AI Article Synopsis
- Mitochondria are vital organelles that undergo fusion and fission, regulated by proteins like Drp1, which is crucial for fission and maintaining the shape of mitochondria based on the cell's needs.
- Recent research has shown that mitochondrial dynamics significantly influence T cell differentiation and metabolism during immune responses.
- This review focuses on how Drp1-dependent fission affects T cell functions such as clonal expansion and migration, suggesting that targeting this process could lead to new therapies for enhancing T cell responses.
Article Abstract
Mitochondria are dynamic organelles whose processes of fusion and fission are tightly regulated by specialized proteins, known as mitochondria-shaping proteins. Among them, Drp1 is the main pro-fission protein and its activity is tightly regulated to ensure a strict control over mitochondria shape according to the cell needs. In the recent years, mitochondrial dynamics emerged as a new player in the regulation of fundamental processes during T cell life. Indeed, the morphology of mitochondria directly regulates T cell differentiation, this by affecting the engagment of alternative metabolic routes upon activation. Further, Drp1-dependent mitochondrial fission sustains both T cell clonal expansion and T cell migration and invasivness. By this review, we aim at discussing the most recent findings about the roles played by the Drp1-dependent mitochondrial fission in T cells, and at highlighting how its pharmacological modulation could open the way to future therapeutic approaches to modulate T cell response.
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| http://dx.doi.org/10.1016/j.phrs.2019.104317 | DOI Listing |
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