2000
DOI: 10.2337/diabetes.49.6.1022
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Thiazolidinedione compounds ameliorate glomerular dysfunction independent of their insulin-sensitizing action in diabetic rats.

Abstract: Thiazolidinedione (TZD) compounds are widely used as oral hypoglycemic agents. Herein, we provide evidence showing that troglitazone, one of the TZD compounds, is able to prevent glomerular dysfunction in diabetic rats through a novel mechanism independent of its insulin-sensitizing action. We examined the effect of troglitazone on functional and biochemical parameters of glomeruli in streptozotocin-induced diabetic rats. Troglitazone was able to prevent not only diabetic glomerular hyperfiltration and albumin… Show more

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Cited by 172 publications
(137 citation statements)
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“…After washing, total cellular lipids were extracted from the cells according to the method of Bligh and Dyer (14). Total DAG contents were determined with a radio-enzymatic assay kit (Habersham, Arlington Heights, IL, USA) employing DG kinase (Caliches, San Diego, CA, USA), according to the instructions provided by the manufacturer, as previously described (5,8), which quantitatively converts DAG to [γ-32 P]-PA in the presence of [γ-32 P]-ATP (NEN, Boston, MA, USA) according to the instructions provided by the manufacturer. The resulting [γ-32 P]-PA was separated by silica-gel thin-layer plates (EM Separations, Gibbstown, NJ, USA) in a chamber containing chloroform/acetone/methanol/ acetic acid/water (10:4:3:2:1) according to the method of Priess et al (15).…”
Section: Culture Of Human Glomerular Mesangial Cellsmentioning
confidence: 99%
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“…After washing, total cellular lipids were extracted from the cells according to the method of Bligh and Dyer (14). Total DAG contents were determined with a radio-enzymatic assay kit (Habersham, Arlington Heights, IL, USA) employing DG kinase (Caliches, San Diego, CA, USA), according to the instructions provided by the manufacturer, as previously described (5,8), which quantitatively converts DAG to [γ-32 P]-PA in the presence of [γ-32 P]-ATP (NEN, Boston, MA, USA) according to the instructions provided by the manufacturer. The resulting [γ-32 P]-PA was separated by silica-gel thin-layer plates (EM Separations, Gibbstown, NJ, USA) in a chamber containing chloroform/acetone/methanol/ acetic acid/water (10:4:3:2:1) according to the method of Priess et al (15).…”
Section: Culture Of Human Glomerular Mesangial Cellsmentioning
confidence: 99%
“…Intracellular hyperglycemia promotes abnormal DAG accumulation from de novo synthesis, and high levels of DAG induce the activation of PKC. High DAG levels and PKC activation have been demonstrated in vascular tissues including the kidneys of diabetic animals (5-7), as well as in cultured renal vascular cells exposed to high glucose (7)(8)(9)(10). DAG is converted by diacylglycerol kinase (DGK) to phosphatidic acid (PA), and enhanced DGK activity leads to a reduction in excess DAG accumulation induced by high glucose, resulting in reduced PKC activation.…”
Section: Introductionmentioning
confidence: 99%
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“…It is unclear, however, whether different antihyperglycemic agents have specific antialbuminuria effects independent of their blood glucose-lowering effects. Animal data and short-term studies in humans suggest that thiazolidinediones that have anti-inflammatory properties and affect levels of adipokines and cytokines may be more potent at lowering albuminuria and preventing its rise than other oral glucose-lowering agents (5)(6)(7).…”
Section: Introductionmentioning
confidence: 99%
“…146 Beyond their hypoglycemic actions, PPARЎ agonists exert a number of beneficial effects in diabetes including improvement in endothelial function, 147,148 reduction in pro-atherogenic inflammatory markers 149 and angiotensin-I and -II, 150 down regulation of AT 1 mRNA and protein in vascular smooth muscle cells, 151,152 decrease in urine endothelin-1 secretion, 153 attenuated lipid accumulation and its related injury in mesangial cells, 154,155 and inhibition of glomerular and tubular cell proliferation 156,157 . Several animal [158][159][160][161][162][163] and human studies 153,[164][165][166][167][168][169][170][171][172][173][174][175] using various TZDs have demonstrated a reduction in proteinuria and BP. Unfortunately; most of these studies were of short duration averaging 1-9 months in the animal studies 158-163 and 3-12 months in human studies.…”
Section: Emerging Therapeutic Agents For Diabetic Nephropathy Thiazolmentioning
confidence: 99%