| Literature DB >> 7458980 |
M Kibata, M Ishida, K Asano, H Uehara, K Saito, T Fuchimoto, K Ugaki, H Murakami, K Matoba, Y Kotakemori, K Shirai, H Yoshioka, M Nanba, M Yasuda, M Ishizaki, N Kitagawa, K Ikejiri, R Inohara, B J Lee, S Saino, J Sakado, H Matuzaka, K Numata, M Mandai, K Miyake, K Nakamura.
Abstract
The effects of niceritrol, a nicotinic acid derivative, on the levels of HDL-cholesterol (HDL-Ch) and a mixture of VLDL- and LDL-Ch (VLDL- + LDL-Ch) were studied in hyperlipidemic patients. Serum total cholesterol (sTC) and serum triglyceride (sTG) were significantly reduced during niceritrol administration. Lipoprotein electrophoresis showed that niceritrol increased the alpha:beta ratio. HDL-Ch showed a significant increase of 12.5% by the 16th week of therapy. This increase was more marked in patients with lower pre-treatment HDL-Ch levels and significant in patients whose pre-treatment sTG levels were in excess of 200 mg/dl. Females displayed higher pre-treatment HDL-Ch levels (38.5 mg/dl) than males (30.6 mg/dl). However, niceritrol increased HDL-Ch significantly in both groups. At 16 weeks, the VLDL- + LDL-Ch level showed a significant decrease of 9.2%; the HDL-Ch:VLDL + LDL-Ch and HDL-CH:sTC ratios were significantly increased throughout niceritrol administration. Niceritrol is thought to be effective in preventing the development and progression of atherosclerosis because it raises the level of anti-atherogenic HDL-Ch and lowers the level of atherogenic VLDL- + LDL-Ch.Entities:
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Year: 1980 PMID: 7458980 DOI: 10.1016/0021-9150(80)90137-9
Source DB: PubMed Journal: Atherosclerosis ISSN: 0021-9150 Impact factor: 5.162