Multidrug Resistance Protein (MRP) 1 and MRP3 Attenuate Cytotoxic and Transactivating Effects of the Cyclopentenone Prostaglandin, 15-Deoxy-Δ<sup>12,14</sup>Prostaglandin J<sub>2</sub> in MCF7 Breast Cancer Cells

Paumi, Christian M.; Wright, Marcus W.; Townsend, Alan J.; Morrow, Charles S.

doi:10.1021/bi027347u

Cited by 69 publications

(88 citation statements)

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“…Media containing viral particles was collected from above the cells and used to transduce MCF7/WT cells. Transduced cells were grown under G418 selection, and clones were selected and analyzed for MRP1 expression via Western blotting as described previously (Paumi et al, 2003). At least two clones for each mutation were analyzed in cytotoxicity, transport, and doxorubicin accumulation assays that yielded similar results.…”

Section: Methodsmentioning

confidence: 99%

“…Cell lysates were then placed in a new tube containing 50 l of 6ϫ SDS-PAGE loading buffer and frozen at Ϫ20°C. Frozen samples were later thawed and incubated at 37°C for 1 h; 70 l of each sample was run on a 7% SDS-PAGE gel followed by Western blotting procedure as described previously (Paumi et al, 2003). MRP1 protein was probed with rat MRP1r1 antibody (1:1000).…”

Section: Methodsmentioning

confidence: 99%

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Casein Kinase 2α Regulates Multidrug Resistance-Associated Protein 1 Function via Phosphorylation of Thr249

et al. 2012

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We have shown previously that the function of Ycf1p, yeast ortholog of multidrug resistance-associated protein 1 (MRP1), is regulated by yeast casein kinase 2␣ (Cka1p) via phosphorylation at Ser251. In this study, we explored whether casein kinase 2␣ (CK2␣), the human homolog of Cka1p, regulates MRP1 by phosphorylation at the semiconserved site Thr249. Knockdown of CK2␣ in MCF7-derived cells expressing MRP1 [MRP1 CK2␣(Ϫ)] resulted in increased doxorubicin sensitivity. MRP1-dependent transport of leukotriene C 4 and estradiol-17␤-D-glucuronide into vesicles derived from MRP1 CK2␣(Ϫ) cells was decreased compared with MRP1 vesicles. Moreover, mutation of Thr249 to alanine (MRP1-T249A) also resulted in decreased MRP1-dependent transport, whereas a phosphomimicking mutation (MRP1-T249E) led to dramatic increase in MRP1-dependent transport. Studies in tissue culture confirmed these findings, showing increased intracellular doxorubicin accumulation in MRP1 CK2␣(Ϫ) and MRP1-T249A cells compared with MRP1 cells. Inhibition of CK2 kinase by 2-dimethylamino-4,5,6,7-tetrabromo-1H-benzimidazole resulted in increased doxorubicin accumulation in MRP1 cells, but not in MRP1 CK2␣(Ϫ), MRP1-T249A, or MRP1-T249E cells, suggesting that CK2␣ regulates MRP1 function via phosphorylation of Thr249. Indeed, CK2␣ and MRP1 interact physically, and recombinant CK2 phosphorylates MRP1-derived peptide in vitro in a Thr249-dependent manner, whereas knockdown of CK2␣ results in decreased phosphorylation at MRP1-Thr249. The role of CK2 in regulating MRP1 was confirmed in other cancer cell lines where CK2 inhibition decreased MRP1-mediated efflux of doxorubicin and increased doxorubicin cytotoxicity. This study supports a model in which CK2␣ potentiates MRP1 function via direct phosphorylation of Thr249.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Casein Kinase 2α Regulates Multidrug Resistance-Associated Protein 1 Function via Phosphorylation of Thr249

et al. 2012

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“…p-Aminohippuric acid [92] 372 Bilirubin biglucuronide [93] 0.8 a Daunorubicin [94,95] 1.4 Atazanavir [59] Bilirubin bisglucuronide [93] Bilirubin monoglucuronide [93] 0.4 a Grepafloxacin [96] Benzbromarone [97,98] Bilirubin monoglucuronide [93] E217bG [99] 22 Irinotecan [100] Benzylpenicillin [98] DHEAS [101] 5 Estradiol sulfate [102] 0.4 Methotrexate [98,103,104] 930/2150 Daunorubicin [99]~8a DNP-GS [105] 3.6 E23SO417bG [99] 1.7 Doxorubicin [99]~5 0 a E217bG [99,[105][106][107] 1.5-4.8 E316bG [99] 45 Mitoxantrone [108] Flurbiprofen [109] Estrone-3-sulfate [102] 0.7/4.2 E317bG [99] 1.4 Saquinavir [110] Furosemide [98] Folic acid [103] Estrone-3-sulfate [102] 0.5 Vinblastine [111] Glibenclamide [77] Glutathione [97,112] Glycholate [99] Vincristine [95,113] Indinavir [114] Leucovorin [103] Glycolithocholate-3-sulfate [99] 1.4 Indometacin …”

Section: Substrates and Inhibitorsmentioning

confidence: 99%

Intestinal transporters for endogenic and pharmaceutical organic anions: the challenges of deriving in-vitro kinetic parameters for the prediction of clinically relevant drug–drug interactions

Grandvuinet

Vestergaard

Rapin³

et al. 2012

Journal of Pharmacy and Pharmacology

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Objectives This review provides an overview of intestinal human transporters for organic anions and stresses the need for standardization of the various in‐vitro methods presently employed in drug–drug interaction (DDI) investigations. Key findings Current knowledge on the intestinal expression of the apical sodium‐dependent bile acid transporter (ASBT), the breast cancer resistance protein (BCRP), the monocarboxylate transporters (MCT) 1, MCT3‐5, the multidrug resistance associated proteins (MRP) 1–6, the organic anion transporting polypetides (OATP) 2B1, 1A2, 3A1 and 4A1, and the organic solute transporter α/β (OSTα/β) has been covered along with an overview of their substrates and inhibitors. Furthermore, the many challenges in predicting clinically relevant DDIs from in‐vitro studies have been discussed with focus on intestinal transporters and the various methods for deducting in‐vitro parameters for transporters (Km/Ki/IC50, efflux ratio). The applicability of using a cut‐off value (estimated based on the intestinal drug concentration divided by the Ki or IC50) has also been considered. Summary A re‐evaluation of the current approaches for the prediction of DDIs is necessary when considering the involvement of other transporters than P‐glycoprotein. Moreover, the interplay between various processes that a drug is subject to in‐vivo such as translocation by several transporters and dissolution should be considered.

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“…The ATP-binding cassette (ABC) superfamily of transporters appears to be particularly important in this context, being specifically dedicated to removal of xenobiotics and toxic endogenous metabolites from the fetal organism (11,22). Although the ABC pumps were initially described as drug efflux pumps, conferring resistance to cancer cells from druginduced apoptosis (13), they have more recently been shown to be implicated in cellular protection from various proapoptotic injuries, such as exposure to endogenous toxins or hypoxic damage (10,19). Human placenta expresses several members of the ABC superfamily; of these, the most effective for drug transfer are P-glycoprotein (Pgp), encoded by the multidrug resistance 1 (MDR1) gene, multidrug resistance proteins (MRPs) 1 and 2, and the breast cancer resistance protein (BCRP; see Refs.…”

mentioning

confidence: 99%

ABC drug transporter expression and functional activity in trophoblast-like cell lines and differentiating primary trophoblast

Evseenko¹,

Paxton²,

Keelan³

2006

American Journal of Physiology-Regulatory, Integrative and Comp

150

129

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Multidrug Resistance Protein (MRP) 1 and MRP3 Attenuate Cytotoxic and Transactivating Effects of the Cyclopentenone Prostaglandin, 15-Deoxy-Δ^12,14Prostaglandin J₂ in MCF7 Breast Cancer Cells

Cited by 69 publications

References 51 publications

Casein Kinase 2α Regulates Multidrug Resistance-Associated Protein 1 Function via Phosphorylation of Thr249

Casein Kinase 2α Regulates Multidrug Resistance-Associated Protein 1 Function via Phosphorylation of Thr249

Intestinal transporters for endogenic and pharmaceutical organic anions: the challenges of deriving in-vitro kinetic parameters for the prediction of clinically relevant drug–drug interactions

ABC drug transporter expression and functional activity in trophoblast-like cell lines and differentiating primary trophoblast

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Multidrug Resistance Protein (MRP) 1 and MRP3 Attenuate Cytotoxic and Transactivating Effects of the Cyclopentenone Prostaglandin, 15-Deoxy-Δ12,14Prostaglandin J2 in MCF7 Breast Cancer Cells

Cited by 69 publications

References 51 publications

Casein Kinase 2α Regulates Multidrug Resistance-Associated Protein 1 Function via Phosphorylation of Thr249

Casein Kinase 2α Regulates Multidrug Resistance-Associated Protein 1 Function via Phosphorylation of Thr249

Intestinal transporters for endogenic and pharmaceutical organic anions: the challenges of deriving in-vitro kinetic parameters for the prediction of clinically relevant drug–drug interactions

ABC drug transporter expression and functional activity in trophoblast-like cell lines and differentiating primary trophoblast

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Resources

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Multidrug Resistance Protein (MRP) 1 and MRP3 Attenuate Cytotoxic and Transactivating Effects of the Cyclopentenone Prostaglandin, 15-Deoxy-Δ^12,14Prostaglandin J₂ in MCF7 Breast Cancer Cells