Sitar D S, Hoban D J, Aoki F Y
Department of Internal Medicine, University of Manitoba and Health Sciences Centre, Winnipeg.
J Clin Pharmacol. 1994 Sep;34(9):924-9. doi: 10.1002/j.1552-4604.1994.tb04006.x.
The pharmacokinetic disposition of 200- and 400-mg doses of a novel carbacephem, loracarbef, was determined over a dose interval on day 8, after ingestion of drug doses twice daily for 7 days, in 20 young, healthy volunteers of both genders. Drug was analyzed in plasma, urine, saliva, vaginal secretions, and fecal filtrate. Peak plasma concentration was proportional to dose for both men (4.0 +/- 1.3 and 8.8 +/- 3.4 mg/L) and women (8.0 +/- 5.6 and 15.3 +/- 3.3 mg/L), and the observed time to peak increased from 1 to 2 hours with the increased dose. Apparent volume of distribution was greater in men than women (0.385 +/- 0.114 versus 0.270 +/- 0.075 L/kg; P < .03). The drug was virtually quantitatively excreted unchanged in urine, and its renal clearance exceeded creatinine clearance in all subjects. Renal loracarbef clearance correlated with neither weight-corrected dose nor creatinine clearance in these healthy subjects. There was no evidence for drug accumulation in the body with chronic ingestion. Loracarbef was detected in the fecal filtrate of seven volunteers, but did not account for more than 7% of the daily dose. Loracarbef was detected in vaginal secretions of two of five volunteers who ingested the 400-mg dose. No drug was detected in saliva obtained just before dose ingestion. These data are consistent with complete bioavailability for an oral beta-lactam antibiotic drug that is virtually completely eliminated unchanged by the kidney.
在20名年轻健康的男女志愿者中,连续7天每天两次服用新型碳头孢烯类药物氯碳头孢,剂量分别为200毫克和400毫克,在第8天的一个给药间隔内测定其药代动力学特征。对血浆、尿液、唾液、阴道分泌物和粪便滤液进行药物分析。男性(4.0±1.3和8.8±3.4毫克/升)和女性(8.0±5.6和15.3±3.3毫克/升)的血浆峰浓度均与剂量成正比,且随着剂量增加,达到峰浓度的时间从1小时增加到2小时。男性的表观分布容积大于女性(0.385±0.114对0.270±0.075升/千克;P<0.03)。该药物几乎定量地以原形经尿液排泄,在所有受试者中其肾清除率超过肌酐清除率。在这些健康受试者中,氯碳头孢的肾清除率与体重校正剂量和肌酐清除率均无相关性。没有证据表明长期摄入该药物会在体内蓄积。在7名志愿者的粪便滤液中检测到氯碳头孢,但不超过每日剂量的7%。在服用400毫克剂量的5名志愿者中的2名的阴道分泌物中检测到氯碳头孢。在给药前采集的唾液中未检测到药物。这些数据与一种口服β-内酰胺类抗生素药物的完全生物利用度一致,该药物几乎完全以原形经肾脏消除。
