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

In order to evaluate the role of persisting virus replication during occult phase immunisation in the live attenuated SIV vaccine model, a novel SIVmac239Δnef variant (SIVrtTA) genetically engineered to replicate in the presence of doxycycline was evaluated for its ability to protect against wild-ty...

Descripción completa

Detalles Bibliográficos
Autores principales: Berry, Neil, Manoussaka, Maria, Ham, Claire, Ferguson, Deborah, Tudor, Hannah, Mattiuzzo, Giada, Klaver, Bep, Page, Mark, Stebbings, Richard, Das, Atze T., Berkhout, Ben, Almond, Neil, Cranage, Martin P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5176322/
https://www.ncbi.nlm.nih.gov/pubmed/28002473
http://dx.doi.org/10.1371/journal.ppat.1006083
_version_ 1782484801761050624
author Berry, Neil
Manoussaka, Maria
Ham, Claire
Ferguson, Deborah
Tudor, Hannah
Mattiuzzo, Giada
Klaver, Bep
Page, Mark
Stebbings, Richard
Das, Atze T.
Berkhout, Ben
Almond, Neil
Cranage, Martin P.
author_facet Berry, Neil
Manoussaka, Maria
Ham, Claire
Ferguson, Deborah
Tudor, Hannah
Mattiuzzo, Giada
Klaver, Bep
Page, Mark
Stebbings, Richard
Das, Atze T.
Berkhout, Ben
Almond, Neil
Cranage, Martin P.
author_sort Berry, Neil
collection PubMed
description In order to evaluate the role of persisting virus replication during occult phase immunisation in the live attenuated SIV vaccine model, a novel SIVmac239Δnef variant (SIVrtTA) genetically engineered to replicate in the presence of doxycycline was evaluated for its ability to protect against wild-type SIVmac239. Indian rhesus macaques were vaccinated either with SIVrtTA or with SIVmac239Δnef. Doxycycline was withdrawn from 4 of 8 SIVrtTA vaccinates before challenge with wild-type virus. Unvaccinated challenge controls exhibited ~10(7) peak plasma viral RNA copies/ml persisting beyond the acute phase. Six vaccinates, four SIVmac239Δnef and two SIVrtTA vaccinates exhibited complete protection, defined by lack of wild-type viraemia post-challenge and virus-specific PCR analysis of tissues recovered post-mortem, whereas six SIVrtTA vaccinates were protected from high levels of viraemia. Critically, the complete protection in two SIVrtTA vaccinates was associated with enhanced SIVrtTA replication in the immediate post-acute vaccination period but was independent of doxycycline status at the time of challenge. Mutations were identified in the LTR promoter region and rtTA gene that do not affect doxycycline-control but were associated with enhanced post-acute phase replication in protected vaccinates. High frequencies of total circulating CD8(+)T effector memory cells and a higher total frequency of SIV-specific CD8(+) mono and polyfunctional T cells on the day of wild-type challenge were associated with complete protection but these parameters were not predictive of outcome when assessed 130 days after challenge. Moreover, challenge virus-specific Nef CD8(+) polyfunctional T cell responses and antigen were detected in tissues post mortem in completely-protected macaques indicating post-challenge control of infection. Within the parameters of the study design, on-going occult-phase replication may not be absolutely required for protective immunity.
format Online
Article
Text
id pubmed-5176322
institution National Center for Biotechnology Information
language English
publishDate 2016
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-51763222017-01-04 Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine Berry, Neil Manoussaka, Maria Ham, Claire Ferguson, Deborah Tudor, Hannah Mattiuzzo, Giada Klaver, Bep Page, Mark Stebbings, Richard Das, Atze T. Berkhout, Ben Almond, Neil Cranage, Martin P. PLoS Pathog Research Article In order to evaluate the role of persisting virus replication during occult phase immunisation in the live attenuated SIV vaccine model, a novel SIVmac239Δnef variant (SIVrtTA) genetically engineered to replicate in the presence of doxycycline was evaluated for its ability to protect against wild-type SIVmac239. Indian rhesus macaques were vaccinated either with SIVrtTA or with SIVmac239Δnef. Doxycycline was withdrawn from 4 of 8 SIVrtTA vaccinates before challenge with wild-type virus. Unvaccinated challenge controls exhibited ~10(7) peak plasma viral RNA copies/ml persisting beyond the acute phase. Six vaccinates, four SIVmac239Δnef and two SIVrtTA vaccinates exhibited complete protection, defined by lack of wild-type viraemia post-challenge and virus-specific PCR analysis of tissues recovered post-mortem, whereas six SIVrtTA vaccinates were protected from high levels of viraemia. Critically, the complete protection in two SIVrtTA vaccinates was associated with enhanced SIVrtTA replication in the immediate post-acute vaccination period but was independent of doxycycline status at the time of challenge. Mutations were identified in the LTR promoter region and rtTA gene that do not affect doxycycline-control but were associated with enhanced post-acute phase replication in protected vaccinates. High frequencies of total circulating CD8(+)T effector memory cells and a higher total frequency of SIV-specific CD8(+) mono and polyfunctional T cells on the day of wild-type challenge were associated with complete protection but these parameters were not predictive of outcome when assessed 130 days after challenge. Moreover, challenge virus-specific Nef CD8(+) polyfunctional T cell responses and antigen were detected in tissues post mortem in completely-protected macaques indicating post-challenge control of infection. Within the parameters of the study design, on-going occult-phase replication may not be absolutely required for protective immunity. Public Library of Science 2016-12-21 /pmc/articles/PMC5176322/ /pubmed/28002473 http://dx.doi.org/10.1371/journal.ppat.1006083 Text en © 2016 Berry et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Berry, Neil
Manoussaka, Maria
Ham, Claire
Ferguson, Deborah
Tudor, Hannah
Mattiuzzo, Giada
Klaver, Bep
Page, Mark
Stebbings, Richard
Das, Atze T.
Berkhout, Ben
Almond, Neil
Cranage, Martin P.
Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine
title Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine
title_full Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine
title_fullStr Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine
title_full_unstemmed Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine
title_short Role of Occult and Post-acute Phase Replication in Protective Immunity Induced with a Novel Live Attenuated SIV Vaccine
title_sort role of occult and post-acute phase replication in protective immunity induced with a novel live attenuated siv vaccine
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5176322/
https://www.ncbi.nlm.nih.gov/pubmed/28002473
http://dx.doi.org/10.1371/journal.ppat.1006083
work_keys_str_mv AT berryneil roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT manoussakamaria roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT hamclaire roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT fergusondeborah roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT tudorhannah roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT mattiuzzogiada roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT klaverbep roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT pagemark roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT stebbingsrichard roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT dasatzet roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT berkhoutben roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT almondneil roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine
AT cranagemartinp roleofoccultandpostacutephasereplicationinprotectiveimmunityinducedwithanovelliveattenuatedsivvaccine

Ejemplares similares