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Distinct roles of prostaglandin H synthases 1 and 2 in T-cell development
Bianca Rocca, … , Carlo Patrono, Garret A. FitzGerald
Bianca Rocca, … , Carlo Patrono, Garret A. FitzGerald
Published May 15, 1999
Citation Information: J Clin Invest. 1999;103(10):1469-1477. https://doi.org/10.1172/JCI6400.
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Article

Distinct roles of prostaglandin H synthases 1 and 2 in T-cell development

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Abstract

Prostaglandin G and H synthases, or cyclooxygenases (COXs), catalyze the formation of prostaglandins (PGs). Whereas COX-1 is diffusely expressed in lymphoid cells in embryonic day 15.5 thymus, COX-2 expression is sparse, apparently limited to stromal cells. By contrast, COX-2 is predominant in a subset of medullary stromal cells in three- to five-week-old mice. The isozymes also differ in their contributions to lymphocyte development. Thus, experiments with selective COX-1 inhibitors in thymic lobes from normal and recombinase-activating gene-1 knockout mice support a role for this isoform in the transition from CD4–CD8– double-negative (DN) to CD4+CD8+ double-positive (DP). Concordant data were obtained in COX-1 knockouts. Pharmacological inhibition and genetic deletion of COX-2, by contrast, support its role during early thymocyte proliferation and differentiation and, later, during maturation of the CD4 helper T-cell lineage. PGE2, but not other PGs, can rescue the effects of inhibition of either isoform, although it acts through distinct EP receptor subtypes. COX-dependent PG generation may represent a mechanism of thymic stromal support for T-cell development.

Authors

Bianca Rocca, Lisa M. Spain, Ellen Puré, Robert Langenbach, Carlo Patrono, Garret A. FitzGerald

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Relative concentration of COX inhibitors required for the increase in th...

Relative concentration of COX inhibitors required for the increase in the percentage of CD4—CD8— cells, reduction in CD4+CD8+ absolute numbers and COX-1 inhibition.


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