Comparison of cefprozil and cefaclor pharmacokinetics and tissue penetration

Author:

Barbhaiya R H1,Shukla U A1,Gleason C R1,Shyu W C1,Wilber R B1,Pittman K A1

Affiliation:

1. Department of Metabolism and Pharmacokinetics, Bristol-Myers Squibb Company, Syracuse, New York 13221-4755.

Abstract

The pharmacokinetics and tissue penetration, as judged by skin blister fluid, of cefprozil and cefaclor were examined in 12 healthy male volunteers. Doses of 250 and 500 mg of each drug were given to fasting subjects in a crossover fashion. Serially obtained plasma, skin blister fluid, and urine samples were analyzed for cefprozil or cefaclor by validated high-pressure liquid chromatographic methods. After oral administration of 250 and 500 mg of cefprozil, mean concentrations in plasma rose to peak levels (Cmax) of 6.1 and 11.2 micrograms/ml, respectively, and those of cefaclor were 10.6 and 17.3 micrograms/ml, respectively. The elimination half-life of cefprozil (1.3 h) was significantly longer than that of cefaclor (0.6 h), and as a result, the area under the curve for cefprozil was about two times greater than that for cefaclor. Both cephalosporins were primarily excreted unchanged in urine. The mean skin blister Cmax values were 3.0 and 5.8 micrograms/ml for cefprozil and 3.6 and 6.5 micrograms/ml for cefaclor after the 250- and 500-mg oral doses, respectively. The mean Cmax values in skin blister fluid for both cephalosporins were comparable and were significantly lower than the corresponding Cmax values in plasma. However, the levels of cefprozil and cefaclor in skin blister fluid declined more slowly than they did in plasma. The skin blister fluid half-life estimates for cefprozil were significantly longer than they were for cefaclor. Parallel to the observation in plasma, the mean skin blister fluid areas under the curve for cefprozil were significantly higher than they were for cefaclor. The plasma and skin blister fluid pharmacokinetic analyses suggest that the exposure of humans to cefprozil is significantly greater than that to cefaclor at the same dose.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

Reference28 articles.

1. Phase I study of single-dose BMY-28100, a new oral cephalosporin;Barbhaiya R. H.;Antimicrob. Agents Chemother.,1990

2. Comparison of the effects of food on the pharmacokinetics of cefprozil and cefaclor;Barbhaiya R. H.;Antimicrob. Agents Chemother.,1990

3. Phase I study of multiple-dose cefprozil and comparison with cefaclor;Barbhaiya R. H.;Antimicrob. Agents Chemother.,1990

4. Cephalosporin associated pseudomembranous colitis due to Clostridium difficile;Bartlett J. G.;Am. J. Med. Assoc.,1979

5. Comparative antibacterial activity of a new oral cephalosporin, BMY-28100;Chin N.;Antimicrob. Agents Chemother.,1987

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