The role of endocytic trafficking in antigen T cell receptor activation

This review article summarizes the molecular mechanisms of T cell receptor (TCR) endocytosis and recycling, both in steady state and after T cell activation. It also discusses the experimental evidence in favor of endosomal TCR signaling and its possible consequences for T cell activation.

Like all the components of multicellular organisms, T lymphocytes constantly communicate with other cells and their extracellular environment. The plasma membrane plays an essential role in this communication since it expresses a plethora of receptors that are capable of detecting extracellular signals, either by binding soluble mediators, or by recognizing ligands expressed by other cells. The expression of these various receptors at the plasma membrane is precisely controlled by endocytosis, an active process by which small regions of the plasma membrane are internalized and form vesicles that undergo homotypic fusion to generate early endosomes (EE). EE are the main sorting hub for internalized plasma membrane receptors, which can be either recycled back to the plasma membrane, or delivered to lysosomes for degradation (Fig. 1) [1]. The balance between lysosomal degradation and endocytic recycling is essential to preserve a sufficient receptor pool for an optimal ability of cells to adapt to environmental changes. Even if the receptor pool is constantly replenished by newly synthesized molecules, the rate of protein synthesis cannot substitute for the endocytic recycling, which is a rapid and massive process. It is estimated that mammalian cells recycle at least half of their plasma membrane within an hour [2], which probably also applies to T cells. In comparison, protein half-life is much longer varying from 0.5 to 35 h in dividing mammalian cells [3]. Thus, the role of constitutive endocytic recycling on the receptor expression at the cell surface must be major. Beside its important role in regulating the cell surface receptor amounts, accumulating evidence supports the concept that endocytosis also promotes signaling amplification and signal diversification for several receptors that recruit signaling adaptors at the endosomal level [4].


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https://www.sciencedirect.com/science/article/pii/S2319417021001293




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David M. Ojcius, PhD - Editorial Board - Journals | Elsevier

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David Ojcius is Professor at the University of the Pacific in San Francisco, USA. He gained his Ph.D. from the University of California, Berkeley, and did research at Rockefeller and Harvard before moving to the Pasteur Institute in Paris, France, where he worked for thirteen years. His research interests include viruses and intracellular bacteria, interactions with the innate immune system, microbiota, biochemistry and cell biology of infected cells, inflammation and aging. https://www.journals.elsevier.com/current-research-in-microbial-sciences/editorial-board/david-m-ojcius-phd
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