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Polyvinylidene fluoride-Hyaluronic acid wound dressing comprised of ionic liquids for controlled drug delivery and dual therapeutic behavior

机译:聚偏二氟乙烯 - 透明质酸伤口敷料由离子液体组成,用于受控药物递送和双重治疗行为

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摘要

To improve the efficacy of transdermal drug delivery systems, the physical and chemical properties of drugs need to be optimized to better penetrate into the stratum corneum and to better diffuse into the epidermis and dermis layers. Accordingly, dual-biological function ionic liquids composed of active pharmaceutical ingredients were synthesized, comprising both analgesic and anti-inflammatory properties, by combining a cation derived from lidocaine and anions derived from hydrophobic nonsteroidal anti-inflammatory drugs. Active pharmaceutical ingredient ionic liquids (API-ILs) were characterized through nuclear magnetic resonance, cytotoxicity assay, and water solubility assay. All properties were compared with those of the original drugs. By converting the analgesic and anti-inflammatory drugs into dual-function API-ILs, their water solubility increased up to 470-fold, without affecting their cytotoxic profile. These API-ILs were incorporated into a bilayer wound dressing composed of a hydrophobic polyvinylidene fluoride (PVDF) membrane to act as a drug reservoir and a biocompatible hyaluronic acid (HA) layer. The prepared bilayer wound dressing was characterized in terms of mechanical properties, membrane drug uptake and drug release behavior, and application in transdermal delivery, demonstrating to have desirable mechanical properties and improved release of API-ILs. The assessment of anti-inflammatory activity through the inhibition of LPS-induced production of nitric oxide and prostaglandin E2 by macrophages revealed that the prepared membranes containing API-ILs are as effective as those with the original drugs. Cell adhesion of fibroblasts on membrane surfaces and cell viability assay confirmed improved the viability and adhesion of fibroblasts on PVDF/HA membranes. Finally, wound healing assay performed with fibroblasts showed that the bilayer membranes containing dual-function API-ILs are not detrimental to wound healing, while displaying increased and controlled drug delivery and dual therapeutic behavior.
机译:为了提高透皮药物递送系统的功效,需要优化药物的物理和化学性质,以更好地渗透到角质层中并更好地扩散到表皮和真皮层中。因此,合成了由活性药物成分组成的双生物功能离子液体,包括镇痛和抗炎特性,通过组合衍生自利多卡因和衍生自疏水性非甾体抗炎药的阴离子的阳离子。通过核磁共振,细胞毒性测定和水溶性测定,表征活性药物成分离子液体(API-ILS)。将所有性质与原始药物的所有性能进行比较。通过将镇痛和抗炎药转化为双功能API-ILS,它们的水溶性高达470倍,而不影响其细胞毒性曲线。将这些API-ILS掺入双层伤口敷料中,该磨削敷料由疏水性聚偏二氟乙烯(PVDF)膜组成,以充当药物储存器和生物相容性透明质酸(HA)层。制备的双层伤口敷料表征在机械性能,膜药吸收和药物释放行为方面,以及在透皮递送中的应用,证明具有所需的机械性能并改善API-ILS的释放。通过巨噬细胞抑制LPS诱导的一氧化物和前列腺素E2的抗炎活性评估抗炎活性显示,含有API-ILS的制备的膜与原有药物一样有效。成纤维细胞对膜表面和细胞活力测定的细胞粘附证实了成分对PVDF / HA膜上成纤维细胞的活力和粘附性。最后,用成纤维细胞进行的伤口愈合测定表明,含有双功能API-ILS的双层膜不是对伤口愈合不利,同时显示增加和控制的药物递送和双重治疗行为。

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