Cytokines tnfα, ifnϒ and il-2 are responsible for signal transmission from the innate immunity protein tag7 (Pglyrp1) to cytotoxic effector lymphocytes

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Abstract

Studies on the mechanisms of activation of cytotoxic lymphocyte subpopulations are an important research direction in modern immunology. This study provides a detailed analysis of the effect of Tag7 (PGRP-S, PGLYRP1) on the development of lymphocyte subpopulations cytotoxic against MHC-negative tumor cells in a pool of peripheral blood mononuclear cells (PBMCs). The results show that Tag7 can bind to the TREM-1 receptor on the surfaces of monocytes, thereby triggering the expression of mRNA TNF and IFN. The appearance of these cytokines in conditioned medium leads to IL-2 cytokine secretion by CD3+CD4+ lymphocytes. In turn, IL-2 facilitates unspecific activation of three cytotoxic cell subpopulations in the PBMC pool: NK (CD16+CD56+), CD3+CD4+ and CD3+CD8+. These subpopulations appear after a certain period of incubation with Tag7 and show toxicity against tumor cells.

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Sharapova, T. N., Romanova, E. A., Ivanova, O. K., Sashchenko, L. P., & Yashin, D. V. (2020). Cytokines tnfα, ifnϒ and il-2 are responsible for signal transmission from the innate immunity protein tag7 (Pglyrp1) to cytotoxic effector lymphocytes. Cells, 9(12), 1–11. https://doi.org/10.3390/cells9122602

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