Journal article

Mutational analysis of P-glycoprotein: Suppression of caspase activation in the absence of ATP-dependent drug efflux

KM Tainton, MJ Smyth, JT Jackson, JE Tanner, L Cerruti, SM Jane, PK Darcy, RW Johnstone

Cell Death and Differentiation | NATURE PUBLISHING GROUP | Published : 2004

DOI: 10.1038/sj.cdd.4401440

Abstract

P-glycoprotein (P-gp) can induce multidrug resistance (MDR) through the ATP-dependent efflux of chemotherapeutic agents. We have previously shown that P-gp can inhibit nondrug apoptotic stimuli by suppressing the activation of caspases. To determine if this additional activity is functionally linked to ATP hydrolysis, we expressed wild-type and ATPase-mutant P-gp and showed that cells expressing mutant P-gp could not efflux chemotherapeutic drugs but remained relatively resistant to apoptosis. CEM lymphoma cells expressing mutant P-gp treated with vincristine showed a decrease in the fraction of cells with apoptotic morphology, cytochrome c release from the mitochondria and suppression of ca..

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Keywords

5.1 Pharmaceuticals
Cell Biology
Tumor-Cells
Biochemistry & Molecular Biology
Cell-Death Pathway
Leukemia
Life Sciences & Biomedicine
Transduction
P-Glycoprotein
Bone-Marrow-Cells
Transporter
Cancer
Expression
32 Biomedical and Clinical Sciences
Drug Resistance
Protein
3101 Biochemistry and Cell Biology
31 Biological Sciences
Generic Health Relevance
Mediated Multidrug-Resistance
Caspase
Science & Technology