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    Evaluation of P-glycoprotein modulation by pharmaceutical excipients

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    Evaluation of P-glycoprotein.pdf (166.4Kb)
    Date
    2017
    Author
    Gerber, Werner
    Hamman, Josias H.
    Steyn, Johan D.
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    Abstract
    Modulation of P-glycoprotein (P-gp) may play a significant role in the systemic delivery of poorly bioavailable drugs e.g. anti-neoplastic drugs. Many compounds from different chemical classes, including pharmaceutical excipients, have been proven to have inhibitory effects on P-gp mediated efflux transport, which leads to increased bioavailability. For the purpose of this study, different sub-classes of a group of excipients (i.e. disintegrants) were selected to evaluate the effect of ex vivo transport of a model compound across excised pig intestinal tissue. The model compound, namely Rhodamine 123 (R123), was selected on the basis that it is a known P-gp substrate. Results showed that certain of the selected disintegrants showed P-gp modulation but other disintegrants had no effect on R123 transport
    URI
    http://hdl.handle.net/10394/21489
    http://www.sapj.co.za/index.php/SAPJ/article/view/2387
    http://www.sapj.co.za/index.php/SAPJ/article/download/2387/4505
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