Solvent-responsive floating liquid crystalline-molecularly imprinted polymers for gastroretentive controlled drug release system

被引:36
作者
Zhang, Li-Ping [1 ]
Wang, Xiao-Lin [1 ]
Pang, Qian-Qian [1 ]
Huang, Yan-Ping [1 ]
Tang, Lei [1 ]
Chen, Meng [1 ]
Liu, Zhao-Sheng [1 ]
机构
[1] Tianjin Med Univ, Sch Pharm, Tianjin Key Lab Technol Enabling Dev Clin Therape, Tianjin 300070, Peoples R China
基金
中国国家自然科学基金;
关键词
Molecularly imprinted polymer; Liquid crystal elastomer; Floating; Gastric-retentive; Controlled release; THERAPEUTIC CONTACT-LENSES; LOW CROSS-LINKING; DELIVERY SYSTEMS; CAPILLARY ELECTROCHROMATOGRAPHY; SUSTAINED-RELEASE; ELASTOMERS; DEVICES; FABRICATION; NETWORKS; SENSORS;
D O I
10.1016/j.ijpharm.2017.09.008
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Liquid crystalline-molecularly imprinted polymer (LC-MIP) particles were first found to possess the floating behavior on the aqueous medium. Combined with molecular recognition, the LC-MIP was fabricated as a novel class of the controlled-release gastric retentive DDS. The LC-MIP was made using co-polymerization of methacrylic acid, 4-methyl phenyl dicyclohexyl ethylene (LC monomer with vinyl group), and ethylene glycol dimethacrylate with S-amlodipine (S-AML) as model template drug. The optimum condition of the preparation of LC-MIP has been obtained relying on release behaviors of S-AML from the LC-MIP. The surface morphology of LC-MIP and three corresponding control samples, i.e., template-free LC-NIP, LC-free MIP, and LC-free NIP, were studied. Applying the LF model for the binding isotherm, imprinting factors was 2.80 for the LC-MIP with the crosslinking degree of 20.0%, whereas 6.70 for the LC-free MIP with high levels of crosslinker (80.0%). Furthermore, the phase transition behaviors of LC-based particles as well as drug-loaded LC elastomers were measured by a differential scanning calorimeter and the formed hydrogen bonding between S-AML and LC-MIP was demonstrated by FT-IR spectra. In vivo imaging experiment proved that the floating LC-MIP had significantly longer gastric residence time (>60min) than the non-floating MIP reference (<30min). In vivo pharmacokinetic study showed a plateau region between 1.5 and 22h on the plasma concentration from the LC-MIP. In spite of lower imprinting factor, the relative bioavailability of the gastro-floating LC-MIP was 180.5%, whereas only 111.7% of the LC-free MIP. As a conclusion, the LC-MIPs indicated potentials for oral administration due to the innovative combination of floating and controlled release properties.
引用
收藏
页码:365 / 373
页数:9
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