Early life vaccination: Generation of adult-quality memory CD8+ T cells in infant mice using non-replicating adenoviral vectors
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Early life vaccination : Generation of adult-quality memory CD8+ T cells in infant mice using non-replicating adenoviral vectors. / Nazerai, Loulieta; Bassi, Maria Rosaria; Uddbäck, Ida Elin Maria; Holst, Peter Johannes; Christensen, Jan Pravsgaard; Thomsen, Allan Randrup.
I: Scientific Reports, Bind 6, 38666, 08.12.2016.Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › fagfællebedømt
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TY - JOUR
T1 - Early life vaccination
T2 - Generation of adult-quality memory CD8+ T cells in infant mice using non-replicating adenoviral vectors
AU - Nazerai, Loulieta
AU - Bassi, Maria Rosaria
AU - Uddbäck, Ida Elin Maria
AU - Holst, Peter Johannes
AU - Christensen, Jan Pravsgaard
AU - Thomsen, Allan Randrup
PY - 2016/12/8
Y1 - 2016/12/8
N2 - Intracellular pathogens represent a serious threat during early life. Importantly, even though the immune system of newborns may be characterized as developmentally immature, with a propensity to develop Th2 immunity, significant CD8+ T-cell responses may still be elicited in the context of optimal priming. Replication deficient adenoviral vectors have been demonstrated to induce potent CD8+ T-cell response in mice, primates and humans. The aim of the present study was therefore to assess whether replication-deficient adenovectors could overcome the risk of overwhelming antigen stimulation during the first period of life and provide a pertinent alternative in infant vaccinology. To address this, infant mice were vaccinated with three different adenoviral vectors and the CD8+ T-cell response after early life vaccination was explored. We assessed the frequency, polyfunctionality and in vivo cytotoxicity of the elicited memory CD8+ T cells, as well as the potential of these cells to respond to secondary infections and confer protection. We further tested the impact of maternal immunity against our replication-deficient adenoviral vector during early life vaccination. Overall, our results indicate that memory CD8+ T cells induced by adenoviral vectors in infant mice are of good quality and match those elicited in the adult host.
AB - Intracellular pathogens represent a serious threat during early life. Importantly, even though the immune system of newborns may be characterized as developmentally immature, with a propensity to develop Th2 immunity, significant CD8+ T-cell responses may still be elicited in the context of optimal priming. Replication deficient adenoviral vectors have been demonstrated to induce potent CD8+ T-cell response in mice, primates and humans. The aim of the present study was therefore to assess whether replication-deficient adenovectors could overcome the risk of overwhelming antigen stimulation during the first period of life and provide a pertinent alternative in infant vaccinology. To address this, infant mice were vaccinated with three different adenoviral vectors and the CD8+ T-cell response after early life vaccination was explored. We assessed the frequency, polyfunctionality and in vivo cytotoxicity of the elicited memory CD8+ T cells, as well as the potential of these cells to respond to secondary infections and confer protection. We further tested the impact of maternal immunity against our replication-deficient adenoviral vector during early life vaccination. Overall, our results indicate that memory CD8+ T cells induced by adenoviral vectors in infant mice are of good quality and match those elicited in the adult host.
U2 - 10.1038/srep38666
DO - 10.1038/srep38666
M3 - Journal article
C2 - 27929135
VL - 6
JO - Scientific Reports
JF - Scientific Reports
SN - 2045-2322
M1 - 38666
ER -
ID: 170188398