在大鼠腹肌袋模型中,全身利福平显示局部植入羟基磷灰石颗粒的增加。

IF 1.8 Q3 INFECTIOUS DISEASES
Sujeesh Sebastian, Jintian Huang, Yang Liu, Mattias Collin, Magnus Tägil, Deepak Bushan Raina, Lars Lidgren
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引用次数: 1

摘要

生物材料联合抗生素通常用于骨感染的治疗。在第一周洗脱高浓度抗生素后,抗生素的亚抑制浓度可能导致顽固细菌的后期重新繁殖。最近的研究表明,全身给予四环素和利福平(RIF)等抗生素可以寻找并结合局部植入的羟基磷灰石(HA)。这项体内研究的目的是测试系统给予利福平是否可以在事先或不事先加载抗生素的情况下补充ha基生物材料,以保护材料免受后期细菌繁殖的影响。方法:系统给药RIF对三种不同类型ha基材料的体内增积。第1组采用纳米(n)和微米(m)大小的HA颗粒,第2组采用不预装抗生素庆大霉素(GEN)或万古霉素(VAN)的硫酸钙/羟基磷灰石(CaS / HA)生物材料,第3组采用含有GEN (CaS / HA + GEN)或VAN (CaS / HA + VAN)的CaS / HA材料。将上述材料植入大鼠腹肌袋模型,术后7 d将动物分为对照组(即不给予全身抗生素)和试验组(即每天单次腹腔注射RIF(4 mg /只大鼠),连续3天)。第三次注射24小时后,处死动物,取出植入的微球,用琼脂扩散法检测金黄色葡萄球菌ATCC 25923的抗性。孵育过夜后,测定微丸周围的抑制带(ZOI)。结果:对照组2 / 6个CaS / HA + GEN微丸出现ZOI,其余微丸均无ZOI。试验1组动物的微丸均无ZOI。试验2组10 / 10 CaS / HA微丸呈ZOI。试验3组5 / 6 CaS / HA + GEN和4 / 6 CaS / HA + VAN微丸均出现ZOI。结论:在这项概念验证研究中,我们已经证明局部植入的双相CaS / HA载体在1周后可以通过系统给药RIF加载并发挥抗菌作用。需要进一步的体内感染模型来验证我们的发现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Systemic rifampicin shows accretion to locally implanted hydroxyapatite particles in a rat abdominal muscle pouch model.

Introduction: biomaterials combined with antibiotics are routinely used for the management of bone infections. After eluting high concentrations of antibiotics during the first week, sub-inhibitory concentrations of antibiotics may lead to late repopulation of recalcitrant bacteria. Recent studies have shown that systemically given antibiotics like tetracycline and rifampicin (RIF) could seek and bind to locally implanted hydroxyapatite (HA). The aim of this in vivo study was to test if systemically administered rifampicin could replenish HA-based biomaterials with or without prior antibiotic loading to protect the material from late bacterial repopulation. Methods: in vivo accretion of systemically administered RIF to three different types of HA-based materials was tested. In group 1, nano (n)- and micro (m)-sized HA particles were used, while group 2 consisted of a calcium sulfate / hydroxyapatite (CaS / HA) biomaterial without preloaded antibiotics gentamycin (GEN) or vancomycin (VAN), and in group 3, the CaS / HA material contained GEN (CaS / HA + GEN) or VAN (CaS / HA + VAN). The above materials were implanted in an abdominal muscle pouch model in rats, and at 7 d post-surgery, the animals were assigned to a control group (i.e., no systemic antibiotic) and a test group (i.e., animals receiving one single intraperitoneal injection of RIF each day (4 mg per rat) for 3 consecutive days). Twenty-four hours after the third injection, the animals were sacrificed and the implanted pellets were retrieved and tested against Staphylococcus aureus ATCC 25923 in an agar diffusion assay. After overnight incubation, the zone of inhibition (ZOI) around the pellets were measured. Results: in the control group, 2 / 6 CaS / HA + GEN pellets had a ZOI, while all other harvested pellets had no ZOI. No pellets from animals in test group 1 had a ZOI. In test group 2, 10 / 10 CaS / HA pellets showed a ZOI. In test group 3, 5 / 6 CaS / HA + GEN and 4 / 6 CaS / HA + VAN pellets showed a ZOI. Conclusions: in this proof-of-concept study, we have shown that a locally implanted biphasic CaS / HA carrier after 1 week can be loaded by systemic RIF administration and exert an antibacterial effect. Further in vivo infection models are necessary to validate our findings.

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来源期刊
CiteScore
3.70
自引率
0.00%
发文量
29
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12 weeks
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