Balfour J A, Todd P A, Peters D H
Adis International Limited, Auckland, New Zealand.
Drugs. 1995 May;49(5):794-850. doi: 10.2165/00003495-199549050-00010.
The fluoroquinolone antibacterial agent fleroxacin has a broad spectrum of in vitro activity which encompasses most Gram-negative species (particularly Enterobacteriaceae) and a number of Gram-positive organisms, including methicillin-sensitive staphylococci. It is available as oral and intravenous formulations. In clinical trials, fleroxacin has been evaluated in the treatment of uncomplicated urinary tract infections (single or multiple once-daily oral doses of 200 or 400mg), gonorrhoea and chancroid (single oral doses of 200 or 400mg), complicated urinary tract, nonpneumococcal lower respiratory tract and skin and soft tissue infections and typhoid fever (multiple once-daily oral or intravenous regimens, usually 400 mg/day), bacterial enteritis, and traveller's diarrhoea (single or multiple once-daily oral doses of 400mg). Bacteriological cure rates were generally around 90% or higher in complicated and uncomplicated urinary tract infections, uncomplicated gonorrhoea (approximately 100%), pyelonephritis, bacterial enteritis and typhoid fever, and exceeded 80% in lower respiratory tract, and skin and soft tissue infections and chancroid. These cure rates were similar to, or better than, those achieved with standard comparator antibacterial agents such as penicillins, cephalosporins, cotrimoxazole, or other quinolones. Fleroxacin 400mg once daily also achieved bacteriological cure in approximately 80% of patients with bone and joint infections in preliminary studies. In Japanese studies using a lower dosage of 200 or 300 mg/day, fleroxacin was reported to be bacteriologically effective in a range of infections, including urinary tract and upper and lower respiratory tract infections. Fleroxacin has a relatively long elimination half-life, which allows once-daily administration, and it appears to have less propensity for interactions with other medications in comparison to many other fluoroquinolones. Its tolerability profile is typical of this class of compound, with adverse events mostly relating to the gastrointestinal tract, CNS, and skin and appendages (including phototoxicity). Recent pooled tolerability data from worldwide clinical trials indicate that adverse events are reported by approximately 27% of patients receiving 200 mg/day orally or 400 mg/day orally or intravenously, and 17% of those receiving a single oral dose of 400mg. These exceed incidences reported for established fluoroquinolones, possibly indicating recent trends towards increased rates of reported adverse effects with these agents. However, in direct comparative studies with twice-daily fluoroquinolones, fleroxacin 400mg once daily produced a similar incidence of adverse effects to ofloxacin 800 mg/day and a slightly higher incidence than ciprofloxacin 1000 mg/day, while fleroxacin 200mg once daily produced a similar incidence to norfloxacin 800 mg/day.(ABSTRACT TRUNCATED AT 400 WORDS)
氟喹诺酮类抗菌药氟罗沙星具有广泛的体外活性,涵盖大多数革兰氏阴性菌(尤其是肠杆菌科细菌)以及许多革兰氏阳性菌,包括对甲氧西林敏感的葡萄球菌。它有口服和静脉制剂。在临床试验中,氟罗沙星已被评估用于治疗单纯性尿路感染(单次或多次每日口服200或400毫克)、淋病和软下疳(单次口服200或400毫克)、复杂性尿路感染、非肺炎球菌性下呼吸道感染、皮肤和软组织感染以及伤寒热(多次每日口服或静脉给药方案,通常为400毫克/天)、细菌性肠炎和旅行者腹泻(单次或多次每日口服400毫克)。在复杂性和单纯性尿路感染、单纯性淋病(约100%)、肾盂肾炎、细菌性肠炎和伤寒热中,细菌学治愈率一般在90%左右或更高,在下呼吸道感染、皮肤和软组织感染以及软下疳中超过80%。这些治愈率与使用标准对照抗菌药物如青霉素、头孢菌素、复方新诺明或其他喹诺酮类药物所达到的治愈率相似或更好。在初步研究中,每日一次400毫克的氟罗沙星也使约80%的骨和关节感染患者实现了细菌学治愈。在日本的研究中,使用较低剂量200或300毫克/天,据报道氟罗沙星在一系列感染中具有细菌学疗效,包括尿路感染以及上、下呼吸道感染。氟罗沙星的消除半衰期相对较长,这使得可以每日给药一次,并且与许多其他氟喹诺酮类药物相比,它与其他药物相互作用的可能性似乎较小。其耐受性特征是这类化合物的典型特征,不良事件大多与胃肠道、中枢神经系统以及皮肤和附属器(包括光毒性)有关。来自全球临床试验的最新汇总耐受性数据表明,接受每日口服200毫克或每日口服或静脉注射400毫克的患者中约27%报告了不良事件,而接受单次口服400毫克的患者中有17%报告了不良事件。这些发生率超过了已确立的氟喹诺酮类药物报告的发生率,可能表明这些药物报告的不良反应发生率有上升的近期趋势。然而,在与每日两次的氟喹诺酮类药物的直接对比研究中,每日一次400毫克的氟罗沙星产生的不良反应发生率与每日800毫克的氧氟沙星相似,比每日1000毫克的环丙沙星略高,而每日一次200毫克的氟罗沙星产生的不良反应发生率与每日800毫克的诺氟沙星相似。(摘要截选至400字)
