Box Behnken Design-Enabled Development of Nanostructured Lipid Carrier Transdermal Patch for Enhancement of Bioavailability of Olmesartan Medoxomil

IF 2.7 4区医学 Q2 PHARMACOLOGY & PHARMACY Journal of Pharmaceutical Innovation Pub Date : 2022-08-22 DOI:10.1007/s12247-022-09675-5

Laxmidhar Sahoo, Goutam Kumar Jena, Chandra Sekhar Patro, Ch.Niranjan Patro, Sukanta Satapathy

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引用次数: 1

Abstract

Objective

Olmesartan medoxomil is an antihypertensive agent used for the management of hypertension but it undergoes first-pass metabolism when taken orally and bioavailability is less than 28%. This can be overcome by choosing it for topical administration by loaded with nanostructured lipid carrier (NLC) and prolonging its action.

Methods

Nanostructured lipid carrier loaded with olmesartan was prepared by high-speed hot homogenization and melt emulsification low-temperature solidification method. The formulation was composed of solid lipid, liquid lipid, surfactants, and polymers. Formulation fabrication and optimization by Box Behnken design with Design Expert software version 8.0.0. The prepared NLC formulations were studied for drug loading, entrapment efficiency, transmission electron microscopy, zeta potential, and particle size and stability study. The transdermal patch loaded with NLC containing olmesartan was fabricated and optimized.

Results

The optimized NLC formulation of olmesartan was used to fabricate it into transdermal patches. The optimized formulation (NLC F13) was found to possess particle size, zeta potential, polydispersity index, and entrapment efficiency of 284 nm, − 24.16 mV, 0.8, and 80.17%, respectively. The prepared optimized NLC-loaded transdermal patch was evaluated for weight variation, folding endurance, drug content, and drug release; the results were found as 0.074 ± 0.003, 122 ± 2.56, 92.44 ± 1.89, and 94.24 ± 0.832, respectively. In vivo pharmacokinetic study was approved by IAEC Regd. No. 926/PO/Re/S/06/CPCSEA. The study was a comparison of the pure drug (oral), drug-loaded NLC (oral), and drug-loaded NLC patch (transdermal). It was found that AUC _0–24 and AUC _0-∞ of drug-loaded NLC patch were 17.257 ng. h/mL and 34.259 ng. h/mL as compared with pure drug for oral 8.603 ng. h/mL and 16.547 ng.h/mL, respectively. The AUC _0–24 and AUC _0-∞ of drug-loaded NLC for the oral route were found at 17.857 ng. h/mL and 29.727 ng. h/mL, respectively.

Conclusion

It was found that formulation was optimized successfully and the bioavailability of the drug enhances significantly as compared to the pure drug and drug-loaded NLC for the oral route. So, optimized formulation was a promising drug delivery system for the effective treatment of hypertension.

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Box Behnken设计开发纳米结构脂质载体透皮贴剂，提高奥美沙坦美多索米的生物利用度

目的奥美沙坦美多索米是一种用于治疗高血压的降压药，但口服时存在首过代谢，生物利用度低于28%。这可以通过负载纳米结构脂质载体(NLC)并延长其作用时间来选择局部给药来克服。方法采用高速热均质和熔融乳化低温凝固法制备奥美沙坦纳米结构脂质载体。该制剂由固体脂质、液体脂质、表面活性剂和聚合物组成。Box Behnken设计与design Expert软件版本8.0.0的配方制作和优化。对制备的NLC进行了载药量、包封效率、透射电镜、zeta电位、粒径及稳定性研究。制备并优化了含奥美沙坦NLC的透皮贴片。结果优化的奥美沙坦液相色谱处方可制备奥美沙坦透皮贴剂。优化后的配方(NLC F13)粒径为284 nm, zeta电位为- 24.16 mV，多分散性指数为0.8，包封效率为80.17%。对优化后的nlc负载透皮贴片进行重量变化、折叠耐力、药物含量和药物释放度评价;结果分别为0.074±0.003、122±2.56、92.44±1.89、94.24±0.832。体内药代动力学研究已获iec926 /PO/Re/S/06/CPCSEA批准。该研究比较了纯药物(口服)、载药NLC(口服)和载药NLC贴片(透皮)。结果表明，载药NLC贴片的AUC 0- 24和AUC 0-∞分别为17.257 ng。h/mL和34.259 ng。h/mL与口服纯药8.603 ng比较。h/mL和16.547 ng.h/mL。口服给药NLC的AUC 0- 24和AUC 0-∞分别为17.857 ng。h/mL, 29.727 ng。分别h /毫升。结论经优化后，该制剂的生物利用度明显提高，与口服给药的纯药和载药NLC相比有显著提高。因此，优化制剂是一种有前景的有效治疗高血压的给药系统。

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来源期刊

Journal of Pharmaceutical Innovation PHARMACOLOGY & PHARMACY-

CiteScore

3.70

自引率

3.80%

发文量

审稿时长

>12 weeks

期刊介绍： The Journal of Pharmaceutical Innovation (JPI), is an international, multidisciplinary peer-reviewed scientific journal dedicated to publishing high quality papers emphasizing innovative research and applied technologies within the pharmaceutical and biotechnology industries. JPI''s goal is to be the premier communication vehicle for the critical body of knowledge that is needed for scientific evolution and technical innovation, from R&D to market. Topics will fall under the following categories: Materials science, Product design, Process design, optimization, automation and control, Facilities; Information management, Regulatory policy and strategy, Supply chain developments , Education and professional development, Journal of Pharmaceutical Innovation publishes four issues a year.