Varatharajan Sudhahar
University of Madras
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Publication
Featured researches published by Varatharajan Sudhahar.
Journal of Natural Products | 2008
Varatharajan Sudhahar; Coothan Kandaswamy Veena; Palaninathan Varalakshmi
The present study was undertaken to explore the efficiency of the pentacyclic triterpene lupeol (1) and its ester derivative, lupeol linoleate (2), in experimental hyperoxaluria. Hyperoxaluria was induced in male Wistar rats with 0.75% ethylene glycol (EG) in drinking water for 28 days. Hyperoxaluric animals were supplemented orally with 1 and 2 (50 mg/kg body wt/day) throughout the experimental period of 28 days. The renal enzymes were assayed as markers of renal tissue integrity. The redox status and oxalate metabolism in animals under oxalate overloading was also assessed. Microscopic analysis was done to investigate the abnormalities associated with oxalate exposure in renal tissues. Increase in oxidative milieu in hyperoxaluria was evident by increased lipid peroxidation (LPO) and decreased enzymic and nonenzymic antioxidants. Decrease in the activities of renal enzymes exemplified the damage induced by oxalate, which correlated positively with increased LPO and increased oxalate synthesis. Renal microscopic analysis further emphasized the oxalate-induced damage. These abnormal biochemical and histological aberrations were attenuated with test compound treatment, with 2 more effective than 1. From the present study, it can be concluded that 1 and 2 may serve as candidates for alleviating oxalate toxicity.
Journal of Pharmacy and Pharmacology | 2005
Periyasamy Thandavan Sudharsan; Yenjerla Mythili; Varatharajan Sudhahar; Palaninathan Varalakshmi
Cyclophosphamide, an alkylating agent widely used in cancer chemotherapy, causes fatal cardiotoxicity. In this study, lupeol, a pentacyclic triterpene isolated from Crataeva nurvala stem bark, and its ester, lupeol linoleate, were investigated for their possible hypocholesterolaemic effects against cyclophosphamide‐induced lipidaemic instabilities. Male albino Wistar rats were categorized into 6 groups. Group I served as control. Rats in groups II, V and VI were injected intraperitoneally with a single dose of cyclophosphamide (200 mg kg−1) dissolved in saline. Cyclophosphamide‐treated groups V and VI respectively received lupeol and lupeol linoleate (50 mg kg−1), dissolved in olive oil, for 10 days by oral gavage. Groups III and IV served as drug controls and were administered lupeol and lupeol linoleate, respectively. Cyclophosphamide administration induced abnormal changes in serum lipoproteins and lipid fractions in both serum and cardiac tissue. The activity of lipid metabolizing enzymes was distorted significantly in the cyclophosphamide‐treated rats. The cyclophosphamide‐treated rats also showed extensive intermuscular haemorrhage in histology. Lupeol and its ester reversed the above alterations induced by cyclophosphamide. This study encapsulates the early lipaemic abnormalities in the heart tissue of cyclophosphamide‐treated rats. Treatment with lupeol linoleate was more effective than lupeol in rendering protection to the cardiac tissue challenged by cyclophosphamide.
Life Sciences | 2006
Varatharajan Sudhahar; Sekar Ashok Kumar; Palaninathan Varalakshmi
Vascular Pharmacology | 2007
Varatharajan Sudhahar; Sekar Ashok Kumar; Periyasamy Thandavan Sudharsan; Palaninathan Varalakshmi
Molecular and Cellular Biochemistry | 2008
Varatharajan Sudhahar; S. Ashok Kumar; Palaninathan Varalakshmi; V. Sujatha
Atherosclerosis | 2006
Sekar Ashok Kumar; Varatharajan Sudhahar; Palaninathan Varalakshmi
Nutrition Research | 2007
Varatharajan Sudhahar; Sekar Ashok Kumar; Yenjerla Mythili; Palaninathan Varalakshmi
Molecular and Cellular Biochemistry | 2007
Varatharajan Sudhahar; S. Ashok Kumar; Palaninathan Varalakshmi; R. Sundarapandiyan
European Journal of Pharmacology | 2006
Yenjerla Mythili; Periyasamy Thandavan Sudharsan; Varatharajan Sudhahar; Palaninathan Varalakshmi
Clinica Chimica Acta | 2005
Sekar Ashok Kumar; Varatharajan Sudhahar; Palaninathan Varalakshmi