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[头孢唑肟栓在实验动物中的药代动力学]

[Pharmacokinetics of ceftizoxime suppository in experimental animals].

作者信息

Nishimura K, Nozaki Y, Yoshimi A, Nakamura S, Kitagawa M, Kitagawa M, Oketani T, Nishimura M, Kakeya N

出版信息

Jpn J Antibiot. 1985 Dec;38(12):3449-57.

PMID:3869264
Abstract

Ceftizoxime suppository (CZX-S) was administered rectally to mice, rats and dogs, and the pharmacokinetics were studied in comparison with those after intravenous, intramuscular and subcutaneous administration of ceftizoxime (CZX). Absorption of CZX given rectally was rapid in all animals, similar to intramuscular or subcutaneous administration. The peak serum levels of CZX in mice, rats and dogs when administered rectally at a dose of 25 mg/kg were 23.1 micrograms/ml at 7.5 minutes, 23.5 micrograms/ml at 15 minutes and 25.2 micrograms/ml at 15 minutes, respectively. These values were about 76%, 68% and 42% of the values for subcutaneous or intramuscular administration in mice, rats and dogs at the same respective doses. Urinary recoveries of CZX after rectal administration of 25 mg/kg were 44.2% (0-12 12 hours) in rats and 27.7% (0-6 hours) in dogs, and 2.7% (0-6 hours) of the dose was excreted into bile fluid in rats. Organ distribution of CZX when administered rectally to rats was similar in distribution pattern to that of muscular administration, although its concentrations in various organs were slightly lower than those for intramuscular administration, as was the case for serum concentration. Serum concentrations of CZX were proportionately elevated with dose when dogs were rectally administered CZX-S in doses of 12.5, 25 and 50 mg/kg. In the case of multiple administrations (t.i.d. for 10 days) of CZX-S to dogs, no remarkable difference was found in serum concentrations of CZX in comparison with single doses, and no accumulation of CZX was demonstrated.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

将头孢唑肟栓剂(CZX - S)经直肠给予小鼠、大鼠和犬,并与静脉注射、肌肉注射和皮下注射头孢唑肟(CZX)后的药代动力学进行比较研究。直肠给予CZX在所有动物中吸收迅速,类似于肌肉注射或皮下注射。当以25mg/kg剂量经直肠给予小鼠、大鼠和犬时,CZX的血清峰值水平分别在7.5分钟时为23.1μg/ml、15分钟时为23.5μg/ml和15分钟时为25.2μg/ml。这些值分别约为相同剂量下小鼠、大鼠和犬皮下或肌肉注射值的76%、68%和42%。经直肠给予25mg/kg剂量后,大鼠CZX的尿回收率为44.2%(0 - 12小时),犬为27.7%(0 - 6小时),大鼠胆汁中排出剂量的2.7%(0 - 6小时)。经直肠给予大鼠CZX时,其在各器官中的分布模式与肌肉注射相似,尽管各器官中的浓度略低于肌肉注射,血清浓度情况也是如此。当以12.5、25和50mg/kg剂量经直肠给予犬CZX - S时,CZX的血清浓度随剂量成比例升高。在犬多次给予CZX - S(每日3次,共10天)的情况下,与单次给药相比,CZX的血清浓度未发现显著差异,且未显示CZX有蓄积。(摘要截短于250字)

相似文献

1
[Pharmacokinetics of ceftizoxime suppository in experimental animals].[头孢唑肟栓在实验动物中的药代动力学]
Jpn J Antibiot. 1985 Dec;38(12):3449-57.
2
[Fundamental study on ceftizoxime suppositories in adults and children].[成人及儿童用头孢唑肟栓剂的基础研究]
Jpn J Antibiot. 1985 Oct;38(10):3013-56.
3
[Effects of ceftizoxime suppository rectal dosing on cecal microflora in mice].[头孢唑肟栓直肠给药对小鼠盲肠微生物区系的影响]
Jpn J Antibiot. 1986 Jan;39(1):94-8.
4
[Clinical study of ceftizoxime suppositories in acute suppurative otitis media in children and tissue concentration of ceftizoxime in the palatine tonsil after administration of ceftizoxime suppositories].头孢唑肟栓治疗小儿急性化脓性中耳炎的临床研究及给药后腭扁桃体中头孢唑肟的组织浓度
Jpn J Antibiot. 1985 Oct;38(10):3070-6.
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[Study on tissue transfer of ceftizoxime suppository in the field of obstetrics and gynecology].[头孢唑肟栓在妇产科领域的组织转移研究]
Jpn J Antibiot. 1986 Jun;39(6):1504-8.
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[Fundamental and clinical studies of ceftizoxime rectal suppositories in the field of pediatrics].头孢唑肟直肠栓剂在儿科领域的基础与临床研究
Jpn J Antibiot. 1985 Oct;38(10):2863-76.
7
[Fundamental and clinical studies of ceftizoxime suppositories in the pediatric field].头孢唑肟栓剂在儿科领域的基础与临床研究
Jpn J Antibiot. 1985 Oct;38(10):2877-88.
8
[Fundamental and clinical studies on ceftizoxime suppositories in children].小儿头孢唑肟栓的基础与临床研究
Jpn J Antibiot. 1985 Oct;38(10):2977-3012.
9
[Clinical and pharmacokinetic evaluations of ceftizoxime suppositories in children].头孢唑肟栓在儿童中的临床及药代动力学评价
Jpn J Antibiot. 1985 Oct;38(10):2838-48.
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[Clinical studies of ceftizoxime suppositories in respiratory tract infections and urinary tract infections in children].头孢唑肟栓用于儿童呼吸道感染和尿路感染的临床研究
Jpn J Antibiot. 1985 Oct;38(10):2903-16.