Subsequent AS01-adjuvanted vaccinations induce similar transcriptional responses in populations with different disease statuses.
Journal
PloS one
ISSN: 1932-6203
Titre abrégé: PLoS One
Pays: United States
ID NLM: 101285081
Informations de publication
Date de publication:
2022
2022
Historique:
received:
25
03
2022
accepted:
07
10
2022
entrez:
10
11
2022
pubmed:
11
11
2022
medline:
15
11
2022
Statut:
epublish
Résumé
Transcriptional responses to adjuvanted vaccines can vary substantially among populations. Interindividual diversity in levels of pathogen exposure, and thus of cell-mediated immunological memory at baseline, may be an important determinant of population differences in vaccine responses. Adjuvant System AS01 is used in licensed or candidate vaccines for several diseases and populations, yet the impact of pre-existing immunity on its adjuvanticity remains to be elucidated. In this exploratory post-hoc analysis of clinical trial samples (clinicalTrials.gov: NCT01424501), we compared gene expression patterns elicited by two immunizations with the candidate tuberculosis (TB) vaccine M72/AS01, between three groups of individuals with different levels of memory responses to TB antigens before vaccination. Analyzed were one group of TB-disease-treated individuals, and two groups of TB-disease-naïve individuals who were (based on purified protein derivative [PPD] skin-test results) stratified into PPD-positive and PPD-negative groups. Although TB-disease-treated individuals displayed slightly stronger transcriptional responses after each vaccine dose, functional gene signatures were overall not distinctly different between groups. Considering the similarities with the signatures found previously for other AS01-adjuvanted vaccines, many features of the response appeared to be adjuvant-driven. Across groups, cell proliferation-related signals at 7 days post-dose 1 were associated with increased anti-M72 antibody response magnitudes. These early signals were stronger in the TB-disease-treated group as compared to both TB-disease-naïve groups. Interindividual homogeneity in gene expression levels was also higher for TB-disease-treated individuals post-dose 1, but increased in all groups post-dose 2 to attain similar levels between the three groups. Altogether, strong cell-mediated memory responses at baseline accelerated and amplified transcriptional responses to a single dose of this AS01-adjuvanted vaccine, resulting in more homogenous gene expression levels among the highly-primed individuals as compared to the disease-naïve individuals. However, after a second vaccination, response heterogeneity decreased and was similar across groups, irrespective of the degree of immune memory acquired at baseline. This information can support the design and analysis of future clinical trials evaluating AS01-adjuvanted vaccines.
Identifiants
pubmed: 36355775
doi: 10.1371/journal.pone.0276505
pii: PONE-D-22-08893
pmc: PMC9648731
doi:
Substances chimiques
Adjuvants, Immunologic
0
Tuberculin
0
Tuberculosis Vaccines
0
Banques de données
ClinicalTrials.gov
['NCT01424501']
Types de publication
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
e0276505Informations de copyright
Copyright: © 2022 Coccia et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Déclaration de conflit d'intérêts
I have read the journal’s policy and the authors of this manuscript have the following competing interests: All authors are or were employees of the GSK group of companies. All authors hold shares in the GSK group of companies. Part of the activities conducted by MC and RAvdB (excluding RAvdB’s salary) were funded by grant OPP1220977 from the Bill and Melinda Gates Foundation. MC is named as an inventor on novel methods for inducing an immune response: Publication Number WO2017/017050 and WO2015/150567. Each of these applications is granted and/or pending in several countries. RvdM is currently an employee of BioNTech (Mainz, Germany). PG is currently an employee of PPD, part of Thermo Fisher Scientific (Zaventem, Belgium). This does not alter our adherence to PLOS ONE policies on sharing data and materials.
Références
NPJ Vaccines. 2017 Sep 8;2:25
pubmed: 29263880
Front Immunol. 2019 Nov 07;10:2616
pubmed: 31787983
Am J Respir Crit Care Med. 2013 Aug 15;188(4):492-502
pubmed: 23306546
Am J Respir Crit Care Med. 2015 Mar 1;191(5):584-91
pubmed: 25562578
Clin Microbiol Rev. 2018 Jul 18;31(4):
pubmed: 30021818
Front Immunol. 2018 Apr 13;9:661
pubmed: 29706954
N Engl J Med. 2016 Sep 15;375(11):1019-32
pubmed: 27626517
Tuberculosis (Edinb). 2016 Sep;100:118-127
pubmed: 27553419
Am J Respir Crit Care Med. 2005 Jun 15;171(12):1430-5
pubmed: 15831840
NPJ Syst Biol Appl. 2017 Mar 13;3:10
pubmed: 28649437
Nat Commun. 2018 Dec 6;9(1):5208
pubmed: 30523338
Hum Vaccin Immunother. 2016 Nov;12(11):2813-2832
pubmed: 27448625
Semin Immunol. 2018 Oct;39:14-21
pubmed: 29801750
Nat Immunol. 2016 Feb;17(2):204-13
pubmed: 26726811
Nat Med. 2010 May;16(5):558-64, 1p following 564
pubmed: 20436484
Lancet Respir Med. 2020 Apr;8(4):395-406
pubmed: 31958400
mSphere. 2018 Aug 1;3(4):
pubmed: 30068557
Expert Rev Vaccines. 2017 Jan;16(1):55-63
pubmed: 27448771
Sci Transl Med. 2020 Nov 11;12(569):
pubmed: 33177181
Am J Respir Crit Care Med. 2000 Apr;161(4 Pt 1):1376-95
pubmed: 10764337
Front Immunol. 2017 Aug 14;8:943
pubmed: 28855902
Nat Immunol. 2009 Jan;10(1):116-125
pubmed: 19029902
N Engl J Med. 2015 May 28;372(22):2087-96
pubmed: 25916341
PLoS Pathog. 2011 Aug;7(8):e1002174
pubmed: 21852947
Lancet Infect Dis. 2020 Mar;20(3):e28-e37
pubmed: 32014117
Am J Respir Crit Care Med. 2018 May 1;197(9):1198-1208
pubmed: 29624071
Nucleic Acids Res. 2015 Apr 20;43(7):e47
pubmed: 25605792
NPJ Vaccines. 2021 May 21;6(1):78
pubmed: 34021167
PLoS One. 2017 Jan 18;12(1):e0167488
pubmed: 28099485
J Intern Med. 2016 Apr;279(4):337-46
pubmed: 26602369
Nat Rev Immunol. 2017 Nov;17(11):691-702
pubmed: 28736436
Vaccine. 2013 Apr 19;31(17):2196-206
pubmed: 22643213
Front Immunol. 2013 Apr 02;4:81
pubmed: 23565115
Sci Rep. 2019 Dec 30;9(1):20362
pubmed: 31889148
Immunol Res. 2011 Aug;50(2-3):202-12
pubmed: 21717066
Infect Immun. 1999 Aug;67(8):3998-4007
pubmed: 10417166
N Engl J Med. 2019 Dec 19;381(25):2429-2439
pubmed: 31661198
Nat Immunol. 2014 Feb;15(2):195-204
pubmed: 24336226
Microbiol Mol Biol Rev. 2014 Dec;78(4):650-71
pubmed: 25428938
Nat Rev Immunol. 2018 Sep;18(9):591-596
pubmed: 29872140
J Infect Dis. 2011 Apr 1;203(7):921-9
pubmed: 21357945
PLoS One. 2008 Jul 09;3(7):e2624
pubmed: 18612425
Enferm Infecc Microbiol Clin. 2010 Apr;28(4):245-52
pubmed: 19783328
Vaccine. 2019 Mar 28;37(14):2004-2015
pubmed: 30850240
Vaccine. 2015 Jul 31;33(32):4025-34
pubmed: 26072017
J Immunol. 2014 Aug 15;193(4):1920-30
pubmed: 25024381
N Engl J Med. 2018 Oct 25;379(17):1621-1634
pubmed: 30280651
Lancet. 2016 Jun 4;387(10035):2312-2322
pubmed: 27017310
Infect Immun. 1999 Jun;67(6):2941-50
pubmed: 10338503
Lancet. 2015 Jul 4;386(9988):31-45
pubmed: 25913272
Clin Immunol. 2016 Aug;169:16-27
pubmed: 27236001
Vaccine. 2018 Oct 8;36(42):6282-6289
pubmed: 30205979
Nat Med. 2019 Jun;25(6):977-987
pubmed: 31110348
Proc Natl Acad Sci U S A. 2017 Feb 28;114(9):2425-2430
pubmed: 28193898
Front Immunol. 2017 May 23;8:557
pubmed: 28588574
Nat Rev Dis Primers. 2016 Oct 27;2:16076
pubmed: 27784885
Front Immunol. 2018 Mar 26;9:564
pubmed: 29632533