Nanostructured Lipid Carrier-Based Codelivery of Raloxifene and Naringin: Formulation, Optimization, In Vitro, Ex Vivo, In Vivo Assessment, and Acute Toxicity Studies

被引:46
作者
Alhalmi, Abdulsalam [1 ]
Amin, Saima [1 ]
Khan, Zafar [1 ]
Beg, Sarwar [2 ]
Al Kamaly, Omkulthom [3 ]
Saleh, Asmaa [3 ]
Kohli, Kanchan [1 ,4 ]
机构
[1] Jamia Hamdard, Dept Pharmaceut, Sch Pharmaceut Educ & Res, New Delhi 110062, India
[2] Univ Cent Lancashire, Sch Pharm & Biomed Sci, Flyde Rd, Preston PR1 2HE, Lancs, England
[3] Princess Nourah Bint Abdulrahman Univ, Coll Pharm, Dept Pharmaceut Sci, POB 84428, Riyadh 11671, Saudi Arabia
[4] Lloyd Inst Management & Technol Pharm, Plot 11,Knowledge Pk 2, Greater Noida 201308, India
关键词
raloxifene; naringin; acute toxicity study; combination; nanostructured lipid carriers; central composite design; breast cancer; TAMOXIFEN CITRATE/COENZYME Q10; DRUG-DELIVERY; NANOPARTICLES; ABSORPTION; CYTOTOXICITY; NANOCARRIERS; RESVERATROL; ANTIOXIDANT; INHIBITION; EXCIPIENTS;
D O I
10.3390/pharmaceutics14091771
中图分类号
R9 [药学];
学科分类号
100702 [药剂学];
摘要
This work aimed to develop dual drug-loaded nanostructured lipid carriers of raloxifene and naringin (RLX/NRG NLCs) for breast cancer. RLX/NRG NLCs were prepared using Compritol 888 ATO and oleic acid using a hot homogenization-sonication method and optimized using central composite design (CCD). The optimized RLX/NRG NLCs were characterized and evaluated using multiple technological means. The optimized RLX/NRG NLCs exhibited a particle size of 137.12 nm, polydispersity index (PDI) of 0.266, zeta potential (ZP) of 25.9 mV, and entrapment efficiency (EE) of 91.05% (raloxifene) and 85.07% (naringin), respectively. In vitro release (81 +/- 2.2% from RLX/NRG NLCs and 31 +/- 1.9% from the RLX/NRG suspension for RLX and 93 +/- 1.5% from RLX/NRG NLCs and 38 +/- 2.01% from the RLX/NRG suspension for NRG within 24 h). Concurrently, an ex vivo permeation study exhibited nearly 2.3 and 2.1-fold improvement in the permeability profiles of RLX and NRG from RLX/NRG NLCs vis-a-vis the RLX/NRG suspension. The depth of permeation was proved with CLSM images which revealed significant permeation of the drug from the RLX/NRG NLCs formulation, 3.5-fold across the intestine, as compared with the RLX/NRG suspension. An in vitro DPPH antioxidant study displayed a better antioxidant potential of RLX/NRG in comparison to RLX and NRG alone due to the synergistic antioxidant effect of RLX and NRG. An acute toxicity study in Wistar rats showed the safety profile of the prepared nanoformulations and their excipients. Our findings shed new light on how poorly soluble and poorly permeable medicines can be codelivered using NLCs in an oral nanoformulation to improve their medicinal performance.
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页数:27
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