Sushma Ramprasad scite author profile

Sushma Ramprasad

4Publications

39Citation Statements Received

41Citation Statements Given

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Affiliations

University of Pennsylvania, Dr. Mohan's Diabetes Specialities Centre, Madras Diabetes Research Foundation

Publications

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Rage gene promoter polymorphisms and diabetic retinopathy in a clinic-based population from South India

Ramprasad

Radha

Mathias

et al. 2006

Eye

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Purpose The main objective of this study was to evaluate if the À429T/C, À374T/A and 63 bp deletion polymorphisms in the RAGE gene are associated with diabetic retinopathy (DR) among Type 2 diabetic subjects in a clinicbased population from South India. Methods We screened 149 normal glucose tolerant subjects (NGT), 189 Type 2 diabetes subjects without retinopathy (DM) and 190 subjects with DR for these polymorphisms using the PCR-RFLP method. DR was diagnosed by grading color fundus photography. Logistic regression models were used to evaluate the association of individual polymorphisms with DR. Expectationmaximization algorithms were implemented in haplotype tests of association to examine the combined effects of À429T/C and À374T/A polymorphisms on DR. Results The allelic frequencies of À429T are 0.83 in NGT, 0.84 in DM and 0.85 in DR subjects, and that of À374T are 0.93 in NGT, 0.92 in DM and 0.88 in DR subjects. The À374 polymorphism was found to be associated with non-proliferative retinopathy when this subgroup was compared to the DM group (OR ¼ 1.814, 95% CI ¼ 1.005-3.273). However, this association was not obvious when both the subphenotypes of DR (the nonproliferative and proliferative DR groups) were studied jointly. We found no evidence for associations between the À429T/C polymorphism and the DR phenotype. Finally, extension to a 2-SNP haplotype did not reveal any significant statistical difference between the groups (P ¼ 0.668).

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103: Changes in Core Temperature Are Related to Free Fatty Acid Rebound from Niacin

Gadi

Dunbar

Lily

et al. 2008

Journal of Clinical Lipidology

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432Pathologic Pyelonephritis In Kidney Transplant Recipients: Bacterial Infection?

Ramprasad¹,

Huang²,

Fischer³

2014

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Abstract 3705: Pioglitazone Augments Niacin-Induced Increases in Adiponectin in Non-Diabetics with Metabolic Syndrome and Low HDL

et al. 2008

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Background Niacin and pioglitazone (PIO) increase HDL by uncertain mechanisms. Both increase adiponectin, whose effects on carbohydrate and fatty acid metabolism may benefit HDL indirectly. Little is known of the combined effects of the drugs on adiponectin and other adipokines. We hypothesized that PIO would complement changes in adipokines from niacin, and in turn, augment HDL. Methods In an open-label run-in, non-diabetics with low HDL titrated from 0 to 2 g extended-release niacin over 4 weeks, and were randomized to add PIO 30 mg or placebo in a double-blind manner. After 6 weeks, PIO was increased to 45 mg for another 6 weeks. We assessed changes in fasting adiponectin, resistin, complement C3 (the serum-detectable precursor of acylation stimulating protein), free fatty acids (FFA), hydroxy-butyrate (HBA), and triglycerides (TG), and their relationship to changes in HDL. Results Of 72 completers, 34 took niacin and placebo and 38 took niacin and PIO. The table shows absolute and relative change of each analyte from baseline to 16 weeks. Relative change in adiponectin was strongly correlated with change in HDL (Spearman’s rho +0.49, p<0.0001), as was change in TG (rho −0.50, p<0.0001); the other analytes had little influence. On multivariable regression, change in HDL was predicted by change in adiponectin (p=0.0001) and TG (p<0.0001), which remained significant on adjustment for changes in glucose and insulin. Conclusion Pioglitazone augments niacin-induced changes in adiponectin and complement C3 thought to be favorable, and neutralizes niacin’s unfavorable increase in FFA. Adiponectin strongly predicted HDL after adjustment for TG. Since PIO had no independent effect on TG, we speculate that additional HDL-raising from PIO is mediated by the large increase in adiponectin. In summary, PIO enhances HDL-raising from niacin in proportion to increased adiponectin.

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