Abstract
Trained innate immunity has recently emerged as a novel concept of innate immune cells, such as myeloid cells, exhibiting immune memory, and nonspecific heterologous immunity to protect against infections. The memory and specificity are mediated by epigenetic, metabolic, and functional reprogramming of the myeloid cells and myeloid progenitors (and/or NK cells) in the bone marrow and peripheral tissues such as gut and lung mucosa. A variety of agents, such as BCG, viruses, and their components, as well as TLR agonists, and cytokines have been shown to be involved in the induction of trained immunity. Since these agents have been widely used in AIDS vaccine development as antigen delivery vectors or adjuvants, myeloid cell mediated trained immunity might also play an important role in protecting against mucosal AIDS virus transmission or in control of virus replication in the major gut mucosal reservoir. Here we review the trained innate immunity induced by these vectors/adjuvants that have been used in AIDS vaccine studies and discuss their role in mucosal vaccine efficacy and possible utilization in AIDS vaccine development. Delineating the protective effect of the trained innate immunity mediated by myeloid cells will guide the design of novel AIDS vaccines.
Highlights
Edited by: Maria Leite-de-Moraes, INSERM U1151 Institut Necker Enfants Malades Centre de Médecine Moléculaire (INEM), France
Trained innate immunity has recently emerged as a novel concept of innate immune cells, such as myeloid cells, exhibiting immune memory, and nonspecific heterologous immunity to protect against infections
Since these agents have been widely used in AIDS vaccine development as antigen delivery vectors or adjuvants, myeloid cell mediated trained immunity might play an important role in protecting against mucosal AIDS virus transmission or in control of virus replication in the major gut mucosal reservoir
Summary
Received: 17 December 2019 Accepted: 07 February 2020 Published: 28 February 2020. Citation: Sui Y and Berzofsky JA (2020) Myeloid Cell-Mediated Trained Innate Immunity in Mucosal AIDS Vaccine Development. We review data on trained immunity induced by these components in myeloid cells and discuss their possible involvement in mediating the vaccine efficacy of the previous published HIV vaccine studies. Previous reports found that MVA induced stronger IFN-stimulated genes, while NYVAC promoted proinflammatory genes after infection in HeLa cells [29, 30] These differences might lead to potentially different biological effects, though it remains unknown to what extent these induced innate immune profiles contributed to vaccine efficacy. Accumulating evidence showed that high IL-1β level, possibly as a inducer or as a mediator of trained immunity, plays an important role in protecting against bacteria, candida and viral infections [55,56,57,58] Another group of cytokines, which are widely induced by most vaccines, including HIV vaccines, are interferons (IFNs). Even AIDS viruses themselves can induce trained innate immunity
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