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Trained Immunity: Long-Term Adaptation in Innate Immune Responses

Journal

Publisher

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1161/ATVBAHA.120.314212

Keywords

epigenomics; immunity; innate; macrophages; metabolism

Funding

  1. IN-CONTROL CVON (Netherlands CardioVascular Research Initiative) [CVON2012-03, CVON2018-27]
  2. European Union Horizon 2020 research and innovation program REPROGRAM [667837]
  3. European Research Council (ERC) [ERC 833247]
  4. Netherlands Organization for Scientific Research Spinoza Grant [NWO SPI 94-212]
  5. Competitiveness Operational Programme grant of the Romanian Ministry of European Funds (HINT) [P_37_762, 103587]
  6. ERA-CVD (European Research Area-Cardiovascular Disease) Joint Transnational Call 2018 - Dutch Heart Foundation (JTC2018) [2018T093]
  7. Dutch Heart Foundation (Dekker grant) [2018T028]

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Trained immunity is a persistent hyperresponsive phenotype developed by innate immune cells after stimulation, causing cells to remember pathogens and endogenous molecules. While providing cross-protection in infectious diseases, trained immunity may lead to excessive immune responses in diseases driven by chronic systemic inflammation.
Adaptive immune responses are characterized by antigen specificity and induction of lifelong immunologic memory. Recently, it has been reported that innate immune cells can also build immune memory characteristics-a process termed trained immunity. Trained immunity describes the persistent hyperresponsive phenotype that innate immune cells can develop after brief stimulation. Pathogenic stimuli such as microorganisms, and also endogenous molecules including uric acid, oxidized LDL (low-density lipoprotein), and catecholamines, are capable of inducing memory in monocytes and macrophages. While trained immunity provides favorable cross-protection in the context of infectious diseases, the heightened immune response can be maladaptive in diseases driven by chronic systemic inflammation, such as atherosclerosis. Trained immunity is maintained by distinct epigenetic and metabolic mechanisms and persists for at least several months in vivo due to reprogramming of myeloid progenitor cells. Additionally, certain nonimmune cells are also found to exhibit trained immunity characteristics. Thus, trained immunity presents an exciting framework to develop new approaches to vaccination and also novel pharmacological targets in the treatment of inflammatory diseases.

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