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A pre-therapeutic coating for medical devices that prevents the attachment of Candida albicans

机译:医疗设备的治疗前涂层,可防止白色念珠菌的附着

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Background Hospital acquired fungal infections are defined as “never events”—medical errors that should never have happened. Systemic Candida albicans infections results in 30–50% mortality rates. Typically, adhesion to abiotic medical devices and implants initiates such infections. Efficient adhesion initiates formation of aggressive biofilms that are difficult to treat. Therefore, inhibitors of adhesion are important for drug development and likely to have a broad spectrum efficacy against many fungal pathogens. In this study we further the development of a small molecule, Filastatin, capable of preventing C. albicans adhesion. We explored the potential of Filastatin as a pre-therapeutic coating of a diverse range of biomaterials. Methods Filastatin was applied on various biomaterials, specifically bioactive glass (cochlear implants, subcutaneous drug delivery devices and prosthetics); silicone (catheters and other implanted devices) and dental resin (dentures and dental implants). Adhesion to biomaterials was evaluated by direct visualization of wild type C. albicans or a non-adherent mutant edt1 ?/? that were stained or fluorescently tagged. Strains grown overnight at 30?°C were harvested, allowed to attach to surfaces for 4?h and washed prior to visualization. The adhesion force of C. albicans cells attached to surfaces treated with Filastatin was measured using Atomic Force Microscopy. Effectiveness of Filastatin was also demonstrated under dynamic conditions using a flow cell bioreactor. The effect of Filastatin under microfluidic flow conditions was quantified using electrochemical impedance spectroscopy. Experiments were typically performed in triplicate. Results Treatment with Filastatin significantly inhibited the ability of C. albicans to adhere to bioactive glass (by 99.06%), silicone (by 77.27%), and dental resin (by 60.43%). Atomic force microcopy indicated that treatment with Filastatin decreased the adhesion force of C. albicans from 0.23 to 0.017?nN. Electrochemical Impedance Spectroscopy in a microfluidic device that mimic physiological flow conditions in vivo showed lower impedance for C. albicans when treated with Filastatin as compared to untreated control cells, suggesting decreased attachment. The anti-adhesive properties were maintained when Filastatin was included in the preparation of silicone materials. Conclusion We demonstrate that Filastatin treated medical devices prevented adhesion of Candida, thereby reducing nosocomial infections.
机译:背景医院获得性真菌感染被定义为“从不发生”,即永远不应该发生的医疗错误。全身性白色念珠菌感染导致30-50%的死亡率。通常,对非生物医疗器械和植入物的粘附会引发此类感染。高效的粘附力会引发难以治疗的侵蚀性生物膜的形成。因此,粘附抑制剂对于药物开发很重要,并且可能对许多真菌病原体具有广谱功效。在这项研究中,我们进一步开发了能够阻止白色念珠菌粘附的小分子Filastatin。我们探索了Filastatin作为多种生物材料的治疗前涂层的潜力。方法:将Filastatin应用于各种生物材料,特别是生物活性玻璃(人工耳蜗,皮下给药装置和假体)。硅树脂(导管和其他植入设备)和牙科树脂(义齿和牙科植入物)。通过直接观察染色或荧光标记的野生型白色念珠菌或非粘附突变体edt1 ?/?评估对生物材料的粘附性。收获在30°C过夜生长的菌株,使其附着在表面4小时,并在可视化之前洗涤。使用原子力显微镜法测量附着在用Filastatin处理过的表面上的白色念珠菌细胞的粘附力。在流动条件下使用流通池生物反应器也证明了Filastatin的有效性。使用电化学阻抗谱定量分析了Filastatin在微流体流动条件下的作用。实验通常一式三份进行。结果Filastatin处理可显着抑制白色念珠菌粘附于生物活性玻璃的能力(达99.06%),硅酮(达77.27%)和牙科树脂(达60.43%)。原子力显微镜检查表明,用Filastatin处理可使白色念珠菌的粘附力从0.23降至0.017?nN。与未经处理的对照细胞相比,当用Filastatin处理时,模仿体内生理流动条件的微流控装置中的电化学阻抗谱显示对白色念珠菌的阻抗较低,这表明附着力降低。当Filastatin包括在有机硅材料的制备中时,保持了抗粘性能。结论我们证明,用Filastatin处理的医疗器械可防止念珠菌粘附,从而减少医院感染。

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