Dose‐dependent increase of saquinavir bioavailability by the pharmaceutic aid cremophor EL

Martin‐Facklam, Meret; Burhenne, Jürgen; Ding, Reinhard; Fricker, Ruth; Mikus, Gerd; Walter‐Sack, Ingeborg; Haefeli, Walter E.

doi:10.1046/j.1365-2125.2002.01595.x

Cited by 74 publications

(41 citation statements)

References 17 publications

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“…In in vitro experiments, polysorbate 80 was able to inhibit P-gp activity and to increase daunorubicin intracellular levels in cell cultures [112]. Polyoxyl castor oil and polysorbate 80 (substances used in drug formulations to dissolve some lipophylic and/or poorly soluble drugs, especially paclitaxel and docetaxel) were reported to increase the oral absorption of saquinavir and digoxin, respectively, through interaction with P-gp activity [113,114].…”

Section: Drug-drug Interactionsmentioning

confidence: 99%

Concise Review: Clinical Relevance of Drug–Drug and Herb–Drug Interactions Mediated by the ABC Transporter ABCB1 (MDR1, P-glycoprotein)

et al. 2007

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Key Words. P-glycoprotein • Drug interaction • Complementary and alternative medicine • CAM • Pharmacokinetics Pharmacodynamics LEARNING OBJECTIVESAfter completing this course, the reader will be able to:1. Identify important sources of variability in drug exposure caused by drug interactions mediated by P-glycoprotein.2. Describe how unwanted drug-drug interactions may lead to unexpected serious toxicity or undertreatment.3. Prevent these interactions by individualizing pharmacotherapy; this means selecting noninteracting drugs or adapting the dose of (the) interacting drug(s).Access and take the CME test online and receive 1 AMA PRA Category 1 Credit ™ at CME.TheOncologist.com CME CME ABSTRACTThe importance of P-glycoprotein (P-gp) in drug-drug interactions is increasingly being identified. P-gp has been reported to affect the pharmacokinetics of numerous structurally and pharmacologically diverse substrate drugs. Furthermore, genetic variability in the multidrug resistance 1 gene influences absorption and tissue distribution of drugs transported. Inhibition or induction of P-gp by coadministered drugs or food as well as herbal constituents may result in pharmacokinetic interactions leading to unexpected toxicities or undertreatment. On the other hand, modulation of P-gp expression and/or activity may be a useful strategy to improve the pharmacological profile of anticancer P-gp substrate drugs. In recent years, the use of complementary and alternative medicine (CAM), like herbs, food, and vitamins, by cancer patients has increased significantly. CAM use substantially increases the risk for interactions with anticancer drugs, especially because of the narrow therapeutic window of these compounds. However, for most CAMs, it is unknown whether they affect metabolizing enzymes and/or drug transporter activity. Clinically relevant interactions are reported between St John's wort or grapefruit juice and anticancer as well as nonanticancer drugs. CAM-drug interactions could explain, at least in part, the large interindividual variation in efficacy and toxicity associated with drug therapy in both cancer and noncancer patients.

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Section: Drug-drug Interactionsmentioning

confidence: 99%

Concise Review: Clinical Relevance of Drug–Drug and Herb–Drug Interactions Mediated by the ABC Transporter ABCB1 (MDR1, P-glycoprotein)

et al. 2007

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“…Intestinal Pgp has been shown to significantly reduce intestinal uptake of saquinavir in-vitro (Alsenz et al 1998;Williams & Sinko 1999) and coadministration of the selective Pgp inhibitor GF120918 resulted in significant increases in saquinavir plasma concentrations in mice (Huisman et al 2003). Martin-Facklam et al (2002) proposed that the dose-dependent increase in saquinavir bioavailability observed following co-administration of cremophor was mediated by a Pgp-mediated effect. However, at a molecular level, the comparative effects of surfactants, such as cremophor and TPGS, on intestinal cells and Pgp-functionality is far from clear, with evidence reported of diverse functionality between surfactants on cell surface membranes or transporters (Rege et al 2001;Bogman et al 2003;Cornaire et al 2004).…”

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A comparison of intestinal lymphatic transport and systemic bioavailability of saquinavir from three lipid-based formulations in the anaesthetised rat model

Griffin

O’Driscoll

2006

Journal of Pharmacy and Pharmacology

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Saquinavir is a lipophilic, poorly water-soluble HIV protease inhibitor that undergoes extensive firstpass metabolism and exhibits poor oral bioavailability. Redirection of the absorption pathway of anti-HIV compounds from the portal blood to the HIV-rich intestinal lymphatics may enhance therapeutic efficacy and reduce the extent of the first-pass effect. This study investigates the potential of targeted intestinal lymphatic transport of saquinavir via a lipid formulation approach. Three formulations containing oleic acid were examined: cremophor-oleic acid mixed micelles, D-alpha tocopheryl polyethylene glycol 1000 succinate (TPGS)-oleic acid mixed micelles and an oleic acid microemulsion. The mesenteric lymph duct cannulated anaesthetised rat model was employed. Plasma and lymph samples were analysed by HPLC. Lymph triglyceride was measured using an enzymatic colorimetric technique. The extent of lymphatic transport from the lipid vehicles was 0.025-0.05% of the dose administered. The microemulsion produced higher and more prolonged mesenteric lymph concentrations than the micellar formulations. A strong correlation existed between the concentration of saquinavir in intestinal lymph and lymph triglyceride levels. The systemic bioavailability was estimated to be 8.5% and 4.8% for the cremophor mixed micelle and the microemulsion, respectively. The cremophor mixed micelles produced higher bioavailability than TPGS mixed micelles, implying that the nature of the surfactant can influence the distribution of drug between lymph and plasma.

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“…Lo (2003) reported that Tween 20 markedly enhanced the intracellular accumulation of epirubicin in Caco-2 cells and enhanced mucosal-to-serosal absorption of epirubicin in the rat jejunum and ileum. Previous reports suggest that coadministration of excipients enhanced oral absorption of P-gp substrates not only because of improved solubilization of drugs, but also inhibition of P-gp-mediated efflux (Yu et al, 1999;Martin-Facklam et al, 2002;Varma and Panchagnula, 2005). These excipients are commonly used in human pharmaceutical formulations and are considered safe and relatively nontoxic.…”

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confidence: 99%

Improvement of the Oral Drug Absorption of Topotecan through the Inhibition of Intestinal Xenobiotic Efflux Transporter, Breast Cancer Resistance Protein, by Excipients

Yamagata¹,

Kusuhara²,

Morishita³

et al. 2007

Drug Metab Dispos

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ABSTRACT:Recently, breast cancer resistance protein (BCRP/ABCG2) has been shown to limit the oral absorption of its substrates in the intestine. The purpose of this study was to examine whether excipients can be used as inhibitors of BCRP, to improve the oral drug absorption of BCRP substrates. In wild-type mice, Pluronic P85 and Tween 20, given orally 15 min before topotecan administration, increased the area under the plasma concentration-time curve (AUC) of topotecan after oral administration (2.0-and 1.8-fold, respectively). In contrast, Pluronic P85 and Tween 20 were less effective (no significant difference) on the AUC of topotecan after oral administration in Bcrp (؊/؊) mice (1.2-and 1.2-fold, respectively). Pluronic P85 and Tween 20 given orally did not affect significantly the AUC of topotecan after intravenous administration in wild-type and Bcrp (؊/؊) mice. Moreover, we determined the mucosal-to-serosal absorptive transport of topotecan using everted mouse ileum. Pluronic P85 and Tween 20 significantly increased the intestinal absorption rate of topotecan in everted sacs from wild-type mice whereas, in everted sacs from Bcrp (؊/؊) mice, the absorption rate was 2.1-fold greater than that in wild-type mice, and these excipients were not significantly effective. There was no significant difference in the intestinal P-glycoprotein (P-gp) expression and serosal-to-mucosal secretory transport of rhodamine 123, a typical P-gp substrate. Taken together, these results suggest that Pluronic P85 and Tween 20 can improve the oral bioavailability of BCRP substrates by inhibiting BCRP function in the small intestine.It is well known that active efflux in the intestinal epithelium by ATP-dependent multidrug efflux transporters, such as P-glycoprotein (P-gp), is one of the mechanisms limiting oral absorption of drugs, and thus, inhibition of active efflux is one of the strategies used to improve oral absorption of drugs that are pumped out from the intestinal epithelium into the lumen by efflux transporter systems (van Asperen et al., 1997;Meerum Terwogt et al., 1999). During the past two decades, several inhibitors of efflux transporters have been developed to enhance the bioavailability of their substrates (Hyafil et al., 1993;Dantzig et al., 1996;Wacher et al., 2001;Stewart et al., 2004). Although effective in animal experiments, their clinical applicability has been limited (Breedveld et al., 2006) and, consequently, more effective and safer inhibitors are needed.Excipients, such as surfactants, are extensively used in "passive" pharmaceutical formulations to improve dissolution of poorly soluble drugs. Previously, it has been found that several excipients can inhibit P-gp. Nerurkar et al. (1996) reported that Cremophor EL and Tween 80 enhanced the absorptive transport of a model peptide by inhibiting the secretory directed transport of this peptide in Caco-2 cells. Yu et al. (1999) also reported that vitamin E-TPGS (D-␣-tocopheryl polyethylene glycol succinate) inhibited the efflux system and enhanced the permea...

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Dose‐dependent increase of saquinavir bioavailability by the pharmaceutic aid cremophor EL

Cited by 74 publications

References 17 publications

Concise Review: Clinical Relevance of Drug–Drug and Herb–Drug Interactions Mediated by the ABC Transporter ABCB1 (MDR1, P-glycoprotein)

Concise Review: Clinical Relevance of Drug–Drug and Herb–Drug Interactions Mediated by the ABC Transporter ABCB1 (MDR1, P-glycoprotein)

A comparison of intestinal lymphatic transport and systemic bioavailability of saquinavir from three lipid-based formulations in the anaesthetised rat model

Improvement of the Oral Drug Absorption of Topotecan through the Inhibition of Intestinal Xenobiotic Efflux Transporter, Breast Cancer Resistance Protein, by Excipients

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