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Tuberculosis-Cancer Parallels in Immune Response Regulation

期刊

出版社

MDPI
DOI: 10.3390/ijms21176136

关键词

immunotherapy; Mycobacterium tuberculosis; radiation therapy; tumor immunology

资金

  1. University of Colorado Anschutz Medical Campus Lung Head and Neck Cancer T32 training program (Ruth L. Kirschstein National Research Service Award) [T32CA17468]
  2. NIDCR [R01 DE028529, R01 DE028282]

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Mycobacterium tuberculosisand cancer are two diseases with proclivity for the development of resistance to the host immune system. Mechanisms behind resistance can be host derived or disease mediated, but they usually depend on the balance of pro-inflammatory to anti-inflammatory immune signals. Immunotherapies have been the focus of efforts to shift that balance and drive the response required for diseases eradication. The immune response to tuberculosis has widely been thought to be T cell dependent, with the majority of research focused on T cell responses. However, the past decade has seen greater recognition of the importance of the innate immune response, highlighting factors such as trained innate immunity and macrophage polarization to mycobacterial clearance. At the same time, there has been a renaissance of immunotherapy treatments for cancer since the first checkpoint inhibitor passed clinical trials, in addition to work highlighting the importance of innate immune responses to cancer. However, there is still much to learn about host-derived responses and the development of resistance to new cancer therapies. This review examines the similarities between the immune responses to cancer and tuberculosis with the hope that their commonalities will facilitate research collaboration and discovery.

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