T cell responses: naive to memory and everything in between
Autor: | Eric W. Cross, Elizabeth E. Cheney, Beth A. Jirón Tamburini, Ross M. Kedl, Jason T. White, Nathan D. Pennock |
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Rok vydání: | 2013 |
Předmět: |
Innate immune system
Physiology T cell T-Lymphocytes Antigen presentation Innate lymphoid cell Lymphokine Refresher Course Cell Differentiation General Medicine Biology Acquired immune system Lymphocyte Activation Education B-1 cell Immune system medicine.anatomical_structure Immunology medicine Humans Neuroscience Immunologic Memory |
Zdroj: | Advances in physiology education. 37(4) |
ISSN: | 1522-1229 |
Popis: | THE MAMMALIAN IMMUNE SYSTEM can be broadly divided into two main arms: innate and adaptive immunity. As its name implies, the cells and receptors of the innate immune system are critical for the rapid recognition of the infectious agent and initiating a proinflammatory response. While the inflammation generated by innate immune cells [neutrophils, macrophages, monocytes, natural killer (NK) cells, dendritic cells (DCs), etc.] is important in the initial containment of the infection, it also informs and directs the expansion and differentiation of adaptive immune cells. Responding to the inflammatory environment created by the innate response, cells of the adaptive arm of the immune response (B cells, T cells, and T cells) are stimulated to expand in number (proliferate) and to differentiate into cells with a range of functions appropriate for the immunological challenge. Upon elimination of the invading pathogen, the majority of adaptive cells die and leave behind an (evergrowing) array of memory cell subsets. These memory cells offer a diversity of migratory properties and functions, collectively mediating a rapid and protective immune response upon reinfection. Thus, the major advantages of an adaptive response to the host are twofold. First, it allows the host to form an immune response that is specifically tailored to the invading pathogen. Second, it forms a pool of memory cells from these specific effectors that can last for many years, capable of protecting the host against reinfection by their rapid response. This combination of specificity and memory are the mechanistic underpinnings for the clinical success of vaccination. Critical to almost all functions of the adaptive immune response is the activation and programming of T cells from their naive/resting state. Although there is much more to be learned, we now have a good basic understanding of the signals and cell types involved in the various stages of the T cell response initiated within the secondary lymphoid organs (SLOs). To provide a comprehensive overview, this review will summarize the T cell response broken down into three major stages: activation, differentiation, and memory formation. We will then assemble these components into a description of the anatomy of an immune response and its relationship to productive immune protection. |
Databáze: | OpenAIRE |
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