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KMID : 0338420110260010019
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The Korean Journal of Internal Medicine
2011 Volume.26 No. 1 p.19 ~ p.24
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PPAR¥ã Agonist Beyond Glucose Lowering Effect
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Sugawara Akira
Uruno Akira
Kudo Masataka
Matsuda Ken
Yang Chul-Woo
Ito Sadayoshi
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Abstract
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The nuclear hormone receptor PPAR¥ã is activated by several agonists, including members of the thiazolidinedione group of insulin sensitizers. Pleiotropic beneficial effects of these agonists, independent of their blood glucose-lowering effects, have recently been demonstrated in the vasculature. PPAR¥ã agonists have been shown to lower blood pressure in animals and humans, perhaps by suppressing the renin-angiotensin (Ang)-aldosterone system (RAAS), including the inhibition of Ang II type 1 receptor expression, Ang-II-mediated signaling pathways, and Ang-II-induced adrenal aldosterone synthesis/secretion. PPAR¥ã agonists also inhibit the progression of atherosclerosis in animals and humans, possibly through a pathway involving the suppression of RAAS and the thromboxane A2 system, as well as the protection of endothelial function. Moreover, PPAR¥ã-agonist-mediated renal protection, especially the reduction of albuminuria, has been observed in diabetic nephropathy, including animal models of the disease, and in non-diabetic renal dysfunction. The renal protective activities may reflect, at least in part, the ability of PPAR¥ã agonists to lower blood pressure, protect endothelial function, and cause vasodilation of the glomerular efferent arterioles. Additionally, anti-neoplastic effects of PPAR¥ã agonists have recently been described. Based on the multiple therapeutic actions of PPAR¥ã agonists, they will no doubt lead to novel approaches in the treatment of lifestyle-related and other diseases.
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KEYWORD
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Thiazolidinediones, Angiotensin II, Thromboxane, Endothelium, Kidney
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