The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype

C. Mee Ling Munier; David van Bockel; Michelle Bailey; Susanna Ip; Yin Xu; Sheilajen Alcantara; Sue Min Liu; Gareth Denyer; Warren Kaplan; Kazuo Suzuki; Nathan Croft; Anthony Purcell; David Tscharke; David A. Cooper; Stephen J. Kent; John J. Zaunders; Anthony D. Kelleher

doi:10.1016/j.vaccine.2016.09.009

The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype

C. Mee Ling Munier^*, David van Bockel, Michelle Bailey, Susanna Ip, Yin Xu, Sheilajen Alcantara, Sue Min Liu, Gareth Denyer, Warren Kaplan, Kazuo Suzuki, Nathan Croft, Anthony Purcell, David Tscharke, David A. Cooper, Stephen J. Kent, John J. Zaunders, Anthony D. Kelleher

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

31 Citations (Scopus)

Abstract

Background Smallpox was eradicated by a global program of inoculation with Vaccinia virus (VV). Robust VV-specific CD4 T-cell responses during primary infection are likely essential to controlling VV replication. Although there is increasing interest in cytolytic CD4 T-cells across many viral infections, the importance of these cells during acute VV infection is unclear. Methods We undertook a detailed functional and genetic characterization of CD4 T-cells during acute VV-infection of humans. VV-specific T-cells were identified by up-regulation of activation markers directly ex vivo and through cytokine and co-stimulatory molecule expression. At day-13-post primary inoculation with VV, CD38highCD45RO+ CD4 T-cells were purified by cell sorting, RNA isolated and analysed by microarray. Differential expression of up-regulated genes in activated CD4 T-cells was confirmed at the mRNA and protein levels. We compared analyses of VV-specific CD4 T-cells to studies on 12 subjects with primary HIV infection (PHI). VV-specific T-cells lines were established from PBMCs collected post vaccination and checked for cytotoxicity potential. Results A median 11.9% CD4 T-cells were CD38highCD45RO+ at day-13 post-VV inoculation, compared to 3.0% prior and 10.4% during PHI. Activated CD4 T-cells had an up-regulation of genes related to cytolytic function, including granzymes K and A, perforin, granulysin, TIA-1, and Rab27a. No difference was seen between CD4 T-cell expression of perforin or TIA-1 to VV and PHI, however granzyme k was more dominant in the VV response. At 25:1 effector to target ratio, two VV-specific T-cell lines exhibited 62% and 30% cytotoxicity respectively and CD107a degranulation. Conclusions We show for the first time that CD4 CTL are prominent in the early response to VV. Understanding the role of CD4 CTL in the generation of an effective anti-viral memory may help develop more effective vaccines for diseases such as HIV.

Original language	English
Pages (from-to)	5251-5261
Number of pages	11
Journal	Vaccine
Volume	34
Issue number	44
DOIs	https://doi.org/10.1016/j.vaccine.2016.09.009
Publication status	Published - 17 Oct 2016

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10.1016/j.vaccine.2016.09.009

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Munier, C. M. L., van Bockel, D., Bailey, M., Ip, S., Xu, Y., Alcantara, S., Liu, S. M., Denyer, G., Kaplan, W., Suzuki, K., Croft, N., Purcell, A., Tscharke, D., Cooper, D. A., Kent, S. J., Zaunders, J. J., & Kelleher, A. D. (2016). The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype. Vaccine, 34(44), 5251-5261. https://doi.org/10.1016/j.vaccine.2016.09.009

@article{731ed8f0ae6e4df9b28072a29e315d84,

title = "The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype",

abstract = "Background Smallpox was eradicated by a global program of inoculation with Vaccinia virus (VV). Robust VV-specific CD4 T-cell responses during primary infection are likely essential to controlling VV replication. Although there is increasing interest in cytolytic CD4 T-cells across many viral infections, the importance of these cells during acute VV infection is unclear. Methods We undertook a detailed functional and genetic characterization of CD4 T-cells during acute VV-infection of humans. VV-specific T-cells were identified by up-regulation of activation markers directly ex vivo and through cytokine and co-stimulatory molecule expression. At day-13-post primary inoculation with VV, CD38highCD45RO+ CD4 T-cells were purified by cell sorting, RNA isolated and analysed by microarray. Differential expression of up-regulated genes in activated CD4 T-cells was confirmed at the mRNA and protein levels. We compared analyses of VV-specific CD4 T-cells to studies on 12 subjects with primary HIV infection (PHI). VV-specific T-cells lines were established from PBMCs collected post vaccination and checked for cytotoxicity potential. Results A median 11.9% CD4 T-cells were CD38highCD45RO+ at day-13 post-VV inoculation, compared to 3.0% prior and 10.4% during PHI. Activated CD4 T-cells had an up-regulation of genes related to cytolytic function, including granzymes K and A, perforin, granulysin, TIA-1, and Rab27a. No difference was seen between CD4 T-cell expression of perforin or TIA-1 to VV and PHI, however granzyme k was more dominant in the VV response. At 25:1 effector to target ratio, two VV-specific T-cell lines exhibited 62% and 30% cytotoxicity respectively and CD107a degranulation. Conclusions We show for the first time that CD4 CTL are prominent in the early response to VV. Understanding the role of CD4 CTL in the generation of an effective anti-viral memory may help develop more effective vaccines for diseases such as HIV.",

keywords = "CD4, CD8, Cytotoxic T-cells, Granzyme K, HIV, Microarray, Vaccinia",

author = "Munier, {C. Mee Ling} and {van Bockel}, David and Michelle Bailey and Susanna Ip and Yin Xu and Sheilajen Alcantara and Liu, {Sue Min} and Gareth Denyer and Warren Kaplan and Kazuo Suzuki and Nathan Croft and Anthony Purcell and David Tscharke and Cooper, {David A.} and Kent, {Stephen J.} and Zaunders, {John J.} and Kelleher, {Anthony D.}",

note = "Publisher Copyright: {\textcopyright} 2016",

year = "2016",

month = oct,

day = "17",

doi = "10.1016/j.vaccine.2016.09.009",

language = "English",

volume = "34",

pages = "5251--5261",

journal = "Vaccine",

issn = "0264-410X",

publisher = "Elsevier B.V.",

number = "44",

}

Munier, CML, van Bockel, D, Bailey, M, Ip, S, Xu, Y, Alcantara, S, Liu, SM, Denyer, G, Kaplan, W, Suzuki, K, Croft, N, Purcell, A, Tscharke, D, Cooper, DA, Kent, SJ, Zaunders, JJ & Kelleher, AD 2016, 'The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype', Vaccine, vol. 34, no. 44, pp. 5251-5261. https://doi.org/10.1016/j.vaccine.2016.09.009

TY - JOUR

T1 - The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype

AU - Munier, C. Mee Ling

AU - van Bockel, David

AU - Bailey, Michelle

AU - Ip, Susanna

AU - Xu, Yin

AU - Alcantara, Sheilajen

AU - Liu, Sue Min

AU - Denyer, Gareth

AU - Kaplan, Warren

AU - Suzuki, Kazuo

AU - Croft, Nathan

AU - Purcell, Anthony

AU - Tscharke, David

AU - Cooper, David A.

AU - Kent, Stephen J.

AU - Zaunders, John J.

AU - Kelleher, Anthony D.

PY - 2016/10/17

Y1 - 2016/10/17

N2 - Background Smallpox was eradicated by a global program of inoculation with Vaccinia virus (VV). Robust VV-specific CD4 T-cell responses during primary infection are likely essential to controlling VV replication. Although there is increasing interest in cytolytic CD4 T-cells across many viral infections, the importance of these cells during acute VV infection is unclear. Methods We undertook a detailed functional and genetic characterization of CD4 T-cells during acute VV-infection of humans. VV-specific T-cells were identified by up-regulation of activation markers directly ex vivo and through cytokine and co-stimulatory molecule expression. At day-13-post primary inoculation with VV, CD38highCD45RO+ CD4 T-cells were purified by cell sorting, RNA isolated and analysed by microarray. Differential expression of up-regulated genes in activated CD4 T-cells was confirmed at the mRNA and protein levels. We compared analyses of VV-specific CD4 T-cells to studies on 12 subjects with primary HIV infection (PHI). VV-specific T-cells lines were established from PBMCs collected post vaccination and checked for cytotoxicity potential. Results A median 11.9% CD4 T-cells were CD38highCD45RO+ at day-13 post-VV inoculation, compared to 3.0% prior and 10.4% during PHI. Activated CD4 T-cells had an up-regulation of genes related to cytolytic function, including granzymes K and A, perforin, granulysin, TIA-1, and Rab27a. No difference was seen between CD4 T-cell expression of perforin or TIA-1 to VV and PHI, however granzyme k was more dominant in the VV response. At 25:1 effector to target ratio, two VV-specific T-cell lines exhibited 62% and 30% cytotoxicity respectively and CD107a degranulation. Conclusions We show for the first time that CD4 CTL are prominent in the early response to VV. Understanding the role of CD4 CTL in the generation of an effective anti-viral memory may help develop more effective vaccines for diseases such as HIV.

AB - Background Smallpox was eradicated by a global program of inoculation with Vaccinia virus (VV). Robust VV-specific CD4 T-cell responses during primary infection are likely essential to controlling VV replication. Although there is increasing interest in cytolytic CD4 T-cells across many viral infections, the importance of these cells during acute VV infection is unclear. Methods We undertook a detailed functional and genetic characterization of CD4 T-cells during acute VV-infection of humans. VV-specific T-cells were identified by up-regulation of activation markers directly ex vivo and through cytokine and co-stimulatory molecule expression. At day-13-post primary inoculation with VV, CD38highCD45RO+ CD4 T-cells were purified by cell sorting, RNA isolated and analysed by microarray. Differential expression of up-regulated genes in activated CD4 T-cells was confirmed at the mRNA and protein levels. We compared analyses of VV-specific CD4 T-cells to studies on 12 subjects with primary HIV infection (PHI). VV-specific T-cells lines were established from PBMCs collected post vaccination and checked for cytotoxicity potential. Results A median 11.9% CD4 T-cells were CD38highCD45RO+ at day-13 post-VV inoculation, compared to 3.0% prior and 10.4% during PHI. Activated CD4 T-cells had an up-regulation of genes related to cytolytic function, including granzymes K and A, perforin, granulysin, TIA-1, and Rab27a. No difference was seen between CD4 T-cell expression of perforin or TIA-1 to VV and PHI, however granzyme k was more dominant in the VV response. At 25:1 effector to target ratio, two VV-specific T-cell lines exhibited 62% and 30% cytotoxicity respectively and CD107a degranulation. Conclusions We show for the first time that CD4 CTL are prominent in the early response to VV. Understanding the role of CD4 CTL in the generation of an effective anti-viral memory may help develop more effective vaccines for diseases such as HIV.

KW - CD4

KW - CD8

KW - Cytotoxic T-cells

KW - Granzyme K

KW - HIV

KW - Microarray

KW - Vaccinia

UR - http://www.scopus.com/inward/record.url?scp=84989186714&partnerID=8YFLogxK

U2 - 10.1016/j.vaccine.2016.09.009

DO - 10.1016/j.vaccine.2016.09.009

M3 - Article

SN - 0264-410X

VL - 34

SP - 5251

EP - 5261

JO - Vaccine

JF - Vaccine

IS - 44

ER -

The primary immune response to Vaccinia virus vaccination includes cells with a distinct cytotoxic effector CD4 T-cell phenotype

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