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Citations to this article

The multistage vaccine H56 boosts the effects of BCG to protect cynomolgus macaques against active tuberculosis and reactivation of latent Mycobacterium tuberculosis infection
Philana Ling Lin, … , JoAnne L. Flynn, Peter Andersen
Philana Ling Lin, … , JoAnne L. Flynn, Peter Andersen
Published December 1, 2011
Citation Information: J Clin Invest. 2012;122(1):303-314. https://doi.org/10.1172/JCI46252.
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Research Article Immunology Article has an altmetric score of 7

The multistage vaccine H56 boosts the effects of BCG to protect cynomolgus macaques against active tuberculosis and reactivation of latent Mycobacterium tuberculosis infection

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Abstract

It is estimated that one-third of the world’s population is infected with Mycobacterium tuberculosis. Infection typically remains latent, but it can reactivate to cause clinical disease. The only vaccine, Mycobacterium bovis bacillus Calmette-Guérin (BCG), is largely ineffective, and ways to enhance its efficacy are being developed. Of note, the candidate booster vaccines currently under clinical development have been designed to improve BCG efficacy but not prevent reactivation of latent infection. Here, we demonstrate that administering a multistage vaccine that we term H56 in the adjuvant IC31 as a boost to vaccination with BCG delays and reduces clinical disease in cynomolgus macaques challenged with M. tuberculosis and prevents reactivation of latent infection. H56 contains Ag85B and ESAT-6, which are two of the M. tuberculosis antigens secreted in the acute phase of infection, and the nutrient stress–induced antigen Rv2660c. Boosting with H56/IC31 resulted in efficient containment of M. tuberculosis infection and reduced rates of clinical disease, as measured by clinical parameters, inflammatory markers, and improved survival of the animals compared with BCG alone. Boosted animals showed reduced pulmonary pathology and extrapulmonary dissemination, and protection correlated with a strong recall response against ESAT-6 and Rv2660c. Importantly, BCG/H56-vaccinated monkeys did not reactivate latent infection after treatment with anti-TNF antibody. Our results indicate that H56/IC31 boosting is able to control late-stage infection with M. tuberculosis and contain latent tuberculosis, providing a rationale for the clinical development of H56.

Authors

Philana Ling Lin, Jes Dietrich, Esterlina Tan, Rodolfo M. Abalos, Jasmin Burgos, Carolyn Bigbee, Matthew Bigbee, Leslie Milk, Hannah P. Gideon, Mark Rodgers, Catherine Cochran, Kristi M. Guinn, David R. Sherman, Edwin Klein, Christopher Janssen, JoAnne L. Flynn, Peter Andersen

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Total citations by year

Year: 2025 2024 2023 2022 2021 2020 2019 2018 2017 2016 2015 2014 2013 2012 2009 Total
Citations: 1 8 8 7 9 5 8 8 10 15 15 17 6 2 1 120
Citation information
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Citations to this article in year 2016 (15)

Title and authors Publication Year
Current status of new tuberculosis vaccine in children
Y Pang, A Zhao, C Cohen, W Kang, J Lu, G Wang, Y Zhao, S Zheng
Human Vaccines & Immunotherapeutics 2016
Heterologous boosting with recombinant VSV-846 in BCG-primed mice confers improved protection against Mycobacterium infection
M Zhang, C Dong, S Xiong
Human Vaccines & Immunotherapeutics 2016
CD4+ T Cells Recognizing PE/PPE Antigens Directly or via Cross Reactivity Are Protective against Pulmonary Mycobacterium tuberculosis Infection
F Sayes, A Pawlik, W Frigui, MI Gröschel, S Crommelynck, C Fayolle, F Cia, GJ Bancroft, D Bottai, C Leclerc, R Brosch, L Majlessi, DM Lewinsohn
PLoS pathogens 2016
Subunit vaccine H56/CAF01 induces a population of circulating CD4 T cells that traffic into the Mycobacterium tuberculosis-infected lung
JS Woodworth, SB Cohen, AO Moguche, CR Plumlee, EM Agger, KB Urdahl, P Andersen
Mucosal Immunology 2016
A multistage mycobacterium tuberculosis subunit vaccine LT70 including latency antigen Rv2626c induces long-term protection against tuberculosis
X Liu, J Peng, L Hu, Y Luo, H Niu, C Bai, Q Wang, F Li, H Yu, B Wang, H Chen, M Guo, B Zhu
Human Vaccines & Immunotherapeutics 2016
Strategic Priming with Multiple Antigens can Yield Memory Cell Phenotypes Optimized for Infection with Mycobacterium tuberculosis: A Computational Study
C Ziraldo, C Gong, DE Kirschner, JJ Linderman
Frontiers in microbiology 2016
The Progress of Therapeutic Vaccination with Regard to Tuberculosis
PJ Cardona
Frontiers in microbiology 2016
Novel adjuvant formulations for delivery of anti-tuberculosis vaccine candidates
EM Agger
Advanced Drug Delivery Reviews 2016
The Zebrafish Breathes New Life into the Study of Tuberculosis
H Myllymäki, CA Bäuerlein, M Rämet
Frontiers in immunology 2016
BCG and New Preventive Tuberculosis Vaccines: Implications for Healthcare Workers
M Hatherill, TJ Scriba, ZF Udwadia, JB Mullerpattan, A Hawkridge, H Mahomed, C Dye
Clinical Infectious Diseases 2016
Testing the H56 Vaccine Delivered in 4 Different Adjuvants as a BCG-Booster in a Non-Human Primate Model of Tuberculosis
R Billeskov, EV Tan, M Cang, RM Abalos, J Burgos, BV Pedersen, D Christensen, EM Agger, P Andersen, AA Izzo
PloS one 2016
PET CT Identifies Reactivation Risk in Cynomolgus Macaques with Latent M. tuberculosis
PL Lin, P Maiello, HP Gideon, MT Coleman, AM Cadena, MA Rodgers, R Gregg, M OMalley, J Tomko, D Fillmore, LJ Frye, T Rutledge, RM DiFazio, C Janssen, E Klein, PL Andersen, SM Fortune, JA Flynn, MA Behr
PLoS pathogens 2016
Comparative Systems Analyses Reveal Molecular Signatures of Clinically tested Vaccine Adjuvants
TA Olafsdottir, M Lindqvist, I Nookaew, P Andersen, J Maertzdorf, J Persson, D Christensen, Y Zhang, J Anderson, S Khoomrung, P Sen, EM Agger, R Coler, D Carter, A Meinke, R Rappuoli, SH Kaufmann, SG Reed, AM Harandi
Scientific Reports 2016
Novel vaccination approaches to prevent tuberculosis in children
JA Triccas, C Counoupas
Pneumonia 2016
Mycobacterium tuberculosis multistage antigens confer comprehensive protection against pre- and post-exposure infections by driving Th1-type T cell immunity
J Ma, M Tian, X Fan, Q Yu, Y Jing, W Wang, L Li, Z Zhou
Oncotarget 2016

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