Prostaglandin F₂α elevates blood pressure and promotes atherosclerosis

Prostaglandin F₂α elevates blood pressure and promotes atherosclerosis

Little is known about prostaglandin F₂α in cardiovascular homeostasis. Prostaglandin F₂α dose-dependently elevates blood pressure in WT mice via activation of the F prostanoid (FP) receptor. The FP is expressed in preglomerular arterioles, renal collecting ducts, and the hypothalamus. Deletion of th...

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Bibliographic Details
Published in:Proceedings of the National Academy of Sciences - PNAS Vol. 106; no. 19; pp. 7985 - 7990
Main Authors: Yu, Ying, Lucitt, Margaret B, Stubbe, Jane, Cheng, Yan, Friis, Ulla G, Hansen, Pernille B, Jensen, Boye L, Smyth, Emer M, FitzGerald, Garret A
Format: Journal Article
Language:English
Published: National Academy of Sciences 12-05-2009
National Acad Sciences
Subjects:
Biological Sciences
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Summary:Little is known about prostaglandin F₂α in cardiovascular homeostasis. Prostaglandin F₂α dose-dependently elevates blood pressure in WT mice via activation of the F prostanoid (FP) receptor. The FP is expressed in preglomerular arterioles, renal collecting ducts, and the hypothalamus. Deletion of the FP reduces blood pressure, coincident with a reduction in plasma renin concentration, angiotensin, and aldosterone, despite a compensatory up-regulation of AT1 receptors and an augmented hypertensive response to infused angiotensin II. Plasma and urinary osmolality are decreased in FP KOs that exhibit mild polyuria and polydipsia. Atherogenesis is retarded by deletion of the FP, despite the absence of detectable receptor expression in aorta or in atherosclerotic lesions in Ldlr KOs. Although vascular TNFα, inducible nitric oxide enzyme and TGFβ are reduced and lesional macrophages are depleted in the FP/Ldlr double KOs, this result reflects the reduction in lesion burden, as the FP is not expressed on macrophages and its deletion does not alter macrophage cytokine generation. Blockade of the FP offers an approach to the treatment of hypertension and its attendant systemic vascular disease.
Bibliography:Author contributions: Y.Y., M.B.L., and G.A.F. designed research; Y.Y., M.B.L., J.S., Y.C., U.G.F., P.B.H., B.L.J., and E.M.S. performed research; Y.Y. and M.B.L. analyzed data; and Y.Y., M.B.L., and G.A.F. wrote the paper.
1Y.Y. and M.B.L. contributed equally to this work.
Edited by Bengt Samuelsson, Karolinska Institutet, Stockholm, Sweden, and approved March 26, 2009
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.0811834106