Sialic acids on T cells are crucial for their maintenance and survival

Sialic acids are found as terminal sugars on glycan structures on cellular surfaces. T cells carry these sialoglycans abundantly, and they are thought to serve multiple functions in cell adhesion, cell migration, and protection from complement attack. We studied the role of sialoglycans on T cells i...

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Veröffentlicht in:Frontiers in immunology 2024-06, Vol.15, p.1359494
Hauptverfasser: Schmidt, Michael, Linder, Alexandra T, Korn, Marina, Schellenberg, Nick, Meyer, Sarah J, Nimmerjahn, Falk, Werner, Anja, Abeln, Markus, Gerardy-Schahn, Rita, Münster-Kühnel, Anja K, Nitschke, Lars
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Sprache:eng
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Zusammenfassung:Sialic acids are found as terminal sugars on glycan structures on cellular surfaces. T cells carry these sialoglycans abundantly, and they are thought to serve multiple functions in cell adhesion, cell migration, and protection from complement attack. We studied the role of sialoglycans on T cells in a mouse model with a T cell-specific deletion of cytidine monophosphate-sialic acid synthase (CMAS), the enzyme that is crucial for the synthesis of sialoglycans. These mice showed a T-cell deficiency in peripheral lymphoid organs. Many T cells with an undeleted allele were found in the periphery, suggesting that they escaped the Cre-mediated deletion. The remaining peripheral T cells of T cell-specific KO mice had a memory-like phenotype. Additional depletion of the complement factor C3 could not rescue the phenotype, showing that the T-cell defect was not caused by a host complement activity. -deficient T cells showed a high level of activated caspase 3, indicating an ongoing apoptosis. In bone marrow chimeric cellular transfer experiments, we observed a strong competitive disadvantage of -deficient T cells compared to wild-type T cells. These results show that sialoglycans on the surface of T cells are crucial for T-cell survival and maintenance. This function has not been recognized before and is similar to the function of sialoglycans on B cells.
ISSN:1664-3224
1664-3224
DOI:10.3389/fimmu.2024.1359494