Urinary coproporphyrin <scp>I</scp>/(<scp>I</scp> + <scp>III</scp>) ratio as a surrogate for <scp>MRP2</scp> or other transporter activities involved in methotrexate clearance

Bretagne, Isabelle Benz-de; Zahr, Noël; Gouge, Amélie Le; Hulot, Jean‐Sébastien; Houillier, Caroline; Hoang-Xuân, Khê; Gyan, Emmanuel; Lissandre, Séverine; Choquet, Sylvain; Guellec, Chantal Le

doi:10.1111/bcp.12326

Cited by 16 publications

(14 citation statements)

References 66 publications

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“…Moreover, PROB is a weak inhibitor of MRP2 that is expressed on the apical surface of renal proximal tubule epithelial cells and hepatocytes. CPI and CPIII are substrates for MRP2 (Gilibili et al, 2017, Kunze et al, 2018, and the urinary CPI/(CPI + CPIII) ratio was proposed as a surrogate for MRP2 activity (Benz-de Bretagne et al, 2011, Benz-de Bretagne et al, 2014.…”

Section: Discussionmentioning

confidence: 99%

Detection of Weak Organic Anion–Transporting Polypeptide 1B Inhibition by Probenecid with Plasma-Based Coproporphyrin in Humans

et al. 2020

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Section: Discussionmentioning

confidence: 99%

Detection of Weak Organic Anion–Transporting Polypeptide 1B Inhibition by Probenecid with Plasma-Based Coproporphyrin in Humans

et al. 2020

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“…By analyzing 5 common SNPs in the ABCC2 gene, subjects with the 3972TT genotype showed a higher urinary CP ratio than those carrying the C allele. 67 These studies suggest that MRP2 may be involved in hepatobiliary excretion of CPs; however, additional in vitro and in vivo data are required to confirm this hypothesis. In summary, CP I and III could be suitable biomarkers for inhibition of OATP1B, but more in vitro and clinical data are needed to establish its sensitivity and specificity.…”

Section: Coproporhyrin I and Iiimentioning

confidence: 98%

Identification of Endogenous Biomarkers to Predict the Propensity of Drug Candidates to Cause Hepatic or Renal Transporter-Mediated Drug-Drug Interactions

Chu

Chan

Evers

2017

Journal of Pharmaceutical Sciences

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Drug transporters expressed in liver and kidney play a critical role in the elimination of a wide range of drugs and xenobiotics and inhibition of these transporters may therefore cause clinically significant drug-drug interactions (DDIs). Currently, in vitro transporter inhibition data are used to assess the risk that a drug candidate may act as an inhibitor of a transporter in patients at clinically relevant exposures. However, this approach is hampered by low confidence in in vitro to in vivo extrapolations, and large inter-system and inter-laboratory variability in in vitro data. Several endogenous compounds have been identified as substrates of drug transporters. Determining the impact of perpetrator drugs on the plasma or urinary exposure of these potential endogenous biomarkers in humans is being explored as an alternative approach to assess the DDI liability of drug candidates, especially in early drug development. In this review, we provide an overview of recently identified biomarkers used to study the inhibition of hepatic and renal transporters; summarize the methods and strategies employed to identify biomarkers; and discuss the utility, limitation, and future direction of biomarker approaches to predict transporter-mediated DDIs.

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“…Coproporphyrin I (CP-I) is one of coproporphyrin byproducts of heme biosynthesis. In the liver, CP-I is taken up into hepatocytes by organic anion-transporting polypeptide transporters and effluxed into bile likely by MRP2 (Benz-de Bretagne et al, 2011, 2014Lai et al, 2016;Shen et al, 2016). As such, a higher proportion of CP-I is secreted into the urine of subjects with Dubin-Johnson syndrome compared with normal subjects.…”

Section: Introductionmentioning

confidence: 99%

Coproporphyrin-I: A Fluorescent, Endogenous Optimal Probe Substrate for ABCC2 (MRP2) Suitable for Vesicle-Based MRP2 Inhibition Assay

et al. 2017

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Inside-out-oriented membrane vesicles are useful tools to investigate whether a compound can be an inhibitor of efflux transporters such as multidrug resistance-associated protein 2 (MRP2). However, because of technical limitations of substrate diffusion and low dynamic uptake windows for interacting drugs used in the clinic, estradiol-17-glucuronide (E17G) remains the probe substrate that is frequently used in MRP2 inhibition assays. Here we recapitulated the sigmoidal kinetics of MRP2-mediated transport of E17G, with apparent Michaelis-Menten constant () and values of 170 ±17M and 1447 ± 137 pmol/mg protein/min, respectively. The Hill coefficient (2.05 ± 0.1) suggests multiple substrate binding sites for E17G transport with cooperative interactions. Using E17G as a probe substrate, 51 of 97 compounds tested (53%) showed up to 6-fold stimulatory effects. Here, we demonstrate for the first time that coproporphyrin-I (CP-I) is a MRP2 substrate in membrane vesicles. The uptake of CP-I followed a hyperbolic relationship, adequately described by the standard Michaelis-Menten equation (apparent and values were 7.7 ± 0.7 M and 48 ± 11 pmol/mg protein/min, respectively), suggesting the involvement of a single binding site. Of the 47 compounds tested, 30 compounds were inhibitors of human MRP2 and 8 compounds (17%) stimulated MRP2-mediated CP-I transport. The stimulators were found to share the basic backbone structure of the physiologic steroids, which suggests a potential in vivo relevance of in vitro stimulation of MRP2 transport. We concluded that CP-I could be an alternative in vitro probe substrate replacing E17G for appreciating MRP2 interactions while minimizing potential false-negative results for MRP2 inhibition due to stimulatory effects.

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Urinary coproporphyrin I/(I + III) ratio as a surrogate for MRP2 or other transporter activities involved in methotrexate clearance

Cited by 16 publications

References 66 publications

Detection of Weak Organic Anion–Transporting Polypeptide 1B Inhibition by Probenecid with Plasma-Based Coproporphyrin in Humans

Detection of Weak Organic Anion–Transporting Polypeptide 1B Inhibition by Probenecid with Plasma-Based Coproporphyrin in Humans

Identification of Endogenous Biomarkers to Predict the Propensity of Drug Candidates to Cause Hepatic or Renal Transporter-Mediated Drug-Drug Interactions

Coproporphyrin-I: A Fluorescent, Endogenous Optimal Probe Substrate for ABCC2 (MRP2) Suitable for Vesicle-Based MRP2 Inhibition Assay

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