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Once daily high dose tigecycline - pharmacokinetic/pharmacodynamic based dosing for optimal clinical effectiveness: dosing matters, revisited

机译:每日高剂量替代霉素 - 药代动力学/药效学基于最佳临床效果的剂量:给药物,重新审视

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Introduction: Tigecycline has emerged as first line therapy for serious systemic infections due to important pathogens (except P. aeruginosa and Proteus sp.), including multi-drug resistant (MDR) and Gram negative bacilli (GNB), including carbapenem resistant Enterobacteriae. Tigecycline has a low resistance potential,' is protective against C. difficile, and is often the only antibiotic effective against MDR GNB, e.g., Klebsiella sp.Areas covered: Standard dose tigecycline therapy has been used for intra-abdominal infections, complicated skin/skin structure infections (cSSSIs), and CAP. Clinical experience with once daily high dose tigecycline (HDT), i.e., 200 - 400mg (IV) x 1, then 100 - 200mg (IV) q24h, is reviewed. Optimal tigecycline efficacy is dependent on PK/PD based dosing. Suboptimal outcomes have been due to inappropriate use or suboptimal dosing.Expert commentary: Tigecycline's spectrum against nearly all important pathogens (including MSSA/MRSA, VSE/VRE, B. fragilis, C. difficile, MDR and GNB) assures tigecycline a critical place in the antibiotic armamentarium. Dosed optimally, HDT can be a cornerstone of antibiotic stewardship programs in preventing C. difficile, treating MDR GNB pathogens, and in preventing resistance. Properly used and optimally dosed, once daily HDT should be considered preferred therapy for severe systemic infections and those due to MDR GNB pathogens.
机译:介绍:由于重要病原体(P. eruginosa和Proteus SP除外),Tigeccline已成为严重的全身感染的第一线疗法,包括多药物抗药性(MDR)和革兰氏阴性杆菌(GNB),包括CarbapeNem耐肠细菌。替霉素具有低电阻潜力,对C.艰难源性是保护性的,并且往往是对MDR GNB的唯一抗生素有效,例如Klebsiella Sp.Areas覆盖:标准剂量Tigeccline疗法已被用于腹内感染,复杂的皮肤复杂/皮肤结构感染(CSSSIS)和帽。综述临床经验,每日高剂量替身素(HDT),即200 - 400mg(iv)x 1,那么100-200mg(iv)Q24h。最佳的替代素疗效取决于PK / Pd基给料。由于不适当的使用或次优剂量的次优的结果是由于评论不适当的评论抗生素的arminalium。最佳地给药,HDT可以是防止C.艰难梭菌,治疗MDR GNB病原体以及预防抗性的抗生素管道方案的基石。适当使用和最佳地给药,每日HDT一次应被认为是优选的治疗,用于严重的全身感染和由于MDR GNB病原体的患者。

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