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使用载有阿霉素的阳离子脂质纳米颗粒和离子电渗疗法的局部皮肤癌治疗

Topical Skin Cancer Therapy Using Doxorubicin-Loaded Cationic Lipid Nanoparticles and lontophoresis.

作者信息

Huber Lucas A, Pereira Tatiana A, Ramos Danielle N, Rezende Lucas C D, Emery Flávio S, Sobral Lays Martin, Leopoldino Andréia Machado, Lopez Renata F V

出版信息

J Biomed Nanotechnol. 2015 Nov;11(11):1975-88. doi: 10.1166/jbn.2015.2139.

Abstract

The topical administration of chemotherapeutics is a promising approach for the treatment of skin cancer; however, different pharmaceutical strategies are required to allow large amounts of drug to penetrate tumors. This work examined the potential of the anodic iontophoresis of doxorubicin-loaded cationic solid lipid nanoparticles (DOX-SLN) to increase the distribution and tumor penetration of DOX. A double-labeled cationic DOX-SLN composed of the lipids stearic acid and monoolein and a new BODIPY dye was prepared and characterized. The skin distribution and penetration of DOX were evaluated in vitro using confocal microscopy and vertical diffusion cells, respectively. The antitumor potential was evaluated in vivo through the anodic iontophoresis of DOX-SLN in squamous cell carcinoma induced in nude BALB/c mice. The encapsulation of DOX drastically altered the DOX partition coefficient and increased the distribution of DOX in the lipid matrix of the stratum corneum (SC). The association with iontophoresis created high-concentration drug reservoir zones in the follicles of the skin. Although the iontophoresis of a DOX solution increased the penetration of DOX in the viable epidermis by approximately 4-fold, the iontophoresis of cationic DOX-SLN increased the DOX penetration by approximately 50-fold. In vivo, the DOX-SLN iontophoretic treatment was effective in inhibiting tumor cell survival and tumor growth and was accompanied by an increase in keratinization and consequent cell death. These results indicate a strong and synergic effect of iontophoresis with DOX-SLN and provide a potential strategy for the treatment of skin cancer.

摘要

化疗药物的局部给药是治疗皮肤癌的一种有前景的方法;然而,需要不同的药物策略来使大量药物渗透到肿瘤中。这项工作研究了载有阿霉素的阳离子固体脂质纳米粒(DOX-SLN)的阳极离子电渗疗法增加阿霉素分布和肿瘤渗透的潜力。制备并表征了一种由硬脂酸和单油酸甘油酯组成的双标记阳离子DOX-SLN以及一种新型BODIPY染料。分别使用共聚焦显微镜和垂直扩散池在体外评估阿霉素的皮肤分布和渗透情况。通过对裸BALB/c小鼠诱导的鳞状细胞癌进行DOX-SLN的阳极离子电渗疗法在体内评估其抗肿瘤潜力。阿霉素的包封极大地改变了阿霉素的分配系数,并增加了阿霉素在角质层(SC)脂质基质中的分布。与离子电渗疗法相结合在皮肤毛囊中形成了高浓度药物储存区。尽管阿霉素溶液的离子电渗疗法使阿霉素在活表皮中的渗透增加了约4倍,但阳离子DOX-SLN的离子电渗疗法使阿霉素的渗透增加了约50倍。在体内,DOX-SLN离子电渗疗法治疗在抑制肿瘤细胞存活和肿瘤生长方面有效,并伴有角质化增加和随之而来的细胞死亡。这些结果表明离子电渗疗法与DOX-SLN具有强大的协同作用,并为皮肤癌的治疗提供了一种潜在策略。

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