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High-velocity microsprays enhance antimicrobial activity in S. mutans biofilms

机译:高速微阵列增强变形链球菌生物膜中的抗微生物活性

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摘要

Streptococcus mutans in dental plaque biofilms play a role in caries development. The biofilm’s complex structure enhances the resistance to antimicrobial agents by limiting the transport of active agents inside the biofilm. We assessed the ability of high-velocity water microsprays to enhance delivery of antimicrobials into 3-days old S. mutans biofilms. Biofilms were exposed to a 90° or 30° impact, firstly using a 1-?m tracer beads solution (109 beads/mL) and secondly, a 0.2% Chlorhexidine (CHX) or 0.085% Cetylpyridinium chloride (CPC) solution. For comparison, a 30-sec diffusive transport and simulated mouthwash were also performed. Confocal microscopy was used to determine number and relative bead penetration depth (RD) into the biofilm. Assessment of antimicrobial penetration was determined by calculating the killing depth (KD) detected by live/dead viability staining. We firstly demonstrated that the microspray was able to deliver significantly more microbeads deeper in the biofilm compared to diffusion and mouthwashing exposures. Next our experiments revealed that the microspray yielded better antimicrobial penetration evidenced by deeper killing inside the biofilm and a wider killing zone around the zone of clearance than a diffusion transport with the same antimicrobials. Interestingly the 30° impact in the distal position delivered approximately 16 times more microbeads and yielded approximately 20% more bacteria killing (for both CHX and CPC) than the 90o impact. These data suggest that high-velocity water microsprays can be used as an effective mechanism to deliver micro-particles and antimicrobials inside S. mutans biofilms. High shear stresses generated at the biofilm/burst interface might have enhanced beads and antimicrobials delivery inside the remaining biofilm by combining forced advection into the biofilm matrix and physical restructuring of the biofilm itself. Further, the impact angle has potential to be optimized both for biofilm removal and active agents’ delivery inside biofilm in those protected areas where some biofilm might remain
机译:牙菌斑生物膜中的变形链球菌在龋齿发育中起作用。生物膜的复杂结构通过限制生物膜内部活性剂的运输来增强对抗菌剂的抵抗力。我们评估了高速水微喷雾增强抗菌素向3天大的变形链球菌生物膜中的传递的能力。首先将生物膜暴露在90°或30°的冲击下,首先使用1-μm示踪剂珠溶液(109个珠子/ mL),其次使用0.2%洗必泰(CHX)或0.085%氯化十六烷基吡啶(CPC)溶液。为了进行比较,还进行了30秒的扩散运输和模拟漱口。共聚焦显微镜用于确定进入生物膜的数量和相对的珠穿透深度(RD)。通过计算通过活/死活力染色检测的杀灭深度(KD)来确定抗微生物渗透性的评估。我们首先证明,与扩散和漱口相比,微喷雾能够在生物膜深处传递更多的微珠。接下来,我们的实验表明,与相同的抗菌剂的扩散转运相比,微喷雾产生的抗菌剂穿透性更好,这是由生物膜内部更深的杀伤力和清除区周围更宽的杀伤力所证明的。有趣的是,远端位置的30°撞击比90o撞击多输送了约16倍的微珠,杀灭细菌(对于CHX和CPC而言)大约多20%。这些数据表明,高速水微喷雾可以用作在变形链球菌生物膜内部输送微粒和抗菌剂的有效机制。在生物膜/爆裂界面处产生的高剪切应力可能通过将强制对流结合到生物膜基质和生物膜本身的物理重组中而增强了在剩余生物膜内部的珠粒和抗菌素的释放。此外,在生物膜内部可能保留一些生物膜的那些受保护区域中,对于生物膜去除和活性剂在生物膜内部的输送,碰撞角度都有可能被优化

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