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Citations to this article

The novel compound NO-1886 increases lipoprotein lipase activity with resulting elevation of high density lipoprotein cholesterol, and long-term administration inhibits atherogenesis in the coronary arteries of rats with experimental atherosclerosis.
K Tsutsumi, … , M Kawamura, T Murase
K Tsutsumi, … , M Kawamura, T Murase
Published July 1, 1993
Citation Information: J Clin Invest. 1993;92(1):411-417. https://doi.org/10.1172/JCI116582.
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The novel compound NO-1886 increases lipoprotein lipase activity with resulting elevation of high density lipoprotein cholesterol, and long-term administration inhibits atherogenesis in the coronary arteries of rats with experimental atherosclerosis.

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Abstract

We have discovered a novel compound, NO-1886, which possesses a powerful lipoprotein lipase (LPL) activity-increasing action. Administration of NO-1886 increased LPL activity in the postheparin plasma, adipose tissue, and myocardium of rats, and produced a reduction in plasma triglyceride levels with concomitant elevation of HDL cholesterol levels. Administration of NO-1886 increased LPL enzyme mass in postheparin plasma and mRNA activity in epididymal adipose tissue, and it was concluded that the mode of action of this compound is stimulation of tissue LPL synthesis. We also conducted long-term studies to assess the impact of increases in LPL activity and HDL levels on the development of atherosclerotic lesions in rats. Administration of NO-1886 for as long as 90 d significantly decreased the degree of atherosclerotic changes in the coronary arteries of vitamin D2-treated, cholesterol-fed rats. Statistical analysis indicated that increased concentration of HDL is the factor contributing mostly to the prevention of coronary artery sclerosis. In summary, the results of our study indicate that compound NO-1886 increases LPL activity, causing an elevation in HDL levels, and that long-term administration of NO-1886 to rats with experimental atherosclerosis provides significant protection against the development of coronary artery lesions.

Authors

K Tsutsumi, Y Inoue, A Shima, K Iwasaki, M Kawamura, T Murase

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High expression of a novel carnitine palmitoyltransferase I like protein in rat brown adipose tissue and heart: isolation and characterization of its cDNA clone
N Yamazaki, Y Shinohara, A Shima, H Terada
FEBS Letters 1995
Steady state transcript levels of the type II hexokinase and type 1 glucose transporter in human tumor cell lines
Y Shinohara, K Yamamoto, K Kogure, J Ichihara, H Terada
Cancer Letters 1994
Oxidative-modified and acetylated low-density lipoproteins differ in their effects on cholesterol synthesis and stimulate synthesis of apolipoprotein E in rat peritoneal macrophages by different mechanisms
MY Zhang, RC Lin
Metabolism 1994
Normal differentiation of rat brown adipocytes in primary culture judged by their expressions of uncoupling protein and the physiological isoform of glucose transporter
A Shima, Y Shinohara, K Doi, H Terada
Biochimica et Biophysica Acta (BBA) - Molecular Cell Research 1994
Alteration of lipid profiles in plasma of transgenic mice expressing human lipoprotein lipase
MS Liu, FR Jirik, RC LeBoeuf, H Henderson, LW Castellani, AJ Lusis, Y Ma, IJ Forsythe, H Zhang, E Kirk
The Journal of biological chemistry 1994

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Referenced in 8 patents
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