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First Insight into the Kinome of Human Regulatory T Cells

Overview of attention for article published in PLOS ONE, July 2012
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Title
First Insight into the Kinome of Human Regulatory T Cells
Published in
PLOS ONE, July 2012
DOI 10.1371/journal.pone.0040896
Pubmed ID
Authors

Sebastian König, Michael Probst-Kepper, Tobias Reinl, Andreas Jeron, Jochen Huehn, Burkhart Schraven, Lothar Jänsch

Abstract

Regulatory T cells (Tregs) are essential for controlling peripheral tolerance by the active suppression of various immune cells including conventional T effector cells (Teffs). Downstream of the T cell receptor (TCR), more than 500 protein kinases encoded by the human genome have to be considered in signaling cascades regulating the activation of Tregs and Teffs, respectively. Following TCR engagement, Tregs posses a number of unique attributes, such as constitutive expression of Foxp3, hyporesponsiveness and poor cytokine production. Furthermore, recent studies showed that altered regulation of protein kinases is important for Treg function. These data indicate that signaling pathways in Tregs are distinctly organized and alterations at the level of protein kinases contribute to the unique Treg phenotype. However, kinase-based signaling networks in Tregs are poorly understood and necessitate further systematic characterization. In this study, we analyzed the differential expression of kinases in Tregs and Teffs by using a kinase-selective proteome strategy. In total, we revealed quantitative information on 185 kinases expressed in the human CD4(+) T cell subsets. The majority of kinases was equally abundant in both T cell subsets, but 11 kinases were differentially expressed in Tregs. Most strikingly, Tregs showed an altered expression of cell cycle kinases including CDK6. Quantitative proteomics generates first comparative insight into the kinase complements of the CD4(+) Teff and Treg subset. Treg-specific expression pattern of 11 protein kinases substantiate the current opinion that TCR-mediated signaling cascades are altered in Tregs and further suggests that Tregs exhibit significant specificities in cell-cycle control and progression.

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Geographical breakdown

Country Count As %
United States 1 2%
Germany 1 2%
Unknown 60 97%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 17 27%
Researcher 14 23%
Professor 6 10%
Student > Master 6 10%
Student > Bachelor 4 6%
Other 11 18%
Unknown 4 6%
Readers by discipline Count As %
Agricultural and Biological Sciences 28 45%
Medicine and Dentistry 9 15%
Immunology and Microbiology 9 15%
Chemistry 5 8%
Biochemistry, Genetics and Molecular Biology 4 6%
Other 3 5%
Unknown 4 6%