The role of CD44 and ERM proteins in expression and functionality of P-glycoprotein in breast cancer cells

Pokharel, D; Padula, MP; Lu, JF; Jaiswal, R; Djordjevic, SP; Bebawy, M

The role of CD44 and ERM proteins in expression and functionality of P-glycoprotein in breast cancer cells

Pokharel, D Padula, MP

Lu, JF Jaiswal, R

Djordjevic, SP

Bebawy, M

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Publication Type:: Journal Article
Citation:: Molecules, 2016, 21 (3)
Issue Date:: 2016-03-01

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Field	Value	Language
dc.contributor.author	Pokharel, D	en_US
dc.contributor.author	Padula, MP https://orcid.org/0000-0002-8283-0643	en_US
dc.contributor.author	Lu, JF	en_US
dc.contributor.author	Jaiswal, R https://orcid.org/0000-0002-8691-1352	en_US
dc.contributor.author	Djordjevic, SP https://orcid.org/0000-0001-9301-5372	en_US
dc.contributor.author	Bebawy, M https://orcid.org/0000-0003-2606-921X	en_US
dc.date.available	2016-02-23	en_US
dc.date.issued	2016-03-01	en_US
dc.identifier.citation	Molecules, 2016, 21 (3)	en_US
dc.identifier.uri	http://hdl.handle.net/10453/43767
dc.description.abstract	© 2016 by the authors. Multidrug resistance (MDR) is often attributed to the over-expression of P-glycoprotein (P-gp), which prevents the accumulation of anticancer drugs within cells by virtue of its active drug efflux capacity. We have previously described the intercellular transfer of P-gp via extracellular vesicles (EVs) and proposed the involvement of a unique protein complex in regulating this process. In this paper, we investigate the role of these mediators in the regulation of P-gp functionality and hence the acquisition of MDR following cell to cell transfer. By sequentially silencing the FERM domain-binding proteins, Ezrin, Radixin and Moesin (ERM), as well as CD44, which we also report a selective packaging in breast cancer derived EVs, we have established a role for these proteins, in particular Radixin and CD44, in influencing the P-gp-mediated MDR in whole cells. We also report for the first time the role of ERM proteins in the vesicular transfer of functional P-gp. Specifically, we demonstrate that intercellular membrane insertion is dependent on Ezrin and Moesin, whilst P-gp functionality is governed by the integrity of all ERM proteins in the recipient cell. This study identifies these candidate proteins as potential new therapeutic targets in circumventing MDR clinically.	en_US
dc.relation	http://purl.org/au-research/grants/nhmrc/GNT1007613
dc.relation.ispartof	Molecules	en_US
dc.relation.isbasedon	10.3390/molecules21030290	en_US
dc.subject.classification	Organic Chemistry	en_US
dc.subject.mesh	Cell Line, Tumor	en_US
dc.subject.mesh	Transport Vesicles	en_US
dc.subject.mesh	Humans	en_US
dc.subject.mesh	Breast Neoplasms	en_US
dc.subject.mesh	Microfilament Proteins	en_US
dc.subject.mesh	ATP Binding Cassette Transporter, Subfamily B	en_US
dc.subject.mesh	Cytoskeletal Proteins	en_US
dc.subject.mesh	Drug Resistance, Multiple	en_US
dc.subject.mesh	Drug Resistance, Neoplasm	en_US
dc.subject.mesh	Female	en_US
dc.subject.mesh	Hyaluronan Receptors	en_US
dc.subject.mesh	MCF-7 Cells	en_US
dc.subject.mesh	Membrane Proteins	en_US
dc.subject.mesh	Proteomics	en_US
dc.title	The role of CD44 and ERM proteins in expression and functionality of P-glycoprotein in breast cancer cells	en_US
dc.type	Journal Article
utslib.citation.volume	3	en_US
utslib.citation.volume	21	en_US
utslib.for	0305 Organic Chemistry	en_US
utslib.for	0304 Medicinal and Biomolecular Chemistry	en_US
utslib.for	0307 Theoretical and Computational Chemistry	en_US
pubs.embargo.period	Not known	en_US
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Science
pubs.organisational-group	/University of Technology Sydney/Faculty of Science/School of Life Sciences
pubs.organisational-group	/University of Technology Sydney/Graduate School of Health
pubs.organisational-group	/University of Technology Sydney/Strength - CHT - Health Technologies
pubs.organisational-group	/University of Technology Sydney/Strength - ithree - Institute of Infection, Immunity and Innovation
utslib.copyright.status	open_access
pubs.issue	3	en_US
pubs.publication-status	Published	en_US
pubs.volume	21	en_US

Abstract:

© 2016 by the authors. Multidrug resistance (MDR) is often attributed to the over-expression of P-glycoprotein (P-gp), which prevents the accumulation of anticancer drugs within cells by virtue of its active drug efflux capacity. We have previously described the intercellular transfer of P-gp via extracellular vesicles (EVs) and proposed the involvement of a unique protein complex in regulating this process. In this paper, we investigate the role of these mediators in the regulation of P-gp functionality and hence the acquisition of MDR following cell to cell transfer. By sequentially silencing the FERM domain-binding proteins, Ezrin, Radixin and Moesin (ERM), as well as CD44, which we also report a selective packaging in breast cancer derived EVs, we have established a role for these proteins, in particular Radixin and CD44, in influencing the P-gp-mediated MDR in whole cells. We also report for the first time the role of ERM proteins in the vesicular transfer of functional P-gp. Specifically, we demonstrate that intercellular membrane insertion is dependent on Ezrin and Moesin, whilst P-gp functionality is governed by the integrity of all ERM proteins in the recipient cell. This study identifies these candidate proteins as potential new therapeutic targets in circumventing MDR clinically.

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http://hdl.handle.net/10453/43767