Human T cells efficiently control RSV infection

De, Chandrav; Pickles, Raymond J.; Yao, Wenbo; Liao, Baolin; Boone, Allison; Choi, Monica-Y; Battaglia, Diana; Askin, Frederic B.; Whitmire, Jason K.; Silvestri, Guido; García, J. Víctor; Wahl, Angela

doi:10.1172/jci.insight.168110

Cited by 10 publications

(7 citation statements)

References 62 publications

(103 reference statements)

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“…Interestingly, some of the cellular immune effects observed in SARS-CoV-2 infection differ from data reported in other respiratory viral infections; specifically, human CD8 + T cells or CD4 + T cells effectively and independently control RSV replication in human lung tissue in the absence of an RSV-specific antibody response 41 , and both RSV and human metapneumovirus (hMPV) demonstrate a virus-specific and subset-specific effect on myeloid dendritic cell function (mDC) 42 not reported in SARS-CoV-2 infection. To the best of our knowledge there are no published reports detailing cellular immune changes following RSV and hMPV in infants and children with solid organ transplants, as such we are unable to comment on differences between non-transplanted children and children with solid organ transplants.…”

Section: Discussionmentioning

confidence: 86%

Non-fatal outcomes of COVID-19 disease in pediatric organ transplantation associates with down-regulation of senescence pathways

Subramanian,

Varghese,

Pochedly

et al. 2024

Sci Rep

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This is a cross-sectional study examining kinetics and durability of immune response in children with solid organ transplants (SOTs) who had COVID-19 disease between November 2020 through June 2022, who were followed for 60-days at a single transplant center. Blood was collected between 1–14 (acute infection), and 15–60 days of a positive PCR (convalescence). SOT children with peripheral blood mononuclear cells (PBMC) cryopreserved before 2019 were non-infected controls (ctrls). PBMCs stimulated with 15-mer peptides from spike protein and anti-CD49d/anti-CD28. Testing done included mass cytometry, mi-RNA sequencing with confirmatory qPCR. 38 children formed the study cohort, 10 in the acute phase and 8 in the convalescence phase. 20 subjects were non-infected controls. Two subjects had severe disease. Subjects in the acute and convalescent phases were different subjects. The median age and tacrolimus level at blood draw was not significantly different. There was no death, and no subject was lost to follow-up. During acute infection CD57 expression was low in NKT, Th17 effector memory, memory Treg, CD4−CD8−, and γδT cells (p = 0.01, p = 0.04, p = 0.03, p = 0.03, p = 0.004 respectively). The frequencies of NK and Th2 effector memory cells increased (p = 0.01, p = 0.02) during acute infection. Non-switched memory B and CD8 central memory cell frequencies were decreased during acute infection (p = 0.02; p = 0.02), but the decrease in CD8 central memory cells did not persist. CD4−CD8− and CD14 monocyte frequencies increased during recovery (p = 0.03; p = 0.007). Our observations suggest down regulation of CD57 with absence of NK cell contraction protect against death from COVID-19 disease in children with SOTs.

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Section: Discussionmentioning

confidence: 86%

Non-fatal outcomes of COVID-19 disease in pediatric organ transplantation associates with down-regulation of senescence pathways

Subramanian,

Varghese,

Pochedly

et al. 2024

Sci Rep

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“…The role of humoral immunity in developing short-lived protective antibodies is well demonstrated; mediated cell immunity would play pivotal roles in both hRSV clearance and pathogenesis [ 90 ]. Alternatively, recent findings from preclinical studies indicate that CD8 + T cells and CD4 + T cells could proficiently and autonomously manage RSV replication in human lung tissue even in the absence of a specific antibody response against RSV [ 91 ]. An initial transient systemic T-cell lymphopenia occurs during RSV LRTI; the underlying mechanism seems to be virus-induced T-cells apoptosis [ 84 ].…”

Section: Immune Responsementioning

confidence: 99%

“…Preclinical investigations indicate that depleting human CD8 + T cells in mice hampers though does not entirely eradicate the ability to control RSV infection. This implies that CD8 + T cells alone are not the exclusive agents responsible for virus clearance [ 91 ]. Likewise, findings from preclinical studies suggest that CD8 + T cells could also play a role in causing lung damage in humans after being exposed to RSV [ 91 ].…”

Section: Immune Responsementioning

confidence: 99%

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Reshaping Our Knowledge: Advancements in Understanding the Immune Response to Human Respiratory Syncytial Virus

Attaianese,

Guiducci,

Trapani

et al. 2023

Pathogens

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Human respiratory syncytial virus (hRSV) is a significant cause of respiratory tract infections, particularly in young children and older adults. In this review, we aimed to comprehensively summarize what is known about the immune response to hRSV infection. We described the innate and adaptive immune components involved, including the recognition of RSV, the inflammatory response, the role of natural killer (NK) cells, antigen presentation, T cell response, and antibody production. Understanding the complex immune response to hRSV infection is crucial for developing effective interventions against this significant respiratory pathogen. Further investigations into the immune memory generated by hRSV infection and the development of strategies to enhance immune responses may hold promise for the prevention and management of hRSV-associated diseases.

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“…Human T-cells are crucial in managing HRSV infection, clearing intracellular pathogens, and maintaining long-lasting immune responses [ 13 , 14 , 15 ]. Moreover, primed human CD8 + T-cells or CD4 + T-cells effectively and independently control HRSV replication in human lung tissue in the absence of an HRSV-specific antibody response [ 16 ]. Consequently, an optimal vaccine can induce both humoral and cellular immunity, thereby eliciting a balanced immune response in the host.…”

Section: Introductionmentioning

confidence: 99%

A Mixture of T-Cell Epitope Peptides Derived from Human Respiratory Syncytial Virus F Protein Conferred Protection in DR1-TCR Tg Mice

Guo,

Song,

et al. 2024

Vaccines

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Human respiratory syncytial virus (HRSV) poses a significant disease burden on global health. To date, two vaccines that primarily induce humoral immunity to prevent HRSV infection have been approved, whereas vaccines that primarily induce T-cell immunity have not yet been well-represented. To address this gap, 25 predicted T-cell epitope peptides derived from the HRSV fusion protein with high human leukocyte antigen (HLA) binding potential were synthesized, and their ability to be recognized by PBMC from previously infected HRSV cases was assessed using an ELISpot assay. Finally, nine T-cell epitope peptides were selected, each of which was recognized by at least 20% of different donors’ PBMC as potential vaccine candidates to prevent HRSV infection. The protective efficacy of F-9PV, a combination of nine peptides along with CpG-ODN and aluminum phosphate (Al) adjuvants, was validated in both HLA-humanized mice (DR1-TCR transgenic mice, Tg mice) and wild-type (WT) mice. The results show that F-9PV significantly enhanced protection against viral challenge as evidenced by reductions in viral load and pathological lesions in mice lungs. In addition, F-9PV elicits robust Th1-biased response, thereby mitigating the potential safety risk of Th2-induced respiratory disease during HRSV infection. Compared to WT mice, the F-9PV mice exhibited superior protection and immunogenicity in Tg mice, underscoring the specificity for human HLA. Overall, our results demonstrate that T-cell epitope peptides provide protection against HRSV infection in animal models even in the absence of neutralizing antibodies, indicating the feasibility of developing an HRSV T-cell epitope peptide-based vaccine.

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Human T cells efficiently control RSV infection

Cited by 10 publications

References 62 publications

Non-fatal outcomes of COVID-19 disease in pediatric organ transplantation associates with down-regulation of senescence pathways

Non-fatal outcomes of COVID-19 disease in pediatric organ transplantation associates with down-regulation of senescence pathways

Reshaping Our Knowledge: Advancements in Understanding the Immune Response to Human Respiratory Syncytial Virus

A Mixture of T-Cell Epitope Peptides Derived from Human Respiratory Syncytial Virus F Protein Conferred Protection in DR1-TCR Tg Mice

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