ZERO-ORDER DRUG-RELEASE FROM HYDROCOLLOID MATRICES

被引:156
作者
MOCKEL, JE
LIPPOLD, BC
机构
[1] HEINRICK HEINE UNIV,INST PHARMACEUT TECHNOL,UNIV STR 1,W-4000 DUSSELDORF 1,GERMANY
[2] BOEHRINGER MANNHEIM GMBH,GALENICAL DEV,W-6800 MANNHEIM 31,GERMANY
关键词
HYDROCOLLOID MATRIX; ZERO-ORDER RELEASE; EROSION; POLYMER DISSOLUTION; RELAXATION;
D O I
10.1023/A:1018931210396
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Matrices are manufactured by direct compression of a powder mixture of a polymer, e.g., methylhydroxypropyl cellulose (MHPC) or polyvinylalcohol (PVAI), and a drug. The following factors that can influence the drug release mode were investigated at constant surface: (i) polymer solution viscosity, glass transition temperature, and swelling; (ii) drug concentration in the matrix and solubility; and (iii) conditions of release experiment (hydrodynamics). In the case of zero-order release profiles (hydrocolloids with low viscosities), only the dissolution of the polymer appears to control the drug release rate. Factors accelerating polymer dissolution resulted in higher release rates. Comparison of swollen and dry hydrocolloid matrices shows that the duration and kinetics of drug release were not controlled by the swelling front moving into the dry polymer, and water penetration and relaxation were not rate controlling. Therefore, the glass transition temperature had no effect on drug release from these hydrocolloids. The higher the hydrodynamic stress exerted on the eroding hydrocolloid, the faster the resulting drug release as a result of accelerated polymer dissolution. With hydrocolloids of very high viscosity the polymer dissolution is slow, and drug relese from the swollen gel appears to be controlled by diffusion according to kinetics of the Higuchi type.
引用
收藏
页码:1066 / 1070
页数:5
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