Regulation and expression of multidrug resistance (MDR) transcripts in the intestinal epithelium

Li, M; Hurren, Rose; Zastawny, Roman L.; Ling, Victor; Buick, Roger

doi:10.1038/sj.bjc.6690475

Cited by 18 publications

(13 citation statements)

References 55 publications

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“…Mdr1b mRNA, however, was relatively evenly expressed in different intestinal parts and at a lower level as compared with the mdr1a isoform. This is consistent with previously published data on intestinal Pgp expression (Fricker et al, 1996;Li et al, 1999;Brady et al, 2002;Mouly and Paine, 2003).…”

Section: Abc Transporter Profile In Selected Intestinalsupporting

confidence: 93%

Closing the Gaps: A Full Scan of the Intestinal Expression of P-Glycoprotein, Breast Cancer Resistance Protein, and Multidrug Resistance-Associated Protein 2 in Male and Female Rats

MacLean

Moenning²,

Reichel³

et al. 2008

Drug Metab Dispos

132

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ABSTRACT:Intestinal ATP binding cassette (ABC) transporters may affect the bioavailability and effectiveness of orally administered drugs. Available studies on regional expression of intestinal efflux transporters were done with selected intestinal segments only and inconsistent with regard to the variability of transporter expression and the course of expression along the intestine. For an evaluation of the consistency between mRNA and protein expression, relative expression levels of P-glycoprotein (Pgp; ABCB1), breast cancer resistance protein (Bcrp; ABCG2), and multidrug resistance-associated protein (Mrp) 2 (ABCC2) were determined using quantitative real-timepolymerase chain reaction and Western blot in rat intestinal segments from duodenum, jejunum, ileum, and colon. In addition, the protein expression of Pgp, Bcrp, and Mrp2 from the entire rat intestine was studied by a complete 3-cm segmentation to evaluate the predictive power of expression analyses from selected intestinal segments. Pgp showed an increase from proximal to distal regions, Bcrp showed an arcuate pattern with highest expression toward the end of small intestine, and Mrp2 decreased along the intestinal axis from proximal to distal parts. No gender specific differences could be observed. Regarding the concordance of mRNA and protein expression, Pgp and Bcrp mRNA samples allow good estimations about the corresponding protein expression (for Pgp limited to the mdr1a isoform), but for Mrp2, pronounced deviation could be observed. All transporters showed considerable intra-and interindividual variability, especially at the protein level, making it problematic to take transporter expressions of small sections exemplary for general assumptions on intestinal abundances.

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Section: Abc Transporter Profile In Selected Intestinalsupporting

confidence: 93%

Closing the Gaps: A Full Scan of the Intestinal Expression of P-Glycoprotein, Breast Cancer Resistance Protein, and Multidrug Resistance-Associated Protein 2 in Male and Female Rats

MacLean

Moenning²,

Reichel³

et al. 2008

Drug Metab Dispos

132

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“…IEC-6 and IEC-18 cell lines have been used extensively in mechanistic studies of the intestinal epithelial lining as well and may represent useful tools for nanoparticle research [127-129]. These cells have been used to measure the activation of various signal pathways after toxicant exposure, as well as cytokine and ROS/RNS release [130,131].…”

Section: 0 Elements Of a Screening Strategy For Nanomaterialsmentioning

confidence: 99%

Principles for characterizing the potential human health effects from exposure to nanomaterials: elements of a screening strategy

et al. 2005

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The rapid proliferation of many different engineered nanomaterials (defined as materials designed and produced to have structural features with at least one dimension of 100 nanometers or less) presents a dilemma to regulators regarding hazard identification. The International Life Sciences Institute Research Foundation/Risk Science Institute convened an expert working group to develop a screening strategy for the hazard identification of engineered nanomaterials. The working group report presents the elements of a screening strategy rather than a detailed testing protocol. Based on an evaluation of the limited data currently available, the report presents a broad data gathering strategy applicable to this early stage in the development of a risk assessment process for

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“…(n ϭ 8 -10). intestine, the Mdr1a-mediated talinolol transport was further studied (Li et al, 1999;Takara et al, 2003). Inhibitory Effect of Naringin on MDR1-and Mdr1a-Mediated Transport of Talinolol.…”

Section: Transcellular Transport Of Talinolol In Llc-pk1/ Mdr1 Llc-pmentioning

confidence: 99%

Species Difference in the Effect of Grapefruit Juice on Intestinal Absorption of Talinolol between Human and Rat

Shirasaka

Kuraoka²,

Spahn‐Langguth³

et al. 2009

J Pharmacol Exp Ther

116

101

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Bioavailability of talinolol, a ␤ 1 -adrenergic receptor antagonist, was enhanced by coadministration with grapefruit juice (GFJ) in rats, whereas GFJ ingestion markedly reduced the absorption of talinolol in humans. Because our recent study indicated that the inhibitory effect of GFJ on organic anion-transporting polypeptide (Oatp)-and P-gp-mediated talinolol absorption depends on the concentration of naringin in ingested GFJ, the apparent inconsistent findings may be explained by the species difference in the affinity of naringin for OATP/Oatp and P-gp multidrug resistance 1 (MDR1/Mdr1) between humans and rats. Although human MDR1-mediated talinolol transport was not inhibited by 2000 M naringin, naringin inhibited human OATP1A2-, rat Oatp1a5-, and rat Mdr1a-mediated talinolol transport with IC 50 values of 343, 12.7, and 604 M, respectively, in LLC-PK1 cell and Xenopus laevis oocyte systems.Because the naringin concentration in commercially prepared GFJ was found to be approximately 1200 M, these results suggested that GFJ would reduce the intestinal absorption of talinolol through inhibition of OATP1A2-mediated talinolol uptake in humans, whereas an increase of talinolol absorption is mainly through inhibition of Mdr1a-mediated efflux in rats. The rat intestinal permeability of talinolol measured by the in situ closed loop method was indeed significantly increased in the presence of GFJ, whereas a significant decrease was observed with 6-fold diluted GFJ, in which the naringin concentration was approximately 200 M. The present study indicated that the species difference in the effect of GFJ on intestinal absorption of talinolol between humans and rats may be due to differences in the affinity of naringin for OATP/Oatp and MDR1/Mdr1 transporters between the two species.

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Regulation and expression of multidrug resistance (MDR) transcripts in the intestinal epithelium

Cited by 18 publications

References 55 publications

Closing the Gaps: A Full Scan of the Intestinal Expression of P-Glycoprotein, Breast Cancer Resistance Protein, and Multidrug Resistance-Associated Protein 2 in Male and Female Rats

Closing the Gaps: A Full Scan of the Intestinal Expression of P-Glycoprotein, Breast Cancer Resistance Protein, and Multidrug Resistance-Associated Protein 2 in Male and Female Rats

Principles for characterizing the potential human health effects from exposure to nanomaterials: elements of a screening strategy

Species Difference in the Effect of Grapefruit Juice on Intestinal Absorption of Talinolol between Human and Rat

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