<it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus

<it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus

<p>Abstract</p> <p>Background</p> <p>Increased functionality of efflux transporters at the blood-brain barrier may contribute to decreased drug concentrations at the target site in CNS diseases like epilepsy. In the rat, pharmacoresistant epilepsy can be mimicked by ind...

Full description

Bibliographic Details
Main Authors: Lammertsma Adriaan A, Huisman Marc C, Windhorst Albert D, Molthoff Carla FM, Luurtsema Gert, Syvänen Stina, Voskuyl Rob A, de Lange Elizabeth C
Format: Article
Language:English
Published: BMC 2011-01-01
Series:BMC Medical Imaging
Online Access:http://www.biomedcentral.com/1471-2342/11/1
id doaj-22533da4a69941199c7c9f678e2488e8
record_format Article
spelling doaj-22533da4a69941199c7c9f678e2488e82020-11-24T21:37:10ZengBMCBMC Medical Imaging1471-23422011-01-01111110.1186/1471-2342-11-1<it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticusLammertsma Adriaan AHuisman Marc CWindhorst Albert DMolthoff Carla FMLuurtsema GertSyvänen StinaVoskuyl Rob Ade Lange Elizabeth C<p>Abstract</p> <p>Background</p> <p>Increased functionality of efflux transporters at the blood-brain barrier may contribute to decreased drug concentrations at the target site in CNS diseases like epilepsy. In the rat, pharmacoresistant epilepsy can be mimicked by inducing status epilepticus by intraperitoneal injection of kainate, which leads to development of spontaneous seizures after 3 weeks to 3 months. The aim of this study was to investigate potential changes in P-glycoprotein (P-gp) expression and functionality at an early stage after induction of status epilepticus by kainate.</p> <p>Methods</p> <p><it>(R)</it>-[<sup>11</sup>C]verapamil, which is currently the most frequently used positron emission tomography (PET) ligand for determining P-gp functionality at the blood-brain barrier, was used in kainate and saline (control) treated rats, at 7 days after treatment. To investigate the effect of P-gp on <it>(R)</it>-[<sup>11</sup>C]verapamil brain distribution, both groups were studied without or with co-administration of the P-gp inhibitor tariquidar. P-gp expression was determined using immunohistochemistry in post mortem brains. <it>(R)</it>-[<sup>11</sup>C]verapamil kinetics were analyzed with approaches common in PET research (Logan analysis, and compartmental modelling of individual profiles) as well as by population mixed effects modelling (NONMEM).</p> <p>Results</p> <p>All data analysis approaches indicated only modest differences in brain distribution of <it>(R)</it>-[<sup>11</sup>C]verapamil between saline and kainate treated rats, while tariquidar treatment in both groups resulted in a more than 10-fold increase. NONMEM provided most precise parameter estimates. P-gp expression was found to be similar for kainate and saline treated rats.</p> <p>Conclusions</p> <p>P-gp expression and functionality does not seem to change at early stage after induction of anticipated pharmacoresistant epilepsy by kainate.</p> http://www.biomedcentral.com/1471-2342/11/1
collection DOAJ
language English
format Article
sources DOAJ
author Lammertsma Adriaan A
Huisman Marc C
Windhorst Albert D
Molthoff Carla FM
Luurtsema Gert
Syvänen Stina
Voskuyl Rob A
de Lange Elizabeth C
spellingShingle Lammertsma Adriaan A
Huisman Marc C
Windhorst Albert D
Molthoff Carla FM
Luurtsema Gert
Syvänen Stina
Voskuyl Rob A
de Lange Elizabeth C
<it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
BMC Medical Imaging
author_facet Lammertsma Adriaan A
Huisman Marc C
Windhorst Albert D
Molthoff Carla FM
Luurtsema Gert
Syvänen Stina
Voskuyl Rob A
de Lange Elizabeth C
author_sort Lammertsma Adriaan A
title <it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
title_short <it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
title_full <it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
title_fullStr <it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
title_full_unstemmed <it>(R)</it>-[<sup>11</sup>C]Verapamil PET studies to assess changes in P-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
title_sort <it>(r)</it>-[<sup>11</sup>c]verapamil pet studies to assess changes in p-glycoprotein expression and functionality in rat blood-brain barrier after exposure to kainate-induced status epilepticus
publisher BMC
series BMC Medical Imaging
issn 1471-2342
publishDate 2011-01-01
description <p>Abstract</p> <p>Background</p> <p>Increased functionality of efflux transporters at the blood-brain barrier may contribute to decreased drug concentrations at the target site in CNS diseases like epilepsy. In the rat, pharmacoresistant epilepsy can be mimicked by inducing status epilepticus by intraperitoneal injection of kainate, which leads to development of spontaneous seizures after 3 weeks to 3 months. The aim of this study was to investigate potential changes in P-glycoprotein (P-gp) expression and functionality at an early stage after induction of status epilepticus by kainate.</p> <p>Methods</p> <p><it>(R)</it>-[<sup>11</sup>C]verapamil, which is currently the most frequently used positron emission tomography (PET) ligand for determining P-gp functionality at the blood-brain barrier, was used in kainate and saline (control) treated rats, at 7 days after treatment. To investigate the effect of P-gp on <it>(R)</it>-[<sup>11</sup>C]verapamil brain distribution, both groups were studied without or with co-administration of the P-gp inhibitor tariquidar. P-gp expression was determined using immunohistochemistry in post mortem brains. <it>(R)</it>-[<sup>11</sup>C]verapamil kinetics were analyzed with approaches common in PET research (Logan analysis, and compartmental modelling of individual profiles) as well as by population mixed effects modelling (NONMEM).</p> <p>Results</p> <p>All data analysis approaches indicated only modest differences in brain distribution of <it>(R)</it>-[<sup>11</sup>C]verapamil between saline and kainate treated rats, while tariquidar treatment in both groups resulted in a more than 10-fold increase. NONMEM provided most precise parameter estimates. P-gp expression was found to be similar for kainate and saline treated rats.</p> <p>Conclusions</p> <p>P-gp expression and functionality does not seem to change at early stage after induction of anticipated pharmacoresistant epilepsy by kainate.</p>
url http://www.biomedcentral.com/1471-2342/11/1
work_keys_str_mv AT lammertsmaadriaana itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT huismanmarcc itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT windhorstalbertd itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT molthoffcarlafm itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT luurtsemagert itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT syvanenstina itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT voskuylroba itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
AT delangeelizabethc itritsup11supcverapamilpetstudiestoassesschangesinpglycoproteinexpressionandfunctionalityinratbloodbrainbarrierafterexposuretokainateinducedstatusepilepticus
_version_ 1725937904453156864

Similar Items