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A Comparison of Oral and Rectal Absorption of L-Dopa Esters in Rats and Mice
Authors:Fix  Joseph A.  Alexander  Jose  Cortese  Margot  Engle  Karen  Leppert  Paula  Repta  A. J.
Affiliation:(1) INTERx Research Corporation, Subsidiary of Merck & Co., Inc., Lawrence, Kansas, 66047
Abstract:Short-chain alkyl esters of L-dopa were administered to rats and mice via oral and rectal routes. Plasma L-dopa esters and L-dopa were determined in the systemic and portal circulation by HPLC. A comparison of isopropyl, butyl, and 4-hydroxybutyl esters of L-dopa demonstrated significantly higher levels of the esters in both systemic and portal blood samples following rectal administration than following oral administration. In most cases, oral administration resulted in nondetectable (<0.01 µg/ml) levels of the esters in plasma. Correspondingly, the plasma levels of L-dopa itself were consistently higher following rectal administration. At very high oral doses (500 mg L-dopa equivalents/kg body weight), systemic plasma levels of the butyl ester could be detected (1.25 µg/ml at 10 min), which might indicate saturation of the esterase activity of the small intestine. These studies indicate that the systemic availability of L-dopa from short-chain alkyl esters of L-dopa may be best optimized by rectal administration, which avoids the relatively high esterase activity characteristic of the small intestine.
Keywords:L-dopa esters  L-dopa  rectal  oral  bioavailability
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