Efficacy and Safety of Controlled-Release Niacin in Dyslipoproteinemic Veterans

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	Gray, D. R.

	Kashyap, M. L.

ARTICLE

Efficacy and Safety of Controlled-Release Niacin in Dyslipoproteinemic Veterans

David R. Gray; Timothy Morgan; Steven D. Chretien; and Moti L. Kashyap

15 August 1994 | Volume 121 Issue 4 | Pages 252-258

Objective: To evaluate the safety and efficacy of controlled-releaseniacin in patients with hyperlipoproteinemia.

Design: A retrospective cohort study.

Setting: A Department of Veterans Affairs Medical Center.

Patients: A consecutive sample of 969 predominantly elderlymale veterans treated for dyslipoproteinemia with controlled-releaseniacin between October 1988 and October 1991.

Main Outcome Measures: Primary outcomes were lipid levels andlipoprotein cholesterol response, alterations in levels of hepaticenzymes and blood chemistry test results, and characterizationof niacin-induced hepatotoxicity abstracted from the patient'smedical, laboratory, and pharmacy records.

Results: 93% (896 of 969) of the cohort was evaluable. Patients(age, 61.7 years [9.4 years], mean [SD]) were treated for 1to 36 months (13.0 months [9.7 months]) with an average maintenancedose of 1.67 g/d (0.8 g/d). Niacin was discontinued in 48.5%(435 of 896) of the patients primarily because of adverse effects.Poor glycemic control led to discontinuation in 40.6% (43 of106) of the patients with diabetes mellitus. The lipoproteinresponse was dose-related and favorable (levels of total cholesterol,–19.1%;low-density lipoprotein cholesterol, –24.0%;high-densitylipoprotein cholesterol, +5.7%; and triglycerides, –32.5%).Statisticallybut not clinically meaningful dose-related increases were seenin levels of liver enzymes and serum glucose (aspartate aminotransferase,+29%; alanine aminotransferase, +23%; alkaline phosphatase,+25%; and glucose, +7%; P = 0.0001). Twenty of 896 (2.2%) and42 of 896 (4.7%) patients met biochemical criteria for probableand for possible or probable niacin-induced hepatotoxicity,respectively. Predisposing factors included high dose, alcoholuse, preexisting liver disease, and concurrent oral sulfonylureatherapy.

Conclusions: Controlled-release niacin is effective in treatingdyslipoproteinemia in selected middle-aged and elderly veterans,but approximately one half of patients discontinued the drugbecause of adverse effects or other causes including noncompliance.Niacin should be avoided in patients with hepatic dysfunctionor a history of liver disease, patients with diabetes mellitus,and patients who abuse alcohol. Because controlled-release niacinseems to be more potent than crystalline niacin, product substitutionwithout dose adjustment should be avoided.

Author and Article Information

From the Long Beach Veterans Affairs Medical Center and the University of California, Irvine, California.
Requests for Reprints: David R. Gray, PharmD, Veterans Affairs Medical Center RF 119, 5901 East Seventh Street, Long Beach, CA 90822.
Acknowledgments: The authors thank Kim Seto, BS, and Katie Paik, BS, for their assistance in data collection.
Grant Support: In part by a grant from Upsher-Smith Laboratories.

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IS CONTROLLED-RELEASE NIACIN SAFE?
Journal Watch (General), August 19, 1994; 1994(819): 2 - 2.
[Full Text]

				T. Sakai, V. S. Kamanna, and M. L. Kashyap Niacin, but Not Gemfibrozil, Selectively Increases LP-AI, a Cardioprotective Subfraction of HDL, in Patients With Low HDL Cholesterol Arterioscler. Thromb. Vasc. Biol., November 1, 2001; 21(11): 1783 - 1789. [Abstract] [Full Text] [PDF]

				M. B. Elam, D. B. Hunninghake, K. B. Davis, R. Garg, C. Johnson, D. Egan, J. B. Kostis, D. S. Sheps, E. A. Brinton, and for the ADMIT Investigators Effect of Niacin on Lipid and Lipoprotein Levels and Glycemic Control in Patients With Diabetes and Peripheral Arterial Disease: The ADMIT Study: A Randomized Trial JAMA, September 13, 2000; 284(10): 1263 - 1270. [Abstract] [Full Text] [PDF]

				J. R. Guyton, M. A. Blazing, J. Hagar, M. L. Kashyap, R. H. Knopp, J. M. McKenney, D. T. Nash, S. D. Nash, and for the Niaspan-Gemfibrozil Study Group Extended-Release Niacin vs Gemfibrozil for the Treatment of Low Levels of High-Density Lipoprotein Cholesterol Arch Intern Med, April 24, 2000; 160(8): 1177 - 1184. [Abstract] [Full Text] [PDF]

				F.-Y. Jin, V. S. Kamanna, and M. L. Kashyap Niacin Accelerates Intracellular ApoB Degradation by Inhibiting Triacylglycerol Synthesis in Human Hepatoblastoma (HepG2) Cells Arterioscler. Thromb. Vasc. Biol., April 1, 1999; 19(4): 1051 - 1059. [Abstract] [Full Text] [PDF]

				IS CONTROLLED-RELEASE NIACIN SAFE? Journal Watch (General), August 19, 1994; 1994(819): 2 - 2. [Full Text]