Development, In Vitro Characterization, and In Vivo Toxicity Evaluation of Chitosan-Alginate Nanoporous Carriers Loaded with Cisplatin for Lung Cancer Treatment

被引:48
作者
Alsmadi, Mo'tasem M. [1 ]
Obaidat, Rana M. [1 ]
Alnaief, Mohammad [2 ]
Albiss, Borhan Aldeen [3 ]
Hailat, Nabil [4 ]
机构
[1] Jordan Univ Sci & Technol, Fac Pharm, Dept Pharmaceut Technol, POB 3030, Irbid 22110, Jordan
[2] German Jordanian Univ, Fac Appl Med Sci, Dept Pharmaceut & Chem Engn, Amman, Jordan
[3] Jordan Univ Sci & Technol, Phys Dept, Superconduct & Magnet Measurements Lab, Irbid, Jordan
[4] Jordan Univ Sci & Technol, Fac Vet Med, Dept Pathol & Publ Hlth, Irbid, Jordan
关键词
acute and subacute toxicity; cisplatin; hybrid aerogels; supercritical fluid technology; sustained release;
D O I
10.1208/s12249-020-01735-8
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Polysaccharide-based aerogels are promising drug carriers. Being nanoporous with a high specific surface area allows their use as a drug vehicle for various delivery routes. Intratracheal and intravenous administration of free cisplatin causes toxicity in the rat liver, lungs, and kidneys. In this work, microspherical particles based on alginate-chitosan without a traditional crosslinker were evaluated for targeted delivery of cisplatin by intratracheal administration. The aerogel particles were prepared using the emulsion gelation method, followed by supercritical carbon dioxide extraction. Loading of cisplatin on the prepared porous particles was performed by impregnation using supercritical fluid technology. The prepared carrier and the loaded drug were evaluated for drug content, release, and in vivo acute and subacute toxicity. Cisplatin was successfully loaded (percent drug loading >76%) on the prepared carrier (particle size=0.4330.091 mu m) without chemically interacting with the carrier and without losing its crystal form. Sixty percent of cisplatin was released within 2 h, and the rest was loaded inside the polymer pores and had a sustained first-order release over 6 h. Loading cisplatin on the carrier developed herein reduced the cisplatin lung toxicity but increased the liver toxicity after intratracheal administration with nephrotoxicity being proportional to cisplatin dose in case of carrier-loaded cisplatin. Moreover, loading cisplatin on the carrier significantly reduced mortality rate and prevented weight loss in rats as compared to free cisplatin in subacute studies after intratracheal administration. Thus, the developed carrier showed high potential for targeted delivery of cisplatin for lung cancer treatment by inhalation.
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页数:12
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