Department of Pharmaceutical Sciences and Drug Research, Punjabi University, Patiala, Patiala, Punjab, 147 002, India.
AAPS PharmSciTech. 2010 Jun;11(2):528-37. doi: 10.1208/s12249-010-9411-2. Epub 2010 Mar 24.
In the present study attempt was made for preparation of isotretinoin-hydroxypropyl beta cyclodextrin (HP-beta-CD) inclusion complex and encapsulate this complex in elastic liposomes to study the effect of dual carrier approach on skin targeting of isotretinoin. The isotretinoin HP-beta-CD complex was prepared by freeze-drying method and characterized by IR spectroscopy. The drug and drug-CD complex loaded elastic liposomal formulation were prepared and characterized in vitro, ex-vivo and in vivo for shape, size, entrapment efficiency, no. of vesicles per cubic mm, in vitro skin permeation and deposition study, photodegradation and skin toxicity assay. The transdermal flux for different vesicular formulations was observed between 10.5 +/- 0.5 to 13.9 +/- 1.6 microg/cm(2)/h. This is about 15-21 folds higher than that obtained from drug solution (0.7 +/- 0.1 microg/cm(2)/h) and 4-5 folds higher than obtained with drug-CD complex solution (2.7 +/- 0.1 microg/cm(2)/h). The amount of drug deposit was found to increase significantly (p < 0.05) by cyclodextrin complexation (30.1 +/- 0.1 microg). The encapsulation of this complex in elastic liposomal formulation further increases its skin deposition (262.2 +/- 21 microg). The results of skin irritation study using Draize test also showed the significant reduction in skin irritation potential of isotretinoin elastic liposomal formulation in comparison to free drug. The results of the present study demonstrated that isotretinoin elastic liposomal formulation possesses great potential for skin targeting, prolonging drug release, reduction of photodegradation, reducing skin irritation and improving topical delivery of isotretinoin.
在本研究中,我们试图制备异维 A 酸-羟丙基-β-环糊精(HP-β-CD)包合物,并将其包封于弹性脂质体中,以研究双载体给药系统对异维 A 酸经皮靶向传递的影响。采用冷冻干燥法制备异维 A 酸 HP-β-CD 包合物,并通过红外光谱对其进行表征。制备并体外、离体和体内评价了载药和载药-CD 复合物的弹性脂质体制剂的形态、粒径、包封率、立方毫米内囊泡数、体外皮肤渗透和沉积研究、光降解和皮肤毒性试验。不同囊泡制剂的经皮通量为 10.5±0.5 至 13.9±1.6μg/cm(2)/h。这大约是药物溶液(0.7±0.1μg/cm(2)/h)的 15-21 倍,是药物-CD 复合物溶液(2.7±0.1μg/cm(2)/h)的 4-5 倍。药物沉积量也显著增加(p<0.05)。将该复合物包封于弹性脂质体制剂中进一步增加了其皮肤沉积量(262.2±21μg)。使用 Draize 试验进行皮肤刺激性研究的结果也表明,与游离药物相比,异维 A 酸弹性脂质体制剂的皮肤刺激性显著降低。本研究结果表明,异维 A 酸弹性脂质体制剂具有很大的经皮靶向传递、延长药物释放、减少光降解、降低皮肤刺激性和提高异维 A 酸局部传递的潜力。