关节内使用抗生素和消毒冲洗及其与软骨溶解的系统性关联的综述。

Kansas journal of medicine Pub Date : 2023-10-30 eCollection Date: 2023-01-01 DOI:10.17161/kjm.vol16.20357
Hunter K Post, Michael G Blankespoor, Victoria K Ierulli, Tucker D Morey, J Paul Schroeppel, Mary K Mulcahey, Bryan G Vopat, Matthew L Vopat
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引用次数: 0

摘要

关节内抗生素已被提议作为脓毒性关节炎的治疗方法,允许局部高浓度,而不会使患者遭受全身治疗的毒性/副作用。然而,在关节内高浓度使用这些溶液会引起软骨毒性。本系统综述的目的是评估关节内使用抗生素和抗菌溶液,并确定它们与体外或体内给药后软骨溶解的关系。方法:通过PubMed、Clinical Key、OVID和谷歌Scholar按照PRISMA指南进行系统评价。如果评估抗生素暴露后的软骨毒性,则纳入英语研究。结果:最初的检索结果为228项研究,其中36项研究符合标准。这36项研究包括研究24种不同药物的手稿。总的来说,24种药物中有7种(29%)是无软骨毒性的:米诺环素、四环素、氯霉素、替柯planin、培氟沙星、利奈唑胺、多粘菌素。8种(33%)药物结果不一致:强力霉素、头孢曲松、庆大霉素、万古霉素、环丙沙星、氧氟沙星、氯己定和聚维酮碘。9种(38%)药物具有明显的软性毒性,根据报道的估计半数最大抑制浓度(IC50),所有药物都具有剂量依赖性的软性毒性:阿米卡星(IC50 = 0.31-2.74 mg/mL)、新霉素(0.82)、头孢唑林(1.67-3.95)、头孢他啶(3.16-3.59)、氨苄西林-沙巴坦(8.64 - >5)、青霉素(11.61)、阿莫西林(14.01)、亚胺培南(>25)和托布霉素(>25)。此外,多西环素和米诺环素的软骨保护作用也有报道。结论:本系统综述确定了可用于治疗脓毒性关节炎的药物。9种药物由于其剂量依赖性的软骨毒性作用而应避免使用。需要进一步的研究来阐明这些药物在人类关节内使用的安全性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Review of Intra-Articular Use of Antibiotics and Antiseptic Irrigation and Their Systematic Association with Chondrolysis.

Introduction: Intra-articular antibiotics have been proposed as a treatment for septic arthritis to allow for high local concentrations without subjecting a patient to the toxicity/side effects of systemic therapy. However, there is concern for chondrotoxicity with intra-articular use of these solutions in high concentrations. The purpose of this systematic review was to evaluate the intra-articular use of antibiotics and antiseptic solutions, and to determine their association with chondrolysis following in vitro or in vivo administration.

Methods: A systematic review was conducted following PRISMA guidelines through PubMed, Clinical Key, OVID, and Google Scholar. Studies in English were included if they evaluated for chondrotoxicity following antibiotic exposure.

Results: The initial search resulted in 228 studies, with 36 studies meeting criteria. These 36 studies included manuscripts that studied 24 different agents. Overall, 7 of the 24 (29%) agents were non-chondrotoxic: minocycline, tetracycline, chloramphenicol, teicoplanin, pefloxacin, linezolid, polymyxin-bacitracin. Eight (33%) agents had inconsistent results: doxycycline, ceftriaxone, gentamicin, vancomycin, ciprofloxacin, ofloxacin, chlorhexidine, and povidone iodine. Chondrotoxicity was evident with 9 (38%) agents, all of which were also dose-dependent chondrotoxic based on reported estimated half maximal inhibitory concentrations (est. IC50): amikacin (est. IC50 = 0.31-2.74 mg/mL), neomycin (0.82), cefazolin (1.67-3.95), ceftazidime (3.16-3.59), ampicillin-sulbactam (8.64 - >25), penicillin (11.61), amoxicillin (14.01), imipenem (>25), and tobramycin (>25). Additionally, chondroprotective effects of doxycycline and minocycline were reported.

Conclusions: This systematic review identified agents that may be used in the treatment of septic arthritis. Nine agents should be avoided due to their dose-dependent chondrotoxic effects. Further studies are needed to clarify the safety of these medications for human intra-articular use.

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