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替莫西林在抗生素相关性结肠炎仓鼠模型中的研究。

Studies with temocillin in the hamster model of antibiotic-associated colitis.

作者信息

Boon R J, Beale A S

出版信息

Drugs. 1985;29 Suppl 5:57-63. doi: 10.2165/00003495-198500295-00012.

Abstract

The studies reported here were designed to ascertain whether or not the new beta-lactam antibiotic, temocillin, would produce antibiotic-associated colitis in the hamster. The experiments were controlled with clindamycin and cefoxitin, which are known to induce antibiotic-associated colitis experimentally and clinically. All three antibiotics were administered to groups of animals both parenterally and orally. Clindamycin, at 1 mg/hamster, caused a slow onset of antibiotic-associated colitis by both routes, with death occurring at between 4 and 8 days. 80 to 100% of the animals had diarrhoea and showed signs of haemorrhage and caecal distension, with the caecal contents being Clostridium difficile toxin-positive. The onset of antibiotic-associated colitis after administration of cefoxitin was less marked at the 1 mg parenteral dose, with only 40% of the hamsters showing signs of colitis. At the higher doses of cefoxitin, colitis was more severe and the animals exhibited dramatic weight loss, with death occurring at between 3 and 5 days. The majority of animals had diarrhoea and were C. difficile toxin-positive; 60 to 80% also showed signs of haemorrhage and caecal distension. In contrast, the hamsters receiving temocillin remained healthy with no signs of diarrhoea, and showed consistent weight gain. No pathological abnormalities were observed and the caecal contents were toxin-negative. These results suggest that temocillin therapy in humans is unlikely to cause significant disturbance of the gastrointestinal flora.

摘要

此处报告的研究旨在确定新型β-内酰胺类抗生素替莫西林是否会在仓鼠中引发抗生素相关性结肠炎。实验用克林霉素和头孢西丁作为对照,已知这两种药物在实验和临床中均可诱发抗生素相关性结肠炎。三种抗生素均通过肌肉注射和口服两种途径给药于动物组。1毫克/只仓鼠的克林霉素通过两种途径均导致抗生素相关性结肠炎发病缓慢,在4至8天内出现死亡。80%至100%的动物出现腹泻,并表现出出血和盲肠扩张迹象,盲肠内容物艰难梭菌毒素检测呈阳性。1毫克肌肉注射剂量的头孢西丁给药后,抗生素相关性结肠炎的发病情况不太明显,只有40%的仓鼠出现结肠炎迹象。在较高剂量的头孢西丁作用下,结肠炎更为严重,动物体重急剧下降,在3至5天内死亡。大多数动物出现腹泻,艰难梭菌毒素检测呈阳性;60%至80%的动物还表现出出血和盲肠扩张迹象。相比之下,接受替莫西林治疗的仓鼠保持健康,没有腹泻迹象,体重持续增加。未观察到病理异常,盲肠内容物毒素检测呈阴性。这些结果表明,替莫西林用于人类治疗不太可能对胃肠道菌群造成显著干扰。

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