Strong influenza-induced T
            <sub>FH</sub>
            generation requires CD4 effectors to recognize antigen locally and receive signals from continuing infection

Devarajan, Priyadharshini; Vong, Allen M.; Castonguay, Catherine; Kugler‐Umana, Olivia; Bautista, Bianca; Jones, M. C.; Kelly, Karen; Xia, Jingya; Swain, Susan L.

doi:10.1073/pnas.2111064119

Cited by 15 publications

(32 citation statements)

References 52 publications

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“…It has long been appreciated that while infection by influenza virus induces robust and long-lived humoral responses, seasonal influenza vaccination strategies have largely failed in this regard. Devarajan and colleagues speculated that this could be due to differences in antigen availability and duration of Tfh responses in the LNs between influenza infection and vaccination with inactivated vaccines ( Devarajan et al., 2022 ). Their 2022 study found that strong influenza-induced Tfh responses require CD4 effectors to continually recognize local antigens and receive signals from ongoing infection ( Devarajan et al., 2022 ).…”

Section: Adaptive Respiratory Immune Response: Priming Antigen-specif...mentioning

confidence: 99%

“…Devarajan and colleagues speculated that this could be due to differences in antigen availability and duration of Tfh responses in the LNs between influenza infection and vaccination with inactivated vaccines ( Devarajan et al., 2022 ). Their 2022 study found that strong influenza-induced Tfh responses require CD4 effectors to continually recognize local antigens and receive signals from ongoing infection ( Devarajan et al., 2022 ). GC reactions stalled with inactivated vaccination but could be prolonged with the administration of LAIV.…”

Section: Adaptive Respiratory Immune Response: Priming Antigen-specif...mentioning

confidence: 99%

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Mucosal immune responses to infection and vaccination in the respiratory tract

Mettelman

Allen²,

Thomas³

2022

Immunity

102

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Section: Adaptive Respiratory Immune Response: Priming Antigen-specif...mentioning

confidence: 99%

Section: Adaptive Respiratory Immune Response: Priming Antigen-specif...mentioning

confidence: 99%

Mucosal immune responses to infection and vaccination in the respiratory tract

Mettelman

Allen²,

Thomas³

2022

Immunity

102

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“…To evaluate the subsets of CD4 effectors generated, we compared donor and host CD4 effectors at 8 dpi by examining cytokine production and phenotype markers: Th1 (T-bet, IFNγ, TNFα, IL-2), Triple cytokine producers (IFNγ, TNFα, IL-2), Th17 (IL-17), and T REG (FoxP3). We used NKG2A/C/E expression to detect cytotoxic CD4 (ThCTL), found only in the lung (31), and CXCR5 and Bcl-6 co-expression markers for T FH in the spleen (32) (Fig. 1B, Supp.…”

Section: Resultsmentioning

confidence: 99%

Peptide Avidity for TCR on CD4 Effectors Determines the Extent of Memory Generation

Jones

Castonguay

Nanaware

et al. 2022

Preprint

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The impact of initial peptide antigen affinity for TCR in driving memory fate has been studied previously, however its contributions when effectors contract to memory is unclear. To become memory, effector CD4 T cells must recognize antigen at 5-8 days post-infection, at what we call the “effector checkpoint.” We examined whether peptide affinity for the TCR of effectors impacts the extent of memory and degree of protection against rechallenge. We made an influenza A virus (IAV) nucleoprotein (NP)-specific TCR transgenic strain, FluNP, and generated NP-peptide variants that bind FluNP TCR with a broad range of avidity. To vary avidity in vivo, we primed naïve donor FluNP in IAV-infected hosts, purified 6d FluNP effectors and co-transferred them with peptide-pulsed APC into uninfected second hosts. Higher affinity peptides yielded higher numbers of FluNP memory cells in the spleen and most dramatically in the lung and dLN, and drove better protection against lethal influenza infection. The major impact of avidity was on memory cell number, not cytokine production, and was already apparent within several days of transfer. We previously showed that autocrine IL-2 production during the effector checkpoint prevented default effector apoptosis and supported memory formation. Here, peptide avidity determined the level of IL-2 produced by effectors. IL-2Rα expression by APC drove more memory cell formation, suggesting that transpresentation of IL-2 by APC at this checkpoint enhanced CD4 memory generation. Secondary memory generation was also avidity-dependent. We propose this pathway selects CD4 effectors of highest affinity to progress to memory.

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“…Transfer of Ag/APC i.n. successfully restricted Ag presentation to the lung, while transfer of Ag/APC i.s restricted Ag presentation to the spleen (Devarajan et al, 2022) (summarized in Figure S4A ).…”

Section: Resultsmentioning

confidence: 99%

“…Our previous data show that after intravenous (i.v.) OVA II /APC transfer they are found predominantly in the spleen and not in the lung, though donor effectors in the lung express Nur77 GFP , suggesting that they recognized Ag in the periphery before migrating to the lung (Devarajan et al, 2022) ( Figure S4A ). To test if peripheral Ag presentation was sufficient to drive 6d effectors to ThCTL, we transferred OVA II /APC i.v.…”

Section: Resultsmentioning

confidence: 99%

Cytotoxic CD4 Development Requires CD4 Effectors to Concurrently Recognize Local Antigen and Encounter Infection-Induced IL-15

Devarajan

Vong

Castonguay

et al. 2020

Preprint

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SummaryT follicular helper (TFH) and Cytotoxic CD4 (ThCTL) are tissue-restricted CD4 effector subsets, functionally specialized to mediate optimal Ab production and cytotoxicity of infected cells. Influenza infection generates robust CD4 responses, including lung ThCTL and SLO TFH, that protect against reinfection by variant strains. Antigen (Ag) presentation after infection, lasts through the effector phase of the response. Here, we show that this effector phase Ag presentation, well after priming, is required to drive CD4 effectors to ThCTL and TFH. Using in vivo influenza models, we varied Ag presentation to effectors acutely, just at the effector phase. Ag presentation was required in the tissue of effector residence. We suggest these requirements contain unnecessary or potentially pathogenic CD4 responses, only allowing them if infection is uncleared. The results imply that providing effector phase Ag, would lead to stronger humoral and CD4 tissue immunity and thus can be applied to improve vaccine design.

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Strong influenza-induced T _FH generation requires CD4 effectors to recognize antigen locally and receive signals from continuing infection

Cited by 15 publications

References 52 publications

Mucosal immune responses to infection and vaccination in the respiratory tract

Mucosal immune responses to infection and vaccination in the respiratory tract

Peptide Avidity for TCR on CD4 Effectors Determines the Extent of Memory Generation

Cytotoxic CD4 Development Requires CD4 Effectors to Concurrently Recognize Local Antigen and Encounter Infection-Induced IL-15

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Strong influenza-induced T FH generation requires CD4 effectors to recognize antigen locally and receive signals from continuing infection

Cited by 15 publications

References 52 publications

Mucosal immune responses to infection and vaccination in the respiratory tract

Mucosal immune responses to infection and vaccination in the respiratory tract

Peptide Avidity for TCR on CD4 Effectors Determines the Extent of Memory Generation

Cytotoxic CD4 Development Requires CD4 Effectors to Concurrently Recognize Local Antigen and Encounter Infection-Induced IL-15

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Product

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Strong influenza-induced T _FH generation requires CD4 effectors to recognize antigen locally and receive signals from continuing infection