Rescuing ESAT-6 Specific CD4 T Cells From Terminal Differentiation Is Critical for Long-Term Control of Murine Mtb Infection

Helena Strand Clemmensen; Niels Peter Hell Knudsen; Rolf Billeskov; Ida Rosenkrands; Gregers Jungersen; Claus Aagaard; Peter Andersen; Rasmus Mortensen

doi:10.3389/fimmu.2020.585359

Rescuing ESAT-6 Specific CD4 T Cells From Terminal Differentiation Is Critical for Long-Term Control of Murine Mtb Infection

Front Immunol. 2020 Nov 6:11:585359. doi: 10.3389/fimmu.2020.585359. eCollection 2020.

Authors

Helena Strand Clemmensen^{1

2}, Niels Peter Hell Knudsen¹, Rolf Billeskov¹, Ida Rosenkrands¹, Gregers Jungersen^{1

2}, Claus Aagaard¹, Peter Andersen^{1

3}, Rasmus Mortensen¹

Affiliations

¹ Department of Infectious Disease Immunology, Statens Serum Institut, Copenhagen, Denmark.
² Department of Health Technology, Technical University of Denmark, Lyngby, Denmark.
³ Department of Immunology and Microbiology, University of Copenhagen, Copenhagen, Denmark.

Abstract

In most cases, Mycobacterium tuberculosis (Mtb) causes life-long chronic infections, which poses unique challenges for the immune system. Most of the current tuberculosis (TB) subunit vaccines incorporate immunodominant antigens and at this point, it is poorly understood how the CD4 T cell subsets recognizing these antigens are affected during long-term infection. Very little is known about the requirements for sustainable vaccine protection against TB. To explore this, we screened 62 human-recognized Mtb antigens during chronic murine Mtb infection and identified the four most immunodominant antigens in this setting (MPT70, Rv3020c, and Rv3019c and ESAT-6). Combined into a subunit vaccine, this fusion protein induced robust protection both in a standard short-term model and in a long-term infection model where immunity from BCG waned. Importantly, replacement of ESAT-6 with another ESAT-6-family antigen, Rv1198, led to similar short-term protection but a complete loss of bacterial control during chronic infection. This observation was further underscored, as the ESAT-6 containing vaccine mediated sustainable protection in a model of post-exposure vaccination, where the ESAT-6-replacement vaccine did not. An individual comparison of the CD4 T cell responses during Mtb infection revealed that ESAT-6-specific T cells were more terminally differentiated than the other immunodominant antigens and immunization with the ESAT-6 containing vaccine led to substantially greater reduction in the overall T cell differentiation status. Our data therefore associates long-term bacterial control with the ability of a vaccine to rescue infection-driven CD4T cell differentiation and future TB antigen discovery programs should focus on identifying antigens with the highest accompanying T cell differentiation, like ESAT-6. This also highlights the importance of long-term readouts in both preclinical and clinical studies with TB vaccines.

Keywords: ESAT-6; Mycobacterium tuberculosis; T cell differentiation; immunodominant antigens; long-term protection; mouse models; tuberculosis; vaccines.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antigens, Bacterial / immunology*
Bacterial Proteins / immunology*
CD4-Positive T-Lymphocytes / immunology*
Cell Differentiation / immunology
Female
Immunodominant Epitopes / immunology
Lymphocyte Activation / immunology
Mice
Mycobacterium tuberculosis
Tuberculosis / immunology*
Tuberculosis / prevention & control
Tuberculosis Vaccines / immunology*
Vaccines, Subunit / immunology

Substances

Antigens, Bacterial
Bacterial Proteins
ESAT-6 protein, Mycobacterium tuberculosis
Immunodominant Epitopes
Tuberculosis Vaccines
Vaccines, Subunit

Grants and funding

R01 AI135721/AI/NIAID NIH HHS/United States