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用于抗生素药物递送的生物可蚀性聚酸酐:大鼠模型系统中的体内骨髓炎治疗

Bioerodible polyanhydrides for antibiotic drug delivery: in vivo osteomyelitis treatment in a rat model system.

作者信息

Laurencin C T, Gerhart T, Witschger P, Satcher R, Domb A, Rosenberg A E, Hanff P, Edsberg L, Hayes W, Langer R

机构信息

Harvard-M.I.T. Division of Health Sciences and Technology, Cambridge, Massachusetts.

出版信息

J Orthop Res. 1993 Mar;11(2):256-62. doi: 10.1002/jor.1100110213.

DOI:10.1002/jor.1100110213
PMID:8483038
Abstract

Acute and chronic osteomyelitis can be difficult to treat by conventional means. Current methods of treatment involve the use of systemic antibiotics, the local implantation of non-degradable drug carriers, and surgical débridement. Each method has specific drawbacks. We report on the use of a new controlled release system utilizing gentamicin and bioerodible, biocompatible polymers (polyanhydrides) designed for drug delivery applications for the treatment of clinical osteomyelitis. We compared this system's ability to reduce bacterial levels in infected bone with that of conventional non-degradable delivery systems based on polymethylmethacrylate (PMMA) and gentamicin. Polyanhydride copolymers of bis-carboxyphenoxypropane and sebacic acid P loaded with gentamicin sulfate and PMMA/gentamicin matrices were implanted in the long bones of Sprague-Dawley rats infected with a strain of Staphylococcus aureus. After 3 weeks of implantation, the polymeric delivery devices were removed and quantitative cultures were used to determine bacterial levels in bone. The polyanhydride/gentamicin matrices demonstrated significant degradation over the 3 week implantation period. Levels of bacteria, measured in colony forming units, were significantly lower in bone implanted with the polyanhydride/gentamicin release system than in long bones of control animals without an implant (p < 0.01), of animals with a polyanhydride polymer implant alone (p < 0.01), and of animals with a PMMA/gentamicin implant (p = 0.03). Bioerodible polyanhydrides show promise as a new treatment modality for infections in bone.

摘要

急性和慢性骨髓炎采用传统方法可能难以治疗。目前的治疗方法包括使用全身性抗生素、植入不可降解的药物载体以及手术清创。每种方法都有特定的缺点。我们报告了一种新型控释系统的应用,该系统利用庆大霉素以及为药物递送应用设计的可生物蚀解、生物相容的聚合物(聚酸酐)来治疗临床骨髓炎。我们将该系统降低感染骨中细菌水平的能力与基于聚甲基丙烯酸甲酯(PMMA)和庆大霉素的传统不可降解递送系统的能力进行了比较。将负载硫酸庆大霉素的双羧基苯氧基丙烷和癸二酸聚酸酐共聚物P以及PMMA/庆大霉素基质植入感染了金黄色葡萄球菌菌株的Sprague-Dawley大鼠的长骨中。植入3周后,取出聚合物递送装置,采用定量培养法测定骨中的细菌水平。在3周的植入期内,聚酸酐/庆大霉素基质显示出明显的降解。以菌落形成单位衡量,植入聚酸酐/庆大霉素释放系统的骨中的细菌水平显著低于未植入的对照动物的长骨(p < 0.01)、仅植入聚酸酐聚合物的动物的长骨(p < 0.01)以及植入PMMA/庆大霉素的动物的长骨(p = 0.03)。可生物蚀解的聚酸酐有望成为治疗骨感染的一种新的治疗方式。

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