Normandie Univ, UNIRouen Normandie, INSA Rouen, CNRS, PBS, 76000 Rouen, France.
Normandie Univ, UNIRouen Normandie, LMSM EA4312, 27000 Evreux, France.
Mater Sci Eng C Mater Biol Appl. 2020 Jan;106:110130. doi: 10.1016/j.msec.2019.110130. Epub 2019 Aug 24.
Chronic infection is a major cause of delayed wound-healing. It is recognized to be associated with infectious bacterial communities called biofilms. Currently used conventional antibiotics alone often reveal themselves ineffective, since they do not specifically target the wound biofilm. Here, we report a new conceptual tool aimed at overcoming this drawback: an antibiofilm drug delivery system targeting the bacterial biofilm as a whole, by inhibiting its formation and/or disrupting it once it is formed. The system consists of a micro/nanostructured poly(butylene-succinate-co-adipate) (PBSA)-based asymmetric membrane (AM) with controlled porosity. By the incorporation of hydrophilic porogen agents, polyvinylpyrrolidone (PVP) and polyethylene glycol (PEG), we were able to obtain AMs with high levels of porosity, exhibiting interconnections between pores. The PBSA-PEG membrane presented a dense upper layer with pores small enough to block bacteria penetration. Upon using such porogen agents, under dry and wet conditions, membrane's integrity and mechanical properties were maintained. Using bovine serum albumin (BSA) as a model protein, we demonstrated that protein loading and release from PBSA membranes were affected by the membrane structure (porosity) and the presence of residual porogen. Furthermore, the release curve profile consisted of a fast initial slope followed by a second slow phase approaching a plateau within 24 h. This can be highly beneficial for the promotion of wound healing. Cross-sectional confocal laser scanning microscopy (CLSM) images revealed a heterogeneous distribution of fluorescein isothiocyanate (FITC) labeled BSA throughout the entire membrane. PBSA membranes were loaded with dispersin B (DB), a specific antibiofilm matrix enzyme. Studies using a Staphylococcus epidermidis model, indicate significant efficiency in both inhibiting or dispersing preformed biofilm (up to 80 % eradication). The asymmetric PBSA membrane prepared with the PVP porogen (PBSA-PVP) displayed highest antibiofilm activity. Moreover, in vitro cytotoxicity assays using HaCaT and reconstructed human epidermis (RHE) models revealed that unloaded and DB-loaded PBSA-PVP membranes had excellent biocompatibility suitable for wound dressing applications.
慢性感染是导致伤口愈合延迟的主要原因。人们认识到,它与被称为生物膜的传染性细菌群落有关。目前单独使用常规抗生素往往效果不佳,因为它们不能专门针对伤口生物膜。在这里,我们报告了一种新的概念工具,旨在克服这一缺点:一种针对细菌生物膜的整体的抗生物膜药物输送系统,通过抑制其形成和/或一旦形成就破坏它。该系统由具有受控孔隙率的微/纳米结构化聚丁二酸丁二醇酯-共-己二酸酯 (PBSA) 基不对称膜 (AM) 组成。通过加入亲水性致孔剂聚维酮 (PVP) 和聚乙二醇 (PEG),我们能够获得具有高孔隙率的 AM,其具有孔之间的连接。PBSA-PEG 膜具有致密的上层,其孔小到足以阻止细菌渗透。在使用此类致孔剂的情况下,无论是在干燥还是湿润条件下,膜的完整性和机械性能都得以维持。使用牛血清白蛋白 (BSA) 作为模型蛋白,我们证明了 PBSA 膜的蛋白负载和释放受膜结构(孔隙率)和残留致孔剂的影响。此外,释放曲线呈快速初始斜率,随后在 24 小时内进入第二缓慢阶段接近平台。这对于促进伤口愈合非常有益。共聚焦激光扫描显微镜 (CLSM) 图像的横截面显示,异硫氰酸荧光素 (FITC) 标记的 BSA 均匀分布在整个膜中。PBSA 膜负载分散素 B (DB),一种特定的抗生物膜基质酶。使用表皮葡萄球菌模型的研究表明,它在抑制或分散已形成的生物膜方面均具有很高的效率(高达 80%的消除率)。用 PVP 致孔剂制备的不对称 PBSA 膜 (PBSA-PVP) 显示出最高的抗生物膜活性。此外,使用 HaCaT 和重建的人表皮 (RHE) 模型进行的体外细胞毒性试验表明,未负载和 DB 负载的 PBSA-PVP 膜具有优异的生物相容性,适用于伤口敷料应用。
