首页> 外文期刊>Asian Journal of Pharmaceutical and Clinical Research >SYNTHESIS AND CHARACTERIZATION OF NOVEL SA-PA-LSA/C-30B/AG NANOCOMPOSITES FOR SWELLING, ANTIBACTERIAL, DRUG DELIVERY, AND ANTICANCER APPLICATIONS
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SYNTHESIS AND CHARACTERIZATION OF NOVEL SA-PA-LSA/C-30B/AG NANOCOMPOSITES FOR SWELLING, ANTIBACTERIAL, DRUG DELIVERY, AND ANTICANCER APPLICATIONS

机译:新型SA-PA-LSA / C-30B / AG纳米复合材料的合成和表征,用于溶胀,抗菌,药物输送和抗癌应用

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Objective: The main objective of this work was to formulate and evaluate Closite-30BanoAg filled hydrogel composites which are further intentended to be used for the study of drug delivery,antibacterial, and anticancer activity Methods: In this study, Cloisite-30B (C-30B) clay dispersed biopolymer sodium alginate (SA)-grafted-poly (acrylamide [AAm]-co-lignosulfonic acid) hydrogel composites were synthesized by free radical in situ polymerization reaction technique using SA, AAm, and lignosulfonic acid biopolymers in different proportions in combination. which are subjected to invitro drug delivery and Minimum inhibitory concentration(MIC) method for antibacterial activity study by using Streptococcus faecalis ( S.faecalis ) and Escherichia coli ( E. coli )bacteria. The biocompatibility of the prepared gels were determined by standard protocol HaCaT-cells and MCF-7 cell lines further the prepared hydrogel composites were characterized for particle size,encapsulation efficiency,swelling properties,compatibility studies by FTIR etc. Results: The formulated hydrogels were characterized by X-ray diffraction (XRD) to analyze the particles size and crystallinity. The presence of functional groups and their chemical interaction with the drug, C-30B, and silver nanoparticles (AgNPs) were confirmed by the FTIR spectroscopy. Furthermore, the presence of AgNPs in the matrix was confirmed by ultraviolet/visible spectroscopy. Thermogravimetric analysis was performed to find out the thermal degradation, thermal stability, and the percentage of weight loss at various temperatures. Swelling studies revealed that C-30B and AgNPs induced composites exhibited higher swelling ratio than pure hydrogels. The hydrogels with C-30B/AgNPs displayed excellent antibacterial activity against both Gram-positive and Gram-negative bacteria. Further, these hydrogel composites were loaded with the drug paclitaxel (PT), and drug release study showed that the sustained release of the drug from C-30B/Ag hydrogel matrix compared to rest of other samples. Hydrogel composites were cytocompatible in nature (with HaCaT cells) and the cell viability decreased (with MCF-7cells) with the presence of lignosulfonic acid as well as C-30B and AgNPs in the samples as evaluated through 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide to its insoluble formazan assay. Conclusion: The synthesized hydrogel composites were successfully characterized and eavaluated for sustained release of paclitaxel drug delivery at different pHs and temperatures and it is found that C30B/Ag filled composites exhibits contolled release of drug with higher rate, especially at lower pH (pH2) and higher temperature (37oC) and the same formulations which exhibits better anitbcterial and anticancer activity compared to the virgin samples So the prepared C30B/AgNPs hydrogels composites used in drug dlivery for the effective treatment of cancer and used against bacterias and cancerous cells.
机译:目的:这项工作的主要目的是配制和评估Closite-30B / nanoAg填充的水凝胶复合材料,该复合材料可进一步用于研究药物递送,抗菌和抗癌活性。方法:在本研究中,Cloisite-30B(通过自由基原位聚合反应技术,分别使用SA,AAm和木质素磺酸生物聚合物,合成了C-30B)粘土分散生物聚合物海藻酸钠(SA)-接枝聚(丙烯酰胺[AAm]-共-木质磺酸)水凝胶复合材料。比例组合。分别使用粪链球菌(S.faecalis)和大肠杆菌(E. coli)进行体外药物递送和最小抑菌浓度(MIC)方法进行抗菌活性研究。通过标准方案HaCaT细胞和MCF-7细胞系测定制备的凝胶的生物相容性,并通过粒度,包封效率,溶胀性,FTIR研究相容性等对制备的水凝胶复合材料进行表征。结果:表征了配制的水凝胶通过X射线衍射(XRD)分析颗粒的大小和结晶度。 FTIR光谱证实了官能团的存在及其与药物,C-30B和银纳米颗粒(AgNPs)的化学相互作用。此外,通过紫外/可见光谱法确认了基质中AgNP的存在。进行热重分析以找出在各种温度下的热降解,热稳定性和重量损失百分比。溶胀研究表明,C-30B和AgNPs诱导的复合材料比纯水凝胶具有更高的溶胀率。具有C-30B / AgNPs的水凝胶对革兰氏阳性菌和革兰氏阴性菌均显示出优异的抗菌活性。此外,这些水凝胶复合材料载有紫杉醇(PT)药物,药物释放研究表明,与其他样品相比,药物从C-30B / Ag水凝胶基质中持续释放。通过3-(4,5-二甲基噻唑)评估,样品中存在木质素磺酸以及C-30B和AgNPs的情况下,水凝胶复合物具有自然的细胞相容性(与HaCaT细胞),并且细胞活力降低(对于MCF-7细胞) -2-基)-2,5-二苯基溴化四氮唑鎓至其不溶的甲assay测定。结论:成功地表征了合成的水凝胶复合材料,并评估了在不同pH和温度下紫杉醇药物释放的持续释放,发现C30B / Ag填充的复合材料具有较高的控制释放率,尤其是在较低pH(pH2)和与原始样品相比,温度更高(37oC),并且具有相同的配方,具有更好的抗细菌和抗癌活性,因此制备的C30B / AgNPs水凝胶复合材料可用于药物输送,有效治疗癌症并用于抵抗细菌和癌细胞。

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