首页> 外文期刊>Journal of biomedical materials research. Part B, Applied biomaterials. >Effect of erythromycin-doped calcium polyphosphate scaffold composite in a mouse pouch infection model
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Effect of erythromycin-doped calcium polyphosphate scaffold composite in a mouse pouch infection model

机译:红霉素掺杂钙多磷酸钙支架复合材料在小鼠袋感染模型的影响

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We previously showed that strontium-doped calcium polyphosphate (SCPP) scaffold with poly(vinyl alcohol) (PVA) coating extended the impregnated erythromycin (EM) release. In this study, we examined the bactericidal effect of EM-doped SCPP (SCPPEM) scaffolds with PVA coating in a Staphylococcus aureus (S. aureus) infected mouse pouch. SCPP scaffolds with or without 5% EM, and SCPPEM scaffolds coated with PVA (with or without 5% EM) were prepared. Scaffolds were implanted in the pouch of BALB/c mice, followed by inoculation of 1 × 103 colony-forming units of S. aureus. Mice were sacrificed 14 days after surgery. Pouch tissues and scaffolds were collected for histology, scanning electron microscopy, and microbiological analysis. In the absence of SCPP scaffolds, the pouch infection was eliminated by the host immune surveillance. In the presence of SCPP scaffolds, both the pouch tissues and scaffolds were infected, but SCPPEM scaffolds successfully inhibited bacterial growth. Although PVA coating of SCPP EM scaffolds enhanced bacterial growth, incorporation of EM into PVA coating inhibited growth. In conclusion, BALB/c mice were capable of eradicating a low grade S. aureus infection. SCPP protected S. aureus growth from host immune surveillance. Though PVA coating sustained EM release in vitro, it was unable to inhibit bacterial growth because PVA gel matrix provided a temporary shelter for bacteria to grow and slowed the EM release from SCPP scaffold. To guarantee a sufficient inhibition of bacterial growth at the initial stage, embedding EM or other antibiotics in the PVA coating is also essential.
机译:我们以前表明,掺杂锶钙多磷酸钙(SCPP)支架具有聚(乙烯醇)(PVA)涂层延伸浸渍的红霉素(EM)释放。在这项研究中,我们检查了EM-DOPED SCPP(SCPPEM)支架用PVA涂层在葡萄球菌(金黄色葡萄球菌)感染的小鼠袋中的杀菌作用。制备SCPP支架或没有5%EM的支架,并制备涂有PVA(有或没有5%EM)的SCPPEM支架。在BALB / C小鼠的小袋中植入支架,然后接种1×103个形成金黄色葡萄球菌的单位。手术后14天处死小鼠。收集袋组织和支架用于组织学,扫描电子显微镜和微生物分析。在没有SCPP支架的情况下,通过宿主免疫监测消除了袋感染。在SCPP支架存在下,袋组织和支架都被感染,但SCPPEM支架成功抑制细菌生长。虽然SCPP EM支架的PVA涂层增强了细菌生长,但将EM掺入PVA涂层抑制生长。总之,Balb / c小鼠能够消除低等级的金黄色葡萄球菌感染。 SCPP保护S. aureus从宿主免疫监测中生长。虽然PVA涂层在体外释放EM释放,但它无法抑制细菌生长,因为PVA凝胶基质为细菌提供了临时避难所,以生长并减慢来自SCPP支架的EM释放。为了保证在初始阶段进行充分抑制细菌生长,在PVA涂层中嵌入EM或其他抗生素也是必需的。

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