Exploration of docetaxel palmitate and its solid lipid nanoparticles as a novel option for alleviating the rising concern of multi-drug resistance

被引:29
作者
Kaushik, Lokesh [1 ]
Srivastava, Shubham [1 ]
Panjeta, Anshul [2 ]
Chaudhari, Dasharath [3 ]
Ghadi, Rohan [3 ]
Kuche, Kaushik [3 ]
Malik, Ruchi [1 ]
Preet, Simran [2 ]
Jain, Sanyog [3 ]
Raza, Kaisar [1 ]
机构
[1] Cent Univ Rajasthan, Sch Chem Sci & Pharm, Dept Pharm, Ajmer 305817, Rajasthan, India
[2] Panjab Univ, Dept Biophys, Chandigarh 160014, India
[3] NIPER, Ctr Pharmaceut Nanotechnol, Dept Pharmaceut, Sect 67, Mohali 160062, Punjab, India
关键词
SLNs; Pharmacokinetics; Drug conjugate; In-vivo tumor; Taxanes; Computational studies; NANO-LIPOIDAL CARRIERS; IN-VITRO; FATTY-ACIDS; CANCER; DELIVERY; CYTOTOXICITY; MICELLES; BRAIN; PHARMACOKINETICS; BIOAVAILABILITY;
D O I
10.1016/j.ijpharm.2020.119088
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Docetaxel (DTX), a widely prescribed anticancer agent, is now associated with increased instances of multidrug resistance. Also, being a problematic BCS class IV drug, it poses challenges for the formulators. Henceforth, it was envisioned to synthesize an analogue of DTX with a biocompatible lipid, i.e., palmitic acid. The in-silico studies (molecular docking and simulation) inferred lesser binding of docetaxel palmitate (DTX-PL) with P-gp vis-alpha-vis DTX and paclitaxel, indicating it to be a poor substrate for P-gp efflux. Solid lipid nanoparticles (SLNs) of the conjugate were prepared using various lipids, viz. palmitic acid, stearic acid, cetyl palmitate and glyceryl monostearate. The characterization studies for the nanocarrier were performed for the surface charge, drug payload, micromeritics, release pattern of drug and surface morphology. From the cytotoxicity assays on resistant MCF-7 cells, it was established that the new analogue offered substantially decreased IC50 to that of DTX. Further, apoptosis assay also corroborated the results obtained in IC50 determination wherein, SA-SLNs showed the highest apoptotic index than free DTX. The conjugate not only enhanced the solubility but also offered lower plasma protein binding and improved pharmacokinetic and pharmacodynamic effect for DTX loaded SA-SLNs in apt animal models, and lower affinity to P-gp efflux. The studies provide preliminary evidence and a ray of hope for a better candidate in its nano version for safer and effective cancer chemotherapy.
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页数:16
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