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β-内酰胺前药对人体肠道微生物群的影响。

Effect of beta-lactam prodrugs on human intestinal microflora.

作者信息

Sjövall J, Huitfeldt B, Magni L, Nord C E

出版信息

Scand J Infect Dis Suppl. 1986;49:73-84.

PMID:3547627
Abstract

The ampicillin prodrugs bacampicillin, pivampicillin, and talampicillin, the mecillinam prodrug pivmecillinam and the sulbactam prodrug sulbactam pivoxil all have a greatly improved oral availability compared to the parent drug. They show no antibacterial activity themselves until transformed into active drugs after absorption. This double advantage makes them less likely to influence the intestinal microbial ecosystem. Ampicillin has been reported to cause marked changes in the colon microflora, particularly as regards Enterobacter species, Klebsiella species, enterococci, lactobacilli, bacteroides, and clostridia, in contrast to pivampicillin, which did not exert much influence. Similarly, talampicillin has been reported to have less influence than ampicillin on the colon flora. Diarrhoea was more common after ampicillin and was accompanied by an overgrowth of Candida. Pivmecillinam has been reported to reduce the number of Escherichia coli and lactobacilli. No changes were seen in the colon flora of subjects receiving bacampicillin tablets. This was verified in a parallel group study, in which one group was given the combination of bacampicillin and sulbactam pivoxil, the other bacampicillin, for seven days. Of the subjects given the combination, five had a moderate and ten a considerable change in their colon microflora. The subjects were often heavily colonized by new aerobic strains such as enterococci, E. coli, Bacillus, Enterobacter, Aeromonas, and yeasts. Among the anaerobes, Veillonella, the bifidobacteria-lactobacillus group, and bacteroides decreased. Some strains of clostridia decreased but there was also a colonization with new strains. One subject was colonized with Clostridium difficile. Diarrhoea was seen only during the week of active drug administration in the group given the combination. The symptoms generally appeared on the second or third day of treatment and had, in most cases, subsided at the end of treatment. The results illustrate the correlation between disturbances in the intestinal microbial ecosystem and intestinal adverse reactions.

摘要

氨苄西林前体药物巴氨西林、匹氨西林和酞氨西林、美西林前体药物匹美西林以及舒巴坦前体药物舒巴坦匹酯与母体药物相比,口服生物利用度均有显著提高。它们自身没有抗菌活性,直到吸收后转化为活性药物才显示出抗菌活性。这一双重优势使得它们对肠道微生物生态系统的影响较小。据报道,氨苄西林会引起结肠微生物群落的显著变化,尤其是肠杆菌属、克雷伯菌属、肠球菌、乳酸菌、拟杆菌和梭菌属方面,相比之下,匹氨西林的影响较小。同样,据报道酞氨西林对结肠菌群的影响比氨苄西林小。氨苄西林治疗后腹泻更为常见,且伴有念珠菌过度生长。据报道,匹美西林可减少大肠杆菌和乳酸菌的数量。接受巴氨西林片治疗的受试者结肠菌群未见变化。这在一项平行组研究中得到了验证,其中一组给予巴氨西林和舒巴坦匹酯的组合,另一组给予巴氨西林,为期7天。在接受联合用药的受试者中,5人结肠微生物群落有中度变化,10人有显著变化。受试者常被新的需氧菌株如肠球菌、大肠杆菌、芽孢杆菌、肠杆菌、气单胞菌和酵母菌大量定植。在厌氧菌中,韦荣球菌、双歧杆菌 - 乳酸菌组和拟杆菌减少。一些梭菌菌株减少,但也有新菌株定植。一名受试者被艰难梭菌定植。仅在接受联合用药组的活性药物给药周期间出现腹泻。症状通常在治疗的第二天或第三天出现,大多数情况下在治疗结束时消退。结果说明了肠道微生物生态系统紊乱与肠道不良反应之间的相关性。

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