Beyond target cell death - Granzyme serine proteases in health and disease
Journal Title
Molecular Aspects of Medicine
Publication Type
Review
Abstract
Granzymes are a family of small ( approximately 32 kDa) serine proteases with a range of substrate specificities that are stored in, and released from, the cytoplasmic secretory vesicles ('granules') of cytotoxic T lymphocytes and natural killer cells. Granzymes are not digestive proteases but finely tuned processing enzymes that target their substrates in specific ways to activate various signalling pathways, or to inactivate viral proteins and other targets. Great emphasis has been placed on studying the pro-apoptotic functions of granzymes, which largely depend on their synergy with the pore-forming protein perforin, on which they rely for penetration into the target cell cytosol to access their substrates. While a critical role for granzyme B in target cell apoptosis is undisputed, both it and the remaining granzymes also influence a variety of other biological processes (including important immunoregulatory functions), which are discussed in this review. This includes the targeting of many extracellular as well as intracellular substrates, and can also lead to deleterious outcomes for the host if granzyme expression or function are dysregulated or abrogated. A final important consideration is that granzyme repertoire, biochemistry and function vary considerably across species, probably resulting from the pressures applied by viruses and other pathogens across evolutionary time. This has implications for the interpretation of granzyme function in preclinical models of disease.
Keywords
Humans; *Serine; Granzymes/genetics/metabolism; Perforin; *T-Lymphocytes, Cytotoxic/metabolism; Killer Cells, Natural/metabolism; Caspases; Apoptosis
Department(s)
Laboratory Research
PubMed ID
36368281
Terms of Use/Rights Notice
Refer to copyright notice on published article.


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