Complete <i>in vivo</i> reversal of P‐glycoprotein pump function in the blood‐brain barrier visualized with positron emission tomography

Hendrikse, N. Harry; Schinkel, AH; Vries, Elisabeth G.E. de; Fluks, E; Graaf, Winette T.A. van der; Willemsen, Antoon T. M.; Vaalburg, W; Franssen, Eric J. F.

doi:10.1038/sj.bjp.0701979

Cited by 170 publications

(128 citation statements)

References 28 publications

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“…Western blot analysis performed in spinal cord homogenates of SOD1-G93A mice showed that immunoreactivity for P-gp remarkably increased during progression of the disease compared to age-matched SOD1-wild type mice (Fig.6 upper and lower panels) or even nontransgenic mice (not shown), suggesting that these drug efflux transporters are markedly upregulated in the ALS mice. We also found that similar to Verapamil, a known substrate for Pgp (Langer et al, 2007;Hendrikse et al, 1998), NDGA modulates the activity of P-gp in isolated membrane vesicles (Table 1) (Seelig, 1998). Although this assay does not provide direct evidence that NDGA can be transported by P-gp, the modulation of P-gp activity strongly indicated that NDGA could serve as substrate for this transporter (Garrigues et al, 2002).…”

Section: Increased Expression Levels Of P-glycoprotein Transporters Imentioning

confidence: 83%

“…It is therefore likely that the lack or loss of the NDGA efficacy in these mice could be consequential to its increased extrusion from the CNS, and the spinal cord in particular, due to the increased expression levels of P-gp proteins. The membrane assay we employed showed that NDGA interacts with P-gp as strongly as another known transported substrate structurally similar, verapamil (Langer et al, 2007;Hendrikse et al, 1998), suggesting that NDGA could be a substrate for these drug efflux transporters. This assay cannot accurately answer the question whether the tested compound that interacts with P-gp could also be a substrate for the drug transporter.…”

Section: Discussionmentioning

confidence: 99%

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Nordihydroguaiaretic acid increases glutamate uptake in vitro and in vivo: Therapeutic implications for amyotrophic lateral sclerosis

Boston-Howes¹,

Williams²,

Bogush³

et al. 2008

Experimental Neurology

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Synaptic accumulation of glutamate causes neuronal death in many neurodegenerative pathologies such as amyotrophic lateral sclerosis. Drugs capable of increasing glutamate uptake could therefore be therapeutically effective. We screened in a cell-based assay a library of 1040 FDA-approved drugs and nutrients for compounds that could enhance glutamate uptake. Nordihydroguaiaretic acid (NDGA), an anti-inflammatory drug that inhibits lipoxygensases, potently enhanced glutamate uptake in MN-1 cells. Given subcutaneously at 1 mg/day for 30 days in mice, NDGA increased glutamate uptake in spinal cord synaptosomes persistently throughout the treatment. However, when administered following the same regimen to the SOD1-G93A transgenic mouse model of ALS at disease onset, NDGA did not extend survival of these mice. We found that NDGA failed to sustain increased glutamate uptake in the SOD1-G93A mice despite an initial upregulation measured during the first 10 days of treatment. SOD1-G93A mice displayed a progressive increase in spinal cord expression levels of the efflux transporter P-glycoprotein beginning at disease onset. This increase was not a specific consequence of the NDGA treatment as we have measured it in untreated SOD1-G93A mice. Because P-glycoproteins control the extrusion of a broad range of toxins and xenobiotics and are responsible for drug resistance in many diseases including cancer and brain diseases such as epilepsy, we propose that the failure of NDGA in maintaining glutamate uptake upregulated in SOD1-G93A mice and its therapeutic inefficacy are due to acquired pharmacoresistance mediated by the increased expression of P-glycoprotein.

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Section: Increased Expression Levels Of P-glycoprotein Transporters Imentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

Nordihydroguaiaretic acid increases glutamate uptake in vitro and in vivo: Therapeutic implications for amyotrophic lateral sclerosis

Boston-Howes¹,

Williams²,

Bogush³

et al. 2008

Experimental Neurology

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“…11 C]verapamil as P-gp substrate in patients (Hendrikse et al, 1998(Hendrikse et al, , 1999Bart et al, 2003Bart et al, , 2005Syvanen et al, 2006;Takano et al, 2006). Future studies should elucidate if these results can be extrapolated to the human setting.…”

Section: Discussionmentioning

confidence: 99%

“…At present the concept of efflux pump inhibition is most frequently studied for P-gp. Studies in rodents have shown that P-gp function can be inhibited with cyclosporin A (CsA) (Hendrikse et al, 1998(Hendrikse et al, , 1999Syvanen et al, 2006). To circumvent toxic side effects of CsA in patients, therapies that influence P-gp function could be utilised, such as radiotherapy.…”

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confidence: 99%

Irradiation of rat brain reduces P-glycoprotein expression and function

et al. 2007

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The blood -brain barrier (BBB) hampers delivery of several drugs including chemotherapeutics to the brain. The drug efflux pump P-glycoprotein (P-gp), expressed on brain capillary endothelial cells, is part of the BBB. P-gp expression on capillary endothelium decreases 5 days after brain irradiation, which may reduce P-gp function and increase brain levels of P-gp substrates. To elucidate whether radiation therapy reduces P-gp expression and function in the brain, right hemispheres of rats were irradiated with single doses of 2 -25 Gy followed by 10 mg kg À1 of the P-gp substrate cyclosporine A (CsA) intravenously (i.v.), with once 15 Gy followed by CsA (10, 15 or 20 mg kg À1 ), or with fractionated irradiation (4 Â 5 Gy) followed by CsA (10 mg kg À1 ) 5 days later. Additionally, four groups of three rats received 25 Gy once and were killed 10, 15, 20 or 25 days later. The brains were removed and P-gp detected immunohistochemically. P-gp function was assessed by [ 11 C]carvedilol uptake using quantitative autoradiography. Irradiation increased [11 C]carvedilol uptake dose-dependently, to a maximum of 20% above non irradiated hemisphere. CsA increased [ 11 C]carvedilol uptake dose-dependently in both hemispheres, but more (Po0.001) in the irradiated hemisphere. Fractionated irradiation resulted in a lost P-gp expression 10 days after start irradiation, which coincided with increased [ 11 C]carvedilol uptake. P-gp expression decreased between day 15 and 20 after single dose irradiation, and increased again thereafter. Rat brain irradiation results in a temporary decreased P-gp function.

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“…Verapamil and cyclosporine are often used as P-gp inhibitors. However, these agents are also substrates of P-gp and inhibit P-gp activity in a competitive manner, 26,27 suggesting that the degree of inhibition of P-gp depends on the concentration ratio of inhibitors and substrates. The concentrations of these inhibitors required to inhibit P-gp-dependent transport of local anesthetics are unknown, since no data are available regarding the inhibition constants of these inhibitors.…”

Section: Measurement Of Lidocaine Megx and Bupivacaine In Plasma Andmentioning

confidence: 99%

The P-glycoprotein inhibitor quinidine decreases the threshold for bupivacaine-induced, but not lidocaine-induced, convulsions in rats

Funao

Oda

Tanaka

et al. 2003

Can J Anesth/J Can Anesth

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P Pu ur rp po os se e: : To examine whether inhibition of P-glycoprotein (P-gp) activity by quinidine affects the central nervous system toxicity of lidocaine and racemic bupivacaine (bupivacaine).M Me et th ho od ds s: : Forty male Sprague-Dawley rats were randomly divided into four groups (n = 10). Fifteen minutes following administration of 15 mg·kg ) was infused until convulsions occurred. Concentrations of lidocaine and its primary metabolite, monoethylglycinexylidide (MEGX) and bupivacaine in plasma and in the brain at the onset of convulsions were measured by high-performance liquid chromatography.R Re es su ul lt ts s: : There were no differences in the dose of lidocaine required to induce convulsions between the L and QL groups. There were no differences in the concentrations of total (L = 17.2 ± 3.5, QL = 16.6 ± 2.6 µg·mL ) in plasma, total lidocaine or MEGX in the brain at the onset of convulsions between the L and QL groups. The dose of bupivacaine required to induce convulsions was comparable in the B and QB groups. At the onset of convulsions, plasma concentrations of both total (B = 4.9 ± 1.1, QB = 4.0 ± 0.6 µg·mL -1 , P = 0.03) and unbound bupivacaine (B = 1.4 ± 0.6, QB = 0.9 ± 0.2 µg·mL -1 , P = 0.02) were significantly lower in the QB group than in the B group. There were no differences in concentration of total bupivacaine in the brain between the B and QB groups.C Co on nc cl lu us si io on n: : These results suggest that quinidine inhibited P-gp activity, resulting in increased brain/plasma concentration ratio of bupivacaine, but not of lidocaine, and decreased the threshold of plasma concentration for bupivacaine-induced convulsions. (L = 17,2 ± 3,5, QL = 16,6 ± 2, ) et libre (L = 7,8 ± 2,5, QL = 7,3 ± 2, ), entre le MEGX total (L = 1,2 ± 0,5, QL = 1,3 ± 0, ) et libre (L = 0,9 ± 0,5, QL = 0,8± 0,4 (B = 4,9 ± 1,1, QB = 4,0 ± 0, , P = 0,03) et libre (B = 1,4 ± 0,6, QB = 0,9 ± 0 The P-glycoprotein inhibitor quinidine decreases the threshold for bupivacaine-induced, but not lidocaine-induced, convulsions in rats La quinidine, un inhibiteur de P-glycoprotéine, abaisse le seuil des convulsions induites par la bupivacaïne, mais non par la lidocaïne, chez les rats Objectif : Vérifier si l'inhibition de l'activité des P-glycoprotéines (P-gp

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Complete in vivo reversal of P‐glycoprotein pump function in the blood‐brain barrier visualized with positron emission tomography

Cited by 170 publications

References 28 publications

Nordihydroguaiaretic acid increases glutamate uptake in vitro and in vivo: Therapeutic implications for amyotrophic lateral sclerosis

Nordihydroguaiaretic acid increases glutamate uptake in vitro and in vivo: Therapeutic implications for amyotrophic lateral sclerosis

Irradiation of rat brain reduces P-glycoprotein expression and function

The P-glycoprotein inhibitor quinidine decreases the threshold for bupivacaine-induced, but not lidocaine-induced, convulsions in rats

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