐like CD4 T cells

et al. 2009

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This study characterizes the diversity of CD4 Th cells produced during a Th2 response in vivo. Kinetics of effector and memory cell differentiation by mouse OVA-specific CD4 T cells was followed during primary responses to alum-precipitated OVA. The complexity of the CD4 T response was assessed in nodes draining and distant from the site of immunization for phenotype, location and function. By 3 days IL-4-producing effector CD4 T cells developed in the draining node and a proportion of the responding cells had migrated to B-cell follicles, while yet others had left the draining node. Some of these early migrant cells were recirculating cells with a central memory phenotype. These had divided four or more times in the draining node before migrating to distant nodes not exposed to antigen. We questioned the responsiveness of these early central-memory-like cells on secondary antigen challenge at sites distant to the primary immunization. They re-entered cell cycle and migrated to B-cell follicles, much more rapidly than naïve CD4 T cells and could still be induced to produce IL-4. Their production and survival were independent of the starting frequency of antigen-specific CD4 T cells. Thus intranodal effector cells and recirculating, rapidly responding central-memory-like cells emerged simultaneously from the third day of a primary Th2 response.

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“…This approach would allow us to identify when populations were generated and clarify the movement of memory CD4 + T cells to other secondary lymphoid tissue or their retention in the draining LN. Immunisation of the murine paw pad has been used to target a specific peripheral LN, often the popliteal LN . We immunised the front paw pad to target the brachial LN (bLN) given its greater size and the scarcity of endogenous CD4 + T cells responsive to a given peptide .…”

Section: Resultsmentioning

confidence: 99%

Retention of Ag‐specific memory CD4⁺ T cells in the draining lymph node indicates lymphoid tissue resident memory populations

et al. 2017

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Several different memory T‐cell populations have now been described based upon surface receptor expression and migratory capabilities. Here we have assessed murine endogenous memory CD4+ T cells generated within a draining lymph node and their subsequent migration to other secondary lymphoid tissues. Having established a model response targeting a specific peripheral lymph node, we temporally labelled all the cells within draining lymph node using photoconversion. Tracking of photoconverted and non‐photoconverted Ag‐specific CD4+ T cells revealed the rapid establishment of a circulating memory population in all lymph nodes within days of immunisation. Strikingly, a resident memory CD4+ T cell population became established in the draining lymph node and persisted for several months in the absence of detectable migration to other lymphoid tissue. These cells most closely resembled effector memory T cells, usually associated with circulation through non‐lymphoid tissue, but here, these cells were retained in the draining lymph node. These data indicate that lymphoid tissue resident memory CD4+ T‐cell populations are generated in peripheral lymph nodes following immunisation.

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Recirculating CD4 memory T cells mount rapid secondary responses without major contributions from follicular CD4 effectors and B cells

Cited by 5 publications

References 51 publications

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Early simultaneous production of intranodal CD4 Th2 effectors and recirculating rapidly responding central‐memory‐like CD4 T cells

Retention of Ag‐specific memory CD4⁺ T cells in the draining lymph node indicates lymphoid tissue resident memory populations

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Recirculating CD4 memory T cells mount rapid secondary responses without major contributions from follicular CD4 effectors and B cells

Cited by 5 publications

References 51 publications

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Systemic Flagellin Immunization Stimulates Mucosal CD103+ Dendritic Cells and Drives Foxp3+ Regulatory T Cell and IgA Responses in the Mesenteric Lymph Node

Early simultaneous production of intranodal CD4 Th2 effectors and recirculating rapidly responding central‐memory‐like CD4 T cells

Retention of Ag‐specific memory CD4+ T cells in the draining lymph node indicates lymphoid tissue resident memory populations

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Retention of Ag‐specific memory CD4⁺ T cells in the draining lymph node indicates lymphoid tissue resident memory populations