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手术部位感染和生物膜的预防:头孢唑林和甲硝唑在肿胀液利多卡因溶液中的皮下药代动力学

Prevention of Surgical Site Infections and Biofilms: Pharmacokinetics of Subcutaneous Cefazolin and Metronidazole in a Tumescent Lidocaine Solution.

作者信息

Klein Jeffrey A, Langman Loralie J

机构信息

Department of Dermatology, University of California, Irvine, School of Medicine, Irvine, Calif.; and Toxicology and Drug Monitoring Laboratory, Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minn.

出版信息

Plast Reconstr Surg Glob Open. 2017 May 30;5(5):e1351. doi: 10.1097/GOX.0000000000001351. eCollection 2017 May.

Abstract

BACKGROUND

Tumescent anesthesia antibiotic delivery (TAAD) consists of subcutaneous infiltration of antibiotic(s) dissolved tumescent lidocaine anesthesia. Tumescent lidocaine anesthesia contains lidocaine (≤ 1 g/L), epinephrine (≤ 1 mg/L), sodium bicarbonate (10 mEq/L) in 0.9% saline. Our aim was to measure cefazolin and metronidazole concentrations over time in subcutaneous tumescent interstitial fluid (TISF) after TAAD, in serum after TAAD and after intravenous antibiotic delivery (IVAD). We hypothesize that the pharmacokinetic/pharmacodynamic profiles of TAAD + IVAD are superior to IVAD alone for the prevention of surgical site infections and biofilms.

METHODS

Concentrations of cefazolin and metronidazole in TISF and serum following TAAD and in serum following IVAD were compared in 5 female volunteers. Subjects received cefazolin or cefazolin plus metronidazole by IVAD alone and by TAAD alone. One subject also received concomitant IVAD and TAAD of these 2 antibiotics. Sequential samples of serum or subcutaneous TISF were assayed for antibiotic concentration.

RESULTS

Cefazolin (1 g) by TAAD resulted in an area under the curve of the concentration-time profile and a maximum concentration (Cmax) in subcutaneous tissue that were 16.5 and 5.6 times greater than in serum following 1 g by IVAD. Metronidazole (500 mg) by TAAD resulted in an area under the curve and Cmax that were 8.1 and 24.7 times greater in TISF, than in serum after 500 mg by intravenous delivery. IVAD + TAAD resulted in superior antibiotic concentrations to IVAD alone.

CONCLUSIONS

TAAD + IVAD produced superior antibiotic bioavailability in both subcutaneous interstitial fluid and serum compared with IVAD alone. There was no evidence that TAAD of cefazolin and metronidazole poses a significant risk of harm to patients.

摘要

背景

肿胀麻醉抗生素给药(TAAD)包括将抗生素溶解于肿胀利多卡因麻醉剂中进行皮下浸润。肿胀利多卡因麻醉剂在0.9%盐水中含有利多卡因(≤1g/L)、肾上腺素(≤1mg/L)、碳酸氢钠(10mEq/L)。我们的目的是测量TAAD后皮下肿胀组织间液(TISF)、TAAD后血清以及静脉抗生素给药(IVAD)后血清中头孢唑林和甲硝唑随时间的浓度。我们假设TAAD+IVAD的药代动力学/药效学特征在预防手术部位感染和生物膜方面优于单纯IVAD。

方法

在5名女性志愿者中比较TAAD后TISF和血清中以及IVAD后血清中头孢唑林和甲硝唑的浓度。受试者分别接受单纯IVAD和单纯TAAD的头孢唑林或头孢唑林加甲硝唑。一名受试者还同时接受了这两种抗生素的IVAD和TAAD。对血清或皮下TISF的连续样本进行抗生素浓度检测。

结果

TAAD给予1g头孢唑林后,皮下组织中浓度-时间曲线下面积和最大浓度(Cmax)分别比IVAD给予1g后血清中的值高16.5倍和5.6倍。TAAD给予500mg甲硝唑后,TISF中的曲线下面积和Cmax分别比静脉给药500mg后血清中的值高8.1倍和24.7倍。IVAD+TAAD产生的抗生素浓度优于单纯IVAD。

结论

与单纯IVAD相比,TAAD+IVAD在皮下组织间液和血清中均产生了更高的抗生素生物利用度。没有证据表明头孢唑林和甲硝唑的TAAD对患者构成重大危害风险。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f401/5459654/657da5d957f5/gox-5-e1351-g001.jpg

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