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咪喹莫特乳膏皮肤毒性的削减:咪喹莫特纳米转醇质体凝胶与 5%市售乳膏在 BALB/c 小鼠的比较皮肤毒性分析。

A cutback in Imiquimod cutaneous toxicity; comparative cutaneous toxicity analysis of Imiquimod nanotransethosomal gel with 5% marketed cream on the BALB/c mice.

机构信息

Nanomedicine Research Group, Department of Pharmacy, Quaid-I-Azam University, Islamabad, 45320, Pakistan.

Department of Pharmacy, Ibadat International University, Islamabad, Pakistan.

出版信息

Sci Rep. 2022 Aug 20;12(1):14244. doi: 10.1038/s41598-022-18671-1.

DOI:10.1038/s41598-022-18671-1
PMID:35987944
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9392762/
Abstract

Herein, Imiquimod (IMQ) was incorporated in nanotransethosomes (nTES) to develop the IMQ-nTES nano-drug delivery system. IMQ-nTES was optimized using 2 factorial design. The optimized formulation was expressed with a particle size of 192.4 ± 1.60 nm, Poly-dispersibility of 0.115 ± 0.008, and IMQ percent entrapment efficiency of 91.05 ± 3.22%. Smooth and round morphology of IMQ-nTES vesicles was confirmed by TEM micrographs. Moreover, FTIR results have shown drug-excipient compatibility. The IMQ-nTES was laden inside the low molecular weight chitosan gel, which exhibited easy application, spreadability and no irritation to the applied skin. The release pattern has clearly exhibited improved dissolution properties of IMQ with the provision of the sustain release pattern. Higher IMQ content was deposited in deeper epidermis and dermis with IMQ-nTES gel, in contrast to ALDARA. In vivo, comparative toxicity study on BALB/c mice has shown significantly reduced (p < 0.001) psoriatic area severity index (PASI) score and less increment in ear thickness. Epidermal hyperplasia was an obvious finding with ALDARA which was, providentially, minimal in IMQ-nTES gel-treated skin. FTIR analysis of skin tissue has shown an enhancement of lipid and protein content in the ALDARA group, however, in the IMQ-nTES group no such change was observed. With ALDARA application, CD4 T-cells and constitutive NF-κβ expression were significantly elevated, in comparison to the IMQ-nTES gel treated group. Moreover, the adequate expression of IFN-γ and cytotoxic CD8 T-cells were suggesting the preserved IMQ efficacy with IMQ-nTES gel. Quantification of cutaneous as well as systemic inflammatory markers has also suggested the reduced psoriatic potential of IMQ-nTES gel. In essence, IMQ-nTES gel can be a suitable alternative to ALDARA owing to its better safety profile.

摘要

本文将咪喹莫特(IMQ)包封于纳米转质体(nTES)中,开发 IMQ-nTES 纳米药物递送系统。采用 2 因素设计对 IMQ-nTES 进行优化。优化后的制剂粒径为 192.4±1.60nm,多分散度为 0.115±0.008,IMQ 包封效率为 91.05±3.22%。TEM 显微照片证实了 IMQ-nTES 囊泡的光滑圆形形态。此外,FTIR 结果表明药物-赋形剂具有相容性。IMQ-nTES 载入低分子量壳聚糖凝胶中,该凝胶具有易于应用、铺展性和对应用皮肤无刺激性。释放模式清楚地表明,提供了持续释放模式,改善了 IMQ 的溶解性能。与 ALDARA 相比,IMQ-nTES 凝胶在更深的表皮和真皮中沉积了更高的 IMQ 含量。体内 BALB/c 小鼠比较毒性研究表明,银屑病面积严重度指数(PASI)评分显著降低(p<0.001),耳厚度增加较少。ALDARA 会导致表皮过度增生,而在 IMQ-nTES 凝胶处理的皮肤中则很少见。皮肤组织的 FTIR 分析表明,ALDARA 组的脂质和蛋白质含量增加,而 IMQ-nTES 组则没有这种变化。与 IMQ-nTES 凝胶处理组相比,ALDARA 组的 CD4 T 细胞和组成型 NF-κβ表达显著升高。此外,IFN-γ 和细胞毒性 CD8 T 细胞的充分表达表明,IMQ-nTES 凝胶保留了 IMQ 的疗效。皮肤和全身炎症标志物的定量也表明,IMQ-nTES 凝胶降低了银屑病的潜力。总之,由于其更好的安全性,IMQ-nTES 凝胶可以成为 ALDARA 的合适替代品。

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