Literature DB >> 1489192

Comparative pharmacokinetics of SCE-2787 and related antibiotics in experimental animals.

Y Kita1, T Yamazaki, A Imada.   

Abstract

The pharmacokinetic properties of SCE-2787 administered intravenously at a dose of 20 mg/kg of body weight were studied with mice, rats, rabbits, dogs, and monkeys and were compared with those of ceftazidime, cefpirome, and cefclidin in mice and dogs. The area under the concentration-time curve for plasma after intravenous administration was the largest in monkeys, followed by those in dogs, rabbits, rats, and mice, in that order. The elimination half-life ranged from 0.2 to 0.3 h in mice and rats to 0.7 to 1.3 h in rabbits, dogs, and monkeys. In young dogs, the concentrations of SCE-2787 in plasma were somewhat lower than those in the mature dogs. SCE-2787 was distributed well to the tissues, and the highest concentration was found in the kidneys in all species tested; the distribution to the lungs, liver, and spleen was also good, but the concentrations in these tissues were lower than those in the plasma. The pharmacokinetic parameters and urinary excretion of SCE-2787 in mice and dogs were similar to those of ceftazidime, cefpirome, and cefclidin. The maximum concentrations in the cerebrospinal fluid of rats and rabbits were 0.8 and 1.3 micrograms/ml, and the relative percentages of the area under the concentration-time curve of SCE-2787 in the cerebrospinal fluid to that in the plasma were 4.6 and 6.4%, respectively. SCE-2787 was excreted mainly in the urine; the recovery rate ranged from 74% (rats) to 90% (dogs) of the dose. The biliary excretion of SCE-2787, however, was low, amounting to about 1.4% for mice and rats and less than 0.5% for rabbits and dogs. In rats, there was no accumulation in the tissues and no delay in urinary excretion upon multiple intravenous administration of 20 mg of SCE-2787 per kg once daily for 7 days. No active metabolites were found in the plasma or urine of animals given SCE-2787. The binding of SCE-2787 to serum protein in mice, rats, dogs, monkeys, and humans was less than 11% and similar to that of cefclidin.

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Year:  1992        PMID: 1489192      PMCID: PMC284358          DOI: 10.1128/AAC.36.11.2481

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  7 in total

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Authors:  R Wise
Journal:  J Antimicrob Chemother       Date:  1983-07       Impact factor: 5.790

2.  Effect of extracellular water volume on the distribution kinetics of beta-lactam antibiotics as a function of age.

Authors:  A Tsuji; T Terasaki; N Imaeda; K Nishide; E Nakashima
Journal:  J Pharmacobiodyn       Date:  1985-03

3.  A pharmacokinetic analysis program (multi) for microcomputer.

Authors:  K Yamaoka; Y Tanigawara; T Nakagawa; T Uno
Journal:  J Pharmacobiodyn       Date:  1981-11

Review 4.  Clincial pharmacokinetics in neonates.

Authors:  P L Morselli
Journal:  Clin Pharmacokinet       Date:  1976       Impact factor: 6.447

5.  Antibacterial properties of SCE-2787, a new cephem antibiotic.

Authors:  M Nakao; Y Noji; T Iwahi; T Yamazaki
Journal:  J Antimicrob Chemother       Date:  1992-05       Impact factor: 5.790

6.  Ultrafiltrable calcium and magnesium in ultrafiltrates of serum prepared with the Amicon MPS-1 system.

Authors:  M D'Costa; P T Cheng
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7.  In vitro and in vivo activities of SCE-2787, a new parenteral cephalosporin with a broad antibacterial spectrum.

Authors:  T Iwahi; K Okonogi; T Yamazaki; S Shiki; M Kondo; A Miyake; A Imada
Journal:  Antimicrob Agents Chemother       Date:  1992-07       Impact factor: 5.191

  7 in total
  8 in total

1.  Pharmacokinetics and penetration of ceftazidime and avibactam into epithelial lining fluid in thigh- and lung-infected mice.

Authors:  Johanna Berkhout; Maria J Melchers; Anita C van Mil; Seyedmojtaba Seyedmousavi; Claudia M Lagarde; Wright W Nichols; Johan W Mouton
Journal:  Antimicrob Agents Chemother       Date:  2015-02-02       Impact factor: 5.191

2.  In vitro and in vivo antifungal activities of TAK-456, a novel oral triazole with a broad antifungal spectrum.

Authors:  Noboru Tsuchimori; Ryogo Hayashi; Naomi Kitamoto; Kentaro Asai; Tomoyuki Kitazaki; Yuji Iizawa; Katsumi Itoh; Kenji Okonogi
Journal:  Antimicrob Agents Chemother       Date:  2002-05       Impact factor: 5.191

3.  Disposition kinetics and urinary excretion of cefpirome after intravenous injection in buffalo calves.

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4.  Therapeutic effect of cefozopran (SCE-2787), a new parenteral cephalosporin, against experimental infections in mice.

Authors:  Y Iizawa; K Okonogi; R Hayashi; T Iwahi; T Yamazaki; A Imada
Journal:  Antimicrob Agents Chemother       Date:  1993-01       Impact factor: 5.191

5.  Enterococcus faecalis aggravates pyelonephritis caused by Pseudomonas aeruginosa in experimental ascending mixed urinary tract infection in mice.

Authors:  N Tsuchimori; R Hayashi; A Shino; T Yamazaki; K Okonogi
Journal:  Infect Immun       Date:  1994-10       Impact factor: 3.441

6.  Broad-spectrum β-lactam antibiotics for treating experimental peritonitis in mice due to Klebsiella pneumoniae producing the carbapenemase OXA-48.

Authors:  Olivier Mimoz; Nicolas Grégoire; Laurent Poirel; Manuella Marliat; William Couet; Patrice Nordmann
Journal:  Antimicrob Agents Chemother       Date:  2012-02-13       Impact factor: 5.191

7.  Modelling concentrations of antimicrobial drugs: comparative pharmacokinetics of cephalosporin antimicrobials and accuracy of allometric scaling in food-producing and companion animals.

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Review 8.  Protein Binding in Translational Antimicrobial Development-Focus on Interspecies Differences.

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  8 in total

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