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Drug delivery diffusion-controlled release

Shah SS, Cha Y, Pitt CG. Poly(glycolic acid-co-dl lactic acid) diffusion or degradation controlled drug delivery J Controlled Release 1992 18 261-270. [Pg.27]

Figure 1. Mechanisms of controlled release drug delivery. Diffusion-controlled (A), dissolution-controlled (B), osmoticSly controlled (C), ion-exchange controlled (D), and degradation-controlled (polymeric prodnig, E) systems. Figure 1. Mechanisms of controlled release drug delivery. Diffusion-controlled (A), dissolution-controlled (B), osmoticSly controlled (C), ion-exchange controlled (D), and degradation-controlled (polymeric prodnig, E) systems.
Shah, S. S., Cha, Y., and Pitt, C. G., 1992, Poly(glycolic acid-co-DL-lactic acid) Diffusion or degradation controlled drug delivery , J. Controlled Release 18 261-270. [Pg.166]

Because PCL hydrolyzes slowly compared to PLA and PLGA, it is most suitable for long-term drug delivery. Capronor , a 1-year contraceptive represents such a system [106]. The release of drugs is diffusion controlled rather than erosion controlled [106]. Nitrofurantoin, an antibacterial agent used in the treatment of urinary tract infections, has been incorporated into PCL microspheres [ 105]. The drug release rate was proportional to the square-root of time, i.e., fol-... [Pg.84]

Levamisole, cimetidine, and chloramphenicol were used as model drugs. A comparative study on the dependence on the pH value of the release of cimetidine, levamisole, and chloramphenicol from the gel was reported [144]. The results reveal that the drug delivery is controlled by diffusion and relaxation processes, while the diffusion coefficient and relaxation time are highly dependent on the pH of the medium. Moreover, the drug solubility in water obviously has an influence on the release [ 144]. [Pg.69]

Among drug delivery systems, those based on a diffusion-controlled release through a polymeric membrane appear to be the most reliable in order to achieve a zero-order release. ... [Pg.179]

Ethylene vinyl acetate has also found major applications in drug delivery. These copolymers used in drug release normally contain 30-50 wt% of vinyl acetate. They have been commercialized by the Alza Corporation for the delivery of pilocarpine over a one-week period (Ocusert) and the delivery of progesterone for over one year in the form of an intrauterine device (Progestasert). Ethylene vinyl acetate has also been evaluated for the release of macromolecules such as proteins. The release of proteins form these polymers is by a porous diffusion and the pore structure can be used to control the rate of release (3). Similar nonbiodegradable polymers such as the polyurethanes, polyethylenes, polytetrafluoroethylene and poly(methyl methacrylate) have also been used to deliver a variety of different pharmaceutical agents usually as implants or removal devices. [Pg.26]

In the pharmaceutical sciences, diffusion processes are central to drug delivery. They are particularly important in the release of drugs from controlled-... [Pg.31]


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See also in sourсe #XX -- [ Pg.485 ]




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Control delivery

Controlled delivery

Controlled drug release

Controlled release

Controlled-release drug delivery

Diffusion control

Diffusion controlled

Diffusion drug delivery

Drug delivery controlled

Drug delivery diffusion-controlled

Drug diffusion

Drug diffusivity

Drug release

Drug release control

Drug release diffusion control

Release diffusion-controlled

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