Synthesis and ABCG2 Inhibitory Activity of Novel Fumitremorgin C Analogs – Specificity and Structure Activity Correlations

Szolomájer-Csikós, Orsolya; Beéry, Erzsébet; Kosa, Levente; Rajnai, Zsuzsanna; Jani, Márton; Hetényi, Anasztázia; Jakab, Katalin Tauber; Krajcsi, Péter; Tóth, Gábor

doi:10.2174/1573406411309040003

Cited by 9 publications

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“…In addition, 77 was the most effective inhibitor of BCRP, with very low activity against P-gp or other known drug transporters [168,170]. In addition, the stereospecificity was shown to be very critical in the Ko family, for example, compounds having the 3S,6S,12αS configuration were 18 times more potent than those with 3S,6R,12αS configuration in inhibiting BCRP; however, this stereoselective effect was not observed in P-gp and MRP-1 [171]. 3S,6S,12αS configuration were 18 times more potent than those with 3S,6R,12αS configuration in inhibiting BCRP; however, this stereoselective effect was not observed in P-gp and MRP-1 [171].…”

Section: Fumitremorgins and Derivativesmentioning

confidence: 99%

“…In addition, the stereospecificity was shown to be very critical in the Ko family, for example, compounds having the 3S,6S,12αS configuration were 18 times more potent than those with 3S,6R,12αS configuration in inhibiting BCRP; however, this stereoselective effect was not observed in P-gp and MRP-1 [171]. 3S,6S,12αS configuration were 18 times more potent than those with 3S,6R,12αS configuration in inhibiting BCRP; however, this stereoselective effect was not observed in P-gp and MRP-1 [171]. The first synthesis of 74 was reported by Hino et al who prepared N-propyl-7-methoxy-β-carboline as the key intermediate [172].…”

Section: Fumitremorgins and Derivativesmentioning

confidence: 99%

“…The reaction was performed by the Pictet-Spengler condensation of the hydroxyethyl functionalized polystyrene resin linked L-tryptophan with excess of aldehyde Scheme 15a [163,169]. 3S,6S,12αS configuration were 18 times more potent than those with 3S,6R,12αS configuration in inhibiting BCRP; however, this stereoselective effect was not observed in P-gp and MRP-1 [171]. The first synthesis of 74 was reported by Hino et al who prepared N-propyl-7-methoxy-β-carboline as the key intermediate [172].…”

Section: Fumitremorgins and Derivativesmentioning

confidence: 99%

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Marine Natural Products as Models to Circumvent Multidrug Resistance

et al. 2016

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Multidrug resistance (MDR) to anticancer drugs is a serious health problem that in many cases leads to cancer treatment failure. The ATP binding cassette (ABC) transporter P-glycoprotein (P-gp), which leads to premature efflux of drugs from cancer cells, is often responsible for MDR. On the other hand, a strategy to search for modulators from natural products to overcome MDR had been in place during the last decades. However, Nature limits the amount of some natural products, which has led to the development of synthetic strategies to increase their availability. This review summarizes the research findings on marine natural products and derivatives, mainly alkaloids, polyoxygenated sterols, polyketides, terpenoids, diketopiperazines, and peptides, with P-gp inhibitory activity highlighting the established structure-activity relationships. The synthetic pathways for the total synthesis of the most promising members and analogs are also presented. It is expected that the data gathered during the last decades concerning their synthesis and MDR-inhibiting activities will help medicinal chemists develop potential drug candidates using marine natural products as models which can deliver new ABC transporter inhibitor scaffolds.

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Section: Fumitremorgins and Derivativesmentioning

confidence: 99%

Section: Fumitremorgins and Derivativesmentioning

confidence: 99%

Section: Fumitremorgins and Derivativesmentioning

confidence: 99%

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Marine Natural Products as Models to Circumvent Multidrug Resistance

et al. 2016

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“…propionic acid tert-butyl ester) was synthetized as published previously [19]. 1-Isobutyl-2,3,4,9-tetrahydro-1H--carboline-3-carboxylic acid acetate (internal standard, IS) was purchased from Sigma-Aldrich (Budapest, Hungary).…”

Section: Chemicals and Materialsmentioning

confidence: 99%

“…3). The basic pharmacokinetic parameters of Ko134 in mice calculated with the PKSolver 2.0 software in the noncompartmental approach [19] are listed in Table 3. As shown in (Fig.…”

Section: Pharmacokinetic Study Of Ko134 In Micementioning

confidence: 99%

Investigation of the Pharmacokinetics of the ABCG2 Transporter Inhibitor Ko134 in Mice by a Newly Developed and Validated HPLC Method

Sztojkov‐Ivanov

Szolomájer-Csikós

Márki

et al. 2014

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Transporters belonging in the ATP-binding cassette (ABC) family are crucially involved in the determination of the pharmacokinetic behavior of xenobiotics and in the development of drug resistance. The targeting of these transporters has been accepted as a rational option via which to modify the absorption or distribution of pharmaceutical agents and to combat ABC-related inefficiency. Inhibitors of the breast cancer resistance protein (BCRP/ABCG2) multidrug transporter are of interest as chemosensitizers for clinical drug resistance, for improving the pharmacokinetics of substrate chemotherapeutic drugs, and in functional assays of BCRP activity for tailoring chemotherapy. In this study, a reversephase high-performance liquid chromatographic method was developed for the determination of a simplified fumitremorgin C analog, Ko134, a potent ABCG2 inhibitor, in murine serum. The assay involves a simple sample preparation step followed by chromatographic separation on a C8 reversed-phase analytical column. The calibration plots were linear over the range 0.1 to10 μg/ml (r > 0.99). The limits of detection and quantification were 10 ng/ml and 50 ng/ml, respectively. The validation results demonstrated that the method is precise, accurate and selective for the determination of Ko134 in mouse serum. The method was successfully applied to evaluate the pharmacokinetic parameters of Ko134 after different modes of administration in mice.

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Structure and function of BCRP, a broad specificity transporter of xenobiotics and endobiotics

et al. 2014

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The discovery and characterization of breast cancer resistance protein (BCRP) as an efflux transporter conferring multidrug resistance has set off a remarkable trajectory in the understanding of its role in physiology and disease. While the relevance in drug resistance and general pharmacokinetic properties quickly became apparent, the lack of a characteristic phenotype in genetically impaired animals and humans cast doubt on the physiological importance of this ATP-binding cassette family member, similarly to fellow multidrug transporters, despite well-known endogenous substrates. Later, high-performance genetic analyses and fine resolution tissue expression data forayed into unexpected territories concerning BCRP relevance, and ultimately, the rise of quantitative proteomics allows putting observed interactions into absolute frameworks for modeling and insight into interindividual and species differences. This overview summarizes existing knowledge on the BCRP transporter on molecular, tissue and system level, both in physiology and disease, and describes a selection of experimental procedures that are the most widely applied for the identification and characterization of substrate and inhibitor-type interactions.

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Synthesis and ABCG2 Inhibitory Activity of Novel Fumitremorgin C Analogs – Specificity and Structure Activity Correlations

Cited by 9 publications

References 0 publications

Marine Natural Products as Models to Circumvent Multidrug Resistance

Marine Natural Products as Models to Circumvent Multidrug Resistance

Investigation of the Pharmacokinetics of the ABCG2 Transporter Inhibitor Ko134 in Mice by a Newly Developed and Validated HPLC Method

Structure and function of BCRP, a broad specificity transporter of xenobiotics and endobiotics

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