The Efficiency of HMG-CoA-Reductase Inhibitors: Medicinal—Chemical Aspects of Statines.

## Abstract This study investigates a proposed design of a peptide sequence that is based on a bioactive conformation of statins that act as the competitive inhibitors of HMG–CoA for HMGR. To bridge these heterogeneous organic compounds, a conformational aspect relating to an analysis of the flexib

The absorption and disposition of fluvastatin have been studied in the female rabbit. In naive rabbits receiving a single oral dose (1 mg kg-I) of [3H]fluvastatin, absorption was rapid and amounted to c. 90 per cent compared with an intravenous reference dose. The drug was subject to considerable fi

The 4.9-kb segment of the Chinese hamster hydroxymethylglutaryl-CoA reductase promoter found in pRedCAT-3 consists of 1.4-kb of the promoter and a 3.5-kb intron. We placed this segment upstream of a reporter gene, lacZ of E. coli. The new construct pRed3lacZ was transfected into human hepatoma cells

SUMMARY Pyrrole-ring labeled \(\left[{ }^{14} \mathrm{C}\right]\) atorvastatin (Lipitor 8 , CI-981), [ \(\left.\mathrm{R}-\left(\mathrm{R}^{*}, \mathrm{R}^{*}\right)\right]-2-\) (4-fluorophenyl)- \(\beta, \gamma\)-dihydroxy-5-(1-methylethyl)-3-phenyl-4-[(phenylamino)carbonyl]-1H-[3- \(\left.{ }^{14}

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