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Organ culture as a model for investigating the effects of antimetabolites and nucleoside transport inhibitors on rodent colonic mucosa
Authors:M. Moorghen  P. Ince  Karen J. Finney  A. J. Watson  A. L. Harris
Affiliation:(1) Departments of Pathology, University of Newcastle upon Tyne, NE1 4LP, United Kingdom;(2) Clinical Oncology, University of Newcastle upon Tyne, NE1 4LP, United Kingdom;(3) Present address: ICRF Clinical Oncology Unit, Churchill Hospital, 0X3 5LJ Headington, Oxford, UK
Abstract:Summary The in-vitro effects of hydroxyurea 5-FU and 5-FUdR have been extensively studied in experimental systems employing cell-line techniques. In this study we investigated the effects of these drugs on the levels of incorporation of labeled nucleosides into DNA in explants of intact rat colonic mucosa maintained in organ culture. The effects of the nucleoside transport inhibitors nitrobenzylthioinosine (NBMPR) and dipyridamole—which are modulators of antimetabolite cytotoxicity—on the incorporation of tritiated thymidine [(3H]TdR) into DNA were also studied. The incorporation of tritiated TdR into DNA was reduced by hydroxyurea but was not altered by either 5-FU or 5-FUdR. The levels of tritiated deoxyuridine were reduced by 5-FU and 5-FUdR in separate experiments; this is in keeping with thymidylate synthase inhibition. NBMPR and dipyridamole also reduced 3H-TdR incorporation into DNA. These results can be explained in terms of the known mechanisms of action of these drugs. This experimental model is therefore useful in assessing the effects of antimetabolites and nucleoside transport inhibitors in intact colonic mucosa.
Keywords:organ culture  5-FU  5-FUdR  colonic mucosa
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