the pi3k p110δ regulates expression of cd38 on regulatory t cellspi3k p110δ调节表达cd38的调节性t细胞.pdfVIP
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the pi3k p110δ regulates expression of cd38 on regulatory t cellspi3k p110δ调节表达cd38的调节性t细胞
The PI3K p110d Regulates Expression of CD38 on
Regulatory T Cells
1 1 2 1 1
Daniel T. Patton , Marcus D. Wilson , Wendy C. Rowan , Dalya R. Soond , Klaus Okkenhaug *
1 Laboratory of Lymphocyte Signalling and Development, Babraham Institute, Cambridge, United Kingdom, 2 Tool Monoclonal Antibody Group, GlaxoSmithKline
Research and Development, Stevenage, United Kingdom
Abstract
The PI3K pathway has emerged as a key regulator of regulatory T cell (Treg) development and homeostasis and is required
for full Treg-mediated suppression. To identify new genes involved in PI3K-dependent suppression, we compared the
transcriptome of WT and p110dD910A Tregs. Among the genes that were differentially expressed was the gene for the
transmembrane cyclic ADP ribose hydrolase CD38. Here we show that CD38 is expressed mainly by a subset of
Foxp3+ + + high
CD25 CD4 T cells originating in the thymus and on Tregs in the spleen. CD38 WT Tregs showed superior
suppressive activity to CD38low Tregs, which failed to upregulate CD73, a surface protein which is important for suppression.
However, Tregs from heterozygous CD38+/ 2 mice were unimpaired despite lower levels of CD38 expression. Therefore,
CD38 can be used as a marker for Tregs with high suppressive activity and the impaired Treg function in p110dD910A mice
can in part be explained by the failure of CD38high cells to develop.
Citation: Patton DT, Wilson MD, Rowan WC, Soond DR, Okkenhaug K (2011) The PI3K p110d Regulates Expression of CD38 on Regulatory T
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