Literature DB >> 12901025

Overview of niacin formulations: differences in pharmacokinetics, efficacy, and safety.

John A Pieper1.   

Abstract

The pharmacokinetics, efficacy, and safety of niacin and its various formulations are discussed. Niacin has been used for decades for the treatment of dyslipidemia because of its favorable effects on all lipoprotein parameters. Niacin significantly increases high-density lipoprotein cholesterol (HDL-C) more than any other available agent and reduces total cholesterol, low-density lipoprotein cholesterol (LDL-C), lipoprotein (a), and triglycerides. Niacin is currently available in immediate-release (IR), sustained-release (SR), and extended-release (ER) formulations that differ in their dissolution, pharmacokinetic, efficacy, and safety profiles. Important drawbacks to niacin therapy such as cutaneous flushing, associated with IR niacin, and hepatotoxicity, associated with SR niacin, have historically limited its use. The adverse effect profiles of the different niacin formulations can be explained by differences in their dissolution and absorption rates and metabolic disposition, which result in production of metabolites associated with the respective adverse effects. The ER niacin formulation, with an intermediate dissolution rate between the dissolution rates of IR and SR niacin, demonstrates reduced rates of cutaneous flushing compared with IR niacin and hepatotoxic effects compared with SR niacin. Pharmacists need to be familiar with the pharmacokinetics, efficacy, and safety of available niacin formulations so that they can optimally educate both patients and health care providers on the differences among niacin formulations, counsel on the proper selection of a niacin product, and provide strategies for improving tolerance and adherence to therapy.

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Year:  2003        PMID: 12901025     DOI: 10.1093/ajhp/60.suppl_2.S9

Source DB:  PubMed          Journal:  Am J Health Syst Pharm        ISSN: 1079-2082            Impact factor:   2.637


  15 in total

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2.  Treatment goals for the management of lipids and inflammation for patients with coronary artery disease.

Authors:  Rakesh K Mishra; Craig T Basson
Journal:  Curr Treat Options Cardiovasc Med       Date:  2007-02

Review 3.  Drug-Induced Hyperglycaemia and Diabetes.

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Journal:  Drug Saf       Date:  2015-12       Impact factor: 5.606

4.  Nicotinic acid inhibits hepatic APOA gene expression: studies in humans and in transgenic mice.

Authors:  Indumathi Chennamsetty; Karam M Kostner; Thierry Claudel; Manjula Vinod; Sasa Frank; Thomas S Weiss; Michael Trauner; Gerhard M Kostner
Journal:  J Lipid Res       Date:  2012-08-28       Impact factor: 5.922

5.  Synthesis and in vitro evaluation of potential sustained release prodrugs via targeting ASBT.

Authors:  Xiaowan Zheng; James E Polli
Journal:  Int J Pharm       Date:  2010-07-01       Impact factor: 5.875

Review 6.  Prolonged-release nicotinic acid: a review of its use in the treatment of dyslipidaemia.

Authors:  Paul L McCormack; Gillian M Keating
Journal:  Drugs       Date:  2005       Impact factor: 9.546

Review 7.  Lipid-lowering agents that cause drug-induced hepatotoxicity.

Authors:  Sidharth S Bhardwaj; Naga Chalasani
Journal:  Clin Liver Dis       Date:  2007-08       Impact factor: 6.126

Review 8.  Biological Properties of Vitamins of the B-Complex, Part 1: Vitamins B1, B2, B3, and B5.

Authors:  Marcel Hrubša; Tomáš Siatka; Iveta Nejmanová; Marie Vopršalová; Lenka Kujovská Krčmová; Kateřina Matoušová; Lenka Javorská; Kateřina Macáková; Laura Mercolini; Fernando Remião; Marek Máťuš; Přemysl Mladěnka
Journal:  Nutrients       Date:  2022-01-22       Impact factor: 5.717

Review 9.  Niacin as a drug repositioning candidate for hyperphosphatemia management in dialysis patients.

Authors:  Sooyoung Shin; Sukhyang Lee
Journal:  Ther Clin Risk Manag       Date:  2014-10-14       Impact factor: 2.423

Review 10.  Mechanisms of flushing due to niacin and abolition of these effects.

Authors:  Aditya Sood; Rohit Arora
Journal:  J Clin Hypertens (Greenwich)       Date:  2009-11       Impact factor: 3.738

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