Literature DB >> 8690750

Modulation of multidrug resistance with dexniguldipine hydrochloride (B8509-035) in the CC531 rat colon carcinoma model.

W Van de Vrie1, J H Schellens, W J Loss, H J Kolker, J Verwey, G Stoter, N M Durante, A M Eggermont.   

Abstract

The chemosensitizing potency of dexniguldipine hydrochloride (B8509-035) on epidoxorubicin was assessed in a multidrug-resistant (MDR) tumour model, the intrinsic MDR rat colon carcinoma CC531. In vitro in the sulphorhodamine B cell-viability assay the cytotoxicity of epidoxorubicin was increased approximately 15-fold by co-incubation with 50 ng/ml dexniguldipine. In vivo concentrations of dexniguldipine 5 h after a single oral dose of 30 mg/kg were 72 (+/- 19 SD) ng/ml in plasma and 925 (+/- 495 SD) ng/g in tumour tissue. Levels of the metabolite of dexniguldipine, M-1, which has the same chemosensitizing potential, were 26 (+/- 6 SD) ng/ml and 289 (+/- 127 SD) ng/g respectively. The efficacy of treatment with 6 mg/kg epidoxorubicin applied intravenously combined with 30 mg kg-1 day-1 dexniguldipine administered orally for 3 days prior to epidoxorubicin injection was evaluated on tumours grown under the renal capsule. Dexniguldipine alone did not show antitumour effects in vivo. Dexniguldipine modestly, but consistently, potentiated the tumour-growth-inhibiting effect of epidoxorubicin, reaching statistical significance in two out of four experiments. In conclusion, these experiments show that dexniguldipine has potency as an MDR reverter in vitro and in vivo in this solid MDR tumour model.

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Year:  1996        PMID: 8690750     DOI: 10.1007/bf01212879

Source DB:  PubMed          Journal:  J Cancer Res Clin Oncol        ISSN: 0171-5216            Impact factor:   4.553


  24 in total

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4.  Reversal of multidrug resistance in Friend leukemia cells by dexniguldipine-HCl.

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6.  The chemosensitizer cyclosporin A enhances the toxic side-effects of doxorubicin in the rat.

Authors:  W Van de Vrie; A M Jonker; R L Marquet; A M Eggermont
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7.  Lack of correlation between mdr-1 expression and volume-activation of cloride-currents in rat colon cancer cells.

Authors:  C De Greef; S van der Heyden; F Viana; J Eggermont; E A De Bruijn; L Raeymaekers; G Droogmans; B Nilius
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8.  The effect of dextro-, levo-, and racemic verapamil on atrioventricular conduction in humans.

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9.  Interferon treatment of a transplantable rat colon adenocarcinoma: importance of tumor site.

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10.  The activity of verapamil as a resistance modifier in vitro in drug resistant human tumour cell lines is not stereospecific.

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Journal:  Biochem Pharmacol       Date:  1990-02-15       Impact factor: 5.858

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