铜绿假单胞菌生物膜杀死超越间隔的抗生素负载硫酸钙珠:一个体外研究。

IF 1.8 Q3 INFECTIOUS DISEASES Journal of Bone and Joint Infection Pub Date : 2021-03-23 eCollection Date: 2021-01-01 DOI:10.5194/jbji-6-119-2021
Jacob R Brooks, Devendra H Dusane, Kelly Moore, Tripti Gupta, Craig Delury, Sean S Aiken, Phillip A Laycock, Anne C Sullivan, Jeffrey F Granger, Matthew V Dipane, Edward J McPherson, Paul Stoodley
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引用次数: 3

摘要

细菌生物膜是慢性假体周围关节感染(PJI)和其他骨科感染的重要毒力因子,因为它们对抗生素和宿主免疫具有高度耐受性。抗生素被混合到载体中,如骨水泥和硫酸钙骨空隙填充物,以实现持续高浓度的抗生素,通过局部释放更有效地控制生物膜感染。采用具有临床意义的“大琼脂板”模型,研究了载抗生素硫酸钙珠(ALCS-B)与PMMA骨水泥间隔剂联合扩散抗生素对铜绿假单胞菌Xen41 (PA-Xen41)生物膜扩散和杀伤的影响。方法:将生长在各种骨科材料圆盘上的生物发光PA-Xen41生物膜放置在一个大的琼脂板上,琼脂板上有一个PMMA全尺寸模拟“间隔剂”,该“间隔剂”卸载或加载万古霉素和妥布霉素,带或不带ALCS-B。通过生物发光成像和活细胞计数来评估距离间隔器不同距离上的生物膜扩散量和对数减少量。结果:在未加载隔离剂的对照组中,PA-Xen41从生物膜上扩散到整个平板上。加载的间隔物产生了一个3 厘米的抑制区,并显著减少了紧挨着间隔物的圆盘上的生物膜细菌,但远离间隔物的圆盘上的生物膜细菌减少很少或为零。ALCS-B和装载的PMMA间隔物的组合极大地减少了细菌的传播,并导致距离间隔物所有距离的圆盘上的生物膜明显减少。讨论:在装载抗生素的间隔模拟物中添加ALCS-B增加了抗生素覆盖面积和对生物膜的有效性,这表明这些仓库的组合可能提供更大的物理抗生素覆盖范围和更有效的死区管理,特别是在抗生素传播受扩散限制的区域(很少或没有流体运动的区域)。
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Pseudomonas aeruginosa biofilm killing beyond the spacer by antibiotic-loaded calcium sulfate beads: an in vitro study.

Introduction: Bacterial biofilms are an important virulence factor in chronic periprosthetic joint infection (PJI) and other orthopedic infection since they are highly tolerant to antibiotics and host immunity. Antibiotics are mixed into carriers such as bone cement and calcium sulfate bone void fillers to achieve sustained high concentrations of antibiotics required to more effectively manage biofilm infections through local release. The effect of antibiotic diffusion from antibiotic-loaded calcium sulfate beads (ALCS-B) in combination with PMMA bone cement spacers on the spread and killing of Pseudomonas aeruginosa Xen41 (PA-Xen41) biofilm was investigated using a "large agar plate" model scaled for clinical relevance. Methods: Bioluminescent PA-Xen41 biofilms grown on discs of various orthopedic materials were placed within a large agar plate containing a PMMA full-size mock "spacer" unloaded or loaded with vancomycin and tobramycin, with or without ALCS-B. The amount of biofilm spread and log reduction on discs at varying distances from the spacer was assessed by bioluminescent imaging and viable cell counts. Results: For the unloaded spacer control, PA-Xen41 spread from the biofilm to cover the entire plate. The loaded spacer generated a 3 cm zone of inhibition and significantly reduced biofilm bacteria on the discs immediately adjacent to the spacer but low or zero reductions on those further away. The combination of ALCS-B and a loaded PMMA spacer greatly reduced bacterial spread and resulted in significantly greater biofilm reductions on discs at all distances from the spacer. Discussion: The addition of ALCS-B to an antibiotic-loaded spacer mimic increased the area of antibiotic coverage and efficacy against biofilm, suggesting that a combination of these depots may provide greater physical antibiotic coverage and more effective dead space management, particularly in zones where the spread of antibiotic is limited by diffusion (zones with little or no fluid motion).

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来源期刊
CiteScore
3.70
自引率
0.00%
发文量
29
审稿时长
12 weeks
期刊最新文献
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