Literature DB >> 3083202

Activation of human erythrocyte, brain, aorta, muscle, and ocular tissue aldose reductase.

S K Srivastava, N H Ansari, G A Hair, S Awasthi, B Das.   

Abstract

Based upon kinetic, structural, and immunologic properties, we have demonstrated that human tissues have three major forms of aldo-keto reductases: aldose reductase (AR), and aldehyde reductases I (AR I) and II (AR II). The proposed subunit compositions are AR, alpha; AR I, alpha-beta; and AR II, delta. Only AR can effectively reduce glucose to sorbitol. The beta subunits in AR I alter the substrate specificity of AR and prevent conformational changes required for the activation of alpha subunits. Partially purified AR (by DE-52) from human erythrocytes expresses biphasic kinetics with glucose and glyceraldehyde. The enzyme can be activated with glucose + glucose-6-P + NADPH and is strongly inhibited by sorbinil, alrestatin, and quercetrin, and by ADP, 2,3DPG, 1,3DPG, and 3PGA. The activated enzyme expresses monophasic kinetics with substrates (Km glucose less than 1 mmol/L) and is less susceptible to inhibition by synthetic AR inhibitors and phosphorylated intermediates. The enzyme from human brain, aorta, muscle, and ocular tissues was also activated under similar conditions. Erythrocyte enzyme was activated by incubation of blood with 30 to 50 mmol/L glucose. In diabetic subjects with blood sugar levels higher than 250 mg%, almost all the erythrocyte enzyme exists in the activated form. As demonstrated by enzyme-linked immunosorbent assay (ELISA), the increase in AR activity (in vivo and in vitro) was due to the activation of the enzyme and not to the de novo synthesis. In each case, the activation of the enzyme was confirmed by NADPH oxidation and the formation of proportionate amounts of sorbitol.

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Year:  1986        PMID: 3083202     DOI: 10.1016/0026-0495(86)90199-x

Source DB:  PubMed          Journal:  Metabolism        ISSN: 0026-0495            Impact factor:   8.694


  8 in total

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Review 2.  The efficacy of aldose reductase inhibitors in the management of diabetic complications. Comparison with intensive insulin treatment and pancreatic transplantation.

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3.  Altered aldose reductase gene regulation in cultured human retinal pigment epithelial cells.

Authors:  D N Henry; M Del Monte; D A Greene; P D Killen
Journal:  J Clin Invest       Date:  1993-08       Impact factor: 14.808

4.  Effects of aldose reductase inhibition with tolrestat on diabetic retinopathy in a six months double blind trial.

Authors:  J M van Gerven; J P Boot; H H Lemkes; J A van Best
Journal:  Doc Ophthalmol       Date:  1994       Impact factor: 2.379

5.  Effects of glucose, insulin or aldose reductase inhibition on responses to endothelin-1 of aortic rings from streptozotocin-induced diabetic rats.

Authors:  W C Hodgson; R G King
Journal:  Br J Pharmacol       Date:  1992-07       Impact factor: 8.739

Review 6.  The role of polyols in the pathophysiology of hypergalactosemia.

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7.  RALBP1 in Oxidative Stress and Mitochondrial Dysfunction in Alzheimer's Disease.

Authors:  Sanjay Awasthi; Ashly Hindle; Neha A Sawant; Mathew George; Murali Vijayan; Sudhir Kshirsagar; Hallie Morton; Lloyd E Bunquin; Philip T Palade; J Josh Lawrence; Hafiz Khan; Chhanda Bose; P Hemachandra Reddy; Sharda P Singh
Journal:  Cells       Date:  2021-11-10       Impact factor: 6.600

8.  Polyol pathway and modulation of ischemia-reperfusion injury in Type 2 diabetic BBZ rat hearts.

Authors:  Qing Li; Yuying C Hwang; Radha Ananthakrishnan; Peter J Oates; Dennis Guberski; Ravichandran Ramasamy
Journal:  Cardiovasc Diabetol       Date:  2008-10-28       Impact factor: 9.951

  8 in total

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