Resistance to Superinfection by a Vigorously Replicating, Uncloned Stock of Simian Immunodeficiency Virus (SIVmac251) Stimulates Replication of a Live Attenuated Virus Vaccine (SIVmacC8)

Overview

Journal J Gen Virol

Specialty Microbiology

Date 2008 Aug 30

PMID 18753233

Citations 24

Authors

Neil Berry

Richard Stebbings

Debbie Ferguson

Claire Ham

Jack Alden

Stuart Brown

Adrian Jenkins

Jenny Lines

Laura Duffy

Leanne Davis

William Elsley

Mark Page

Robin Hull

Jim Stott

Neil Almond

Affiliations

Soon will be listed here.

Abstract

Vaccination with live attenuated simian immunodeficiency virus (SIVmacC8) confers potent, reproducible protection against homologous wild-type virus challenge (SIVmacJ5). The ability of SIVmacC8 to confer resistance to superinfection with an uncloned ex vivo derivative of SIVmac251 (SIVmac32H/L28) was investigated. In naïve, Mauritian-derived cynomolgus macaques (Macaca fascicularis), SIVmac32H/L28 replicated to high peak titres (>10(8) SIV RNA copies ml(-1)), persisted at high levels and induced distinctive pathology in lymphoid tissues. In cynomolgus macaques vaccinated with SIVmacC8, no evidence of detectable superinfection was observed in 3/8 vaccinates following challenge 3 or 20 weeks later with SIVmac32H/L28. Analyses after SIVmac32H/L28 challenge revealed a significant reduction in viral RNA (P<0.001) and DNA levels between 20 week vaccinates and challenge controls. Amongst 3 week vaccinates, less potent protection was observed. However, analysis of env from breakthrough virus indicated >99% sequence similarity with the vaccine virus. Highly sensitive PCR assays that distinguish vaccine and challenge virus stocks demonstrated restimulation of replication of the vaccine virus SIVmacC8 in the face of potent protection against a vigorous, homologous challenge virus. Vaccine-induced antiviral neutralizing antibodies and anti-Nef CD8+ cytotoxic T cell responses did not correlate with the outcome of the challenge. Defining the mechanism of vaccine protection will need to account for the effective control of a genetically closely related challenge virus whilst remaining unable to suppress replication of the pre-existing vaccine virus. The role of innate and intrinsic anti-retroviral immunity in the protection conferred by live attenuated SIV vaccines warrants careful study.

Citing Articles

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Almond N, Berry N, Stebbings R, Preston M, Ham C, Page M J Virol. 2019; 93(21).

PMID: 31413132 PMC: 6803269. DOI: 10.1128/JVI.00606-19.

Variable Baseline Endogenous Retrovirus (PcEV) Expression Is Upregulated in Acutely SIV-Infected Macaques and Correlated to STAT1 Expression in the Spleen.

Atangana Maze E, Ham C, Kelly J, Ussher L, Almond N, Towers G Front Immunol. 2019; 10:901.

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Immune Responses in the Central Nervous System Are Anatomically Segregated in a Non-Human Primate Model of Human Immunodeficiency Virus Infection.

Tavano B, Tsipouri V, Hardy G, Royle C, Keegan M, Fuchs D Front Immunol. 2017; 8:361.

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Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine.

Berry N, Manoussaka M, Ham C, Ferguson D, Tudor H, Mattiuzzo G PLoS Pathog. 2016; 12(12):e1006083.

PMID: 28002473 PMC: 5176322. DOI: 10.1371/journal.ppat.1006083.

Attenuated SIV causes persisting neuroinflammation in the absence of a chronic viral load and neurotoxic antiretroviral therapy.

Ferguson D, Clarke S, Berry N, Almond N AIDS. 2016; 30(16):2439-2448.

PMID: 27258396 PMC: 5051525. DOI: 10.1097/QAD.0000000000001178.