Mrp4 confers resistance to topotecan and protects the brain from chemotherapy

Markos Leggas; Masashi Adachi; George L. Scheffer; Daxi Sun; Peter Wielinga; Guoqing Du; Kelly E. Mercer; Yanli Zhuang; John C. Panetta; Brad Johnston; Rik J. Scheper; Clinton F. Stewart; John D. Schuetz

doi:10.1128/MCB.24.17.7612-7621.2004

Mrp4 confers resistance to topotecan and protects the brain from chemotherapy

Markos Leggas, Masashi Adachi, George L. Scheffer, Daxi Sun, Peter Wielinga, Guoqing Du, Kelly E. Mercer, Yanli Zhuang, John C. Panetta, Brad Johnston, Rik J. Scheper, Clinton F. Stewart, John D. Schuetz

Pharmaceutical Sciences

Research output: Contribution to journal › Article › peer-review

383 Scopus citations

Abstract

The role of the multidrug resistance protein MRP4/ABCC4 in vivo remains undefined. To explore this role, we generated Mrp4-deficient mice. Unexpectedly, these mice showed enhanced accumulation of the anticancer agent topotecan in brain tissue and cerebrospinal fluid (CSF). Further studies demonstrated that topotecan was an Mrp4 substrate and that cells overexpressing Mrp4. were resistant to its cytotoxic effects. We then used new antibodies to discover that Mrp4 is unique among the anionic ATP-dependent transporters in its dual localization at the basolateral membrane of the choroid plexus epithelium and in the apical membrane of the endothelial cells of the brain capillaries. Microdialysis sampling of ventricular CSF demonstrated that localization of Mrp4 at the choroid epithelium is integral to its function in limiting drug penetration into the CSF. The topotecan resistance of cells overexpressing Mrp4 and the polarized expression of Mrp4 in the choroid plexus and brain capillary endothelial cells indicate that Mrp4 has a dual role in protecting the brain from cytotoxins and suggest that the therapeutic efficacy of central nervous system-directed drugs that are Mrp4 substrates may be improved by developing Mrp4 inhibitors.

Original language	English
Pages (from-to)	7612-7621
Number of pages	10
Journal	Molecular and Cellular Biology
Volume	24
Issue number	17
DOIs	https://doi.org/10.1128/MCB.24.17.7612-7621.2004
State	Published - Sep 2004

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1128/MCB.24.17.7612-7621.2004

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title = "Mrp4 confers resistance to topotecan and protects the brain from chemotherapy",

abstract = "The role of the multidrug resistance protein MRP4/ABCC4 in vivo remains undefined. To explore this role, we generated Mrp4-deficient mice. Unexpectedly, these mice showed enhanced accumulation of the anticancer agent topotecan in brain tissue and cerebrospinal fluid (CSF). Further studies demonstrated that topotecan was an Mrp4 substrate and that cells overexpressing Mrp4. were resistant to its cytotoxic effects. We then used new antibodies to discover that Mrp4 is unique among the anionic ATP-dependent transporters in its dual localization at the basolateral membrane of the choroid plexus epithelium and in the apical membrane of the endothelial cells of the brain capillaries. Microdialysis sampling of ventricular CSF demonstrated that localization of Mrp4 at the choroid epithelium is integral to its function in limiting drug penetration into the CSF. The topotecan resistance of cells overexpressing Mrp4 and the polarized expression of Mrp4 in the choroid plexus and brain capillary endothelial cells indicate that Mrp4 has a dual role in protecting the brain from cytotoxins and suggest that the therapeutic efficacy of central nervous system-directed drugs that are Mrp4 substrates may be improved by developing Mrp4 inhibitors.",

author = "Markos Leggas and Masashi Adachi and Scheffer, {George L.} and Daxi Sun and Peter Wielinga and Guoqing Du and Mercer, {Kelly E.} and Yanli Zhuang and Panetta, {John C.} and Brad Johnston and Scheper, {Rik J.} and Stewart, {Clinton F.} and Schuetz, {John D.}",

year = "2004",

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doi = "10.1128/MCB.24.17.7612-7621.2004",

language = "English",

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T1 - Mrp4 confers resistance to topotecan and protects the brain from chemotherapy

AU - Leggas, Markos

AU - Adachi, Masashi

AU - Scheffer, George L.

AU - Sun, Daxi

AU - Wielinga, Peter

AU - Du, Guoqing

AU - Mercer, Kelly E.

AU - Zhuang, Yanli

AU - Panetta, John C.

AU - Johnston, Brad

AU - Scheper, Rik J.

AU - Stewart, Clinton F.

AU - Schuetz, John D.

PY - 2004/9

Y1 - 2004/9

N2 - The role of the multidrug resistance protein MRP4/ABCC4 in vivo remains undefined. To explore this role, we generated Mrp4-deficient mice. Unexpectedly, these mice showed enhanced accumulation of the anticancer agent topotecan in brain tissue and cerebrospinal fluid (CSF). Further studies demonstrated that topotecan was an Mrp4 substrate and that cells overexpressing Mrp4. were resistant to its cytotoxic effects. We then used new antibodies to discover that Mrp4 is unique among the anionic ATP-dependent transporters in its dual localization at the basolateral membrane of the choroid plexus epithelium and in the apical membrane of the endothelial cells of the brain capillaries. Microdialysis sampling of ventricular CSF demonstrated that localization of Mrp4 at the choroid epithelium is integral to its function in limiting drug penetration into the CSF. The topotecan resistance of cells overexpressing Mrp4 and the polarized expression of Mrp4 in the choroid plexus and brain capillary endothelial cells indicate that Mrp4 has a dual role in protecting the brain from cytotoxins and suggest that the therapeutic efficacy of central nervous system-directed drugs that are Mrp4 substrates may be improved by developing Mrp4 inhibitors.

AB - The role of the multidrug resistance protein MRP4/ABCC4 in vivo remains undefined. To explore this role, we generated Mrp4-deficient mice. Unexpectedly, these mice showed enhanced accumulation of the anticancer agent topotecan in brain tissue and cerebrospinal fluid (CSF). Further studies demonstrated that topotecan was an Mrp4 substrate and that cells overexpressing Mrp4. were resistant to its cytotoxic effects. We then used new antibodies to discover that Mrp4 is unique among the anionic ATP-dependent transporters in its dual localization at the basolateral membrane of the choroid plexus epithelium and in the apical membrane of the endothelial cells of the brain capillaries. Microdialysis sampling of ventricular CSF demonstrated that localization of Mrp4 at the choroid epithelium is integral to its function in limiting drug penetration into the CSF. The topotecan resistance of cells overexpressing Mrp4 and the polarized expression of Mrp4 in the choroid plexus and brain capillary endothelial cells indicate that Mrp4 has a dual role in protecting the brain from cytotoxins and suggest that the therapeutic efficacy of central nervous system-directed drugs that are Mrp4 substrates may be improved by developing Mrp4 inhibitors.

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Mrp4 confers resistance to topotecan and protects the brain from chemotherapy

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