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细菌性败血症:诊断与计算得出的抗生素治疗方案

Bacterial sepsis : Diagnostics and calculated antibiotic therapy.

作者信息

Richter D C, Heininger A, Brenner T, Hochreiter M, Bernhard M, Briegel J, Dubler S, Grabein B, Hecker A, Kruger W A, Mayer K, Pletz M W, Storzinger D, Pinder N, Hoppe-Tichy T, Weiterer S, Zimmermann S, Brinkmann A, Weigand M A, Lichtenstern C

机构信息

Department of Anesthesiology, Heidelberg University Hospital, Im Neuenheimer Feld 110, 69120, Heidelberg, Germany.

Zentrum für Infektiologie, Sektion für Krankenhaus- und Umwelthygiene, Universitätsklinikum Heidelberg, Heidelberg, Germany.

出版信息

Anaesthesist. 2019 Feb;68(Suppl 1):40-62. doi: 10.1007/s00101-017-0396-z.

Abstract

The mortality of patients with sepsis and septic shock is still unacceptably high. An effective calculated antibiotic treatment within 1 h of recognition of sepsis is an important target of sepsis treatment. Delays lead to an increase in mortality; therefore, structured treatment concepts form a rational foundation, taking relevant diagnostic and treatment steps into consideration. In addition to the assumed infection and individual risks of each patient, local resistance patterns and specific problem pathogens must be taken into account during the selection of anti-infective treatment. Many pathophysiologic alterations influence the pharmacokinetics (PK) of antibiotics during sepsis. The principle of standard dosing should be abandoned and replaced by an individual treatment approach with stronger weighting of the pharmacokinetics/pharmacodynamics (PK/PD) index of the substance groups. Although this is not yet the clinical standard, prolonged (or continuous) infusion of β‑lactam antibiotics and therapeutic drug monitoring (TDM) can help to achieve defined PK targets. Prolonged infusion is sufficient without TDM, but for continuous infusion, TDM is generally necessary. A further argument for individual PK/PD-oriented antibiotic approaches is the increasing number of infections due to multidrug-resistant (MDR) pathogens in the intensive care unit. For effective treatment, antibiotic stewardship teams (ABS teams) are becoming more established. Interdisciplinary cooperation of the ABS team with infectious disease (ID) specialists, microbiologists, and clinical pharmacists leads not only to rational administration of antibiotics, but also has a positive influence on treatment outcome. The gold standards for pathogen identification are still culture-based detection and microbiologic resistance testing for the various antibiotic groups. Despite the rapid investigation time, novel polymerase chain reaction(PCR)-based procedures for pathogen identification and resistance determination are currently only an adjunct to routine sepsis diagnostics, due to the limited number of studies, high costs, and limited availability. In complicated septic courses with multiple anti-infective therapies or recurrent sepsis, PCR-based procedures can be used in addition to treatment monitoring and diagnostics. Novel antibiotics represent potent alternatives in the treatment of MDR infections. Due to the often defined spectrum of pathogens and the practically (still) absent resistance, they are suitable for targeted treatment of severe MDR infections (therapy escalation). (Contribution available free of charge by "Free Access" [ https://link.springer.com/article/10.1007/s00101-017-0396-z ].).

摘要

脓毒症和脓毒性休克患者的死亡率仍然高得令人难以接受。在识别脓毒症后1小时内进行有效的精准抗生素治疗是脓毒症治疗的一个重要目标。治疗延迟会导致死亡率上升;因此,结构化治疗理念形成了一个合理的基础,其中考虑了相关的诊断和治疗步骤。在选择抗感染治疗时,除了假定的感染和每个患者的个体风险外,还必须考虑当地的耐药模式和特定的问题病原体。脓毒症期间,许多病理生理改变会影响抗生素的药代动力学(PK)。应摒弃标准给药原则,代之以根据药物组的药代动力学/药效学(PK/PD)指标进行更强加权的个体化治疗方法。虽然这尚未成为临床标准,但延长(或持续)输注β-内酰胺类抗生素和治疗药物监测(TDM)有助于实现既定的PK目标。延长输注在没有TDM的情况下就足够了,但对于持续输注,TDM通常是必要的。以PK/PD为导向的个体化抗生素治疗方法的另一个理由是重症监护病房中耐多药(MDR)病原体导致的感染越来越多。为了进行有效治疗,抗生素管理团队(ABS团队)越来越成熟。ABS团队与传染病(ID)专家、微生物学家和临床药师的跨学科合作不仅能实现抗生素的合理使用,而且对治疗结果也有积极影响。病原体鉴定的金标准仍然是基于培养物的检测以及针对各种抗生素组的微生物耐药性检测。尽管检测时间较快,但由于研究数量有限、成本高以及可及性有限,目前基于新型聚合酶链反应(PCR)的病原体鉴定和耐药性测定程序仅是常规脓毒症诊断的辅助手段。在复杂的脓毒症病程中,如采用多种抗感染治疗或脓毒症复发时,除了治疗监测和诊断外,还可使用基于PCR的程序。新型抗生素是治疗MDR感染的有效替代药物。由于其病原体谱通常明确且实际上(目前)不存在耐药性,它们适用于严重MDR感染的靶向治疗(治疗升级)。(本文可通过“免费获取”[https://link.springer.com/article/10.1007/s00101-017-0396-z]免费获取。)

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