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Research ArticleExperimental Studies

Benzo[a]phenoxazines: A New Group of Potent P-glycoprotein Inhibitors

OLGA WESOLOWSKA, JOSEPH MOLNAR, GUNNAR WESTMAN, KRISTIN SAMUELSSON, MASAMI KAWASE, IMRE OCSOVSZKI, NOBORU MOTOHASHI and KRYSTYNA MICHALAK
In Vivo January 2006, 20 (1) 109-113;
OLGA WESOLOWSKA
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  • For correspondence: olawes{at}biofiz.am.wroc.pl
JOSEPH MOLNAR
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GUNNAR WESTMAN
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KRISTIN SAMUELSSON
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MASAMI KAWASE
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IMRE OCSOVSZKI
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NOBORU MOTOHASHI
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KRYSTYNA MICHALAK
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Abstract

The ability of fifteen novel phenoxazine derivatives (four phenoxazines and eleven benzo[a]phenoxazines) to modulate multidrug resistance (MDR) in a P-gp-overexpressing mouse T lymphoma cell line (L5178 MDR) was studied. A flow cytometric functional test, based on the differential accumulation of rhodamine 123 by sensitive and multidrug-resistant cells, was employed. Seven benzo[a]phenoxazines were observed to increase the amount of rhodamine 123 accumulated by resistant cells, i.e. to be new effective MDR modulators. The results allowed us to draw preliminary conclusions about the structural features of benzo[a]phenoxazines which are important for MDR modulation.

  • P-glycoprotein
  • multidrug resistance
  • phenoxazine derivatives
  • flow cytometry

Footnotes

  • Received April 12, 2005.
  • Accepted September 16, 2005.
  • Copyright © 2006 The Author(s). Published by the International Institute of Anticancer Research.
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Vol. 20, Issue 1
January-February 2006
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Benzo[a]phenoxazines: A New Group of Potent P-glycoprotein Inhibitors
OLGA WESOLOWSKA, JOSEPH MOLNAR, GUNNAR WESTMAN, KRISTIN SAMUELSSON, MASAMI KAWASE, IMRE OCSOVSZKI, NOBORU MOTOHASHI, KRYSTYNA MICHALAK
In Vivo Jan 2006, 20 (1) 109-113;

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Benzo[a]phenoxazines: A New Group of Potent P-glycoprotein Inhibitors
OLGA WESOLOWSKA, JOSEPH MOLNAR, GUNNAR WESTMAN, KRISTIN SAMUELSSON, MASAMI KAWASE, IMRE OCSOVSZKI, NOBORU MOTOHASHI, KRYSTYNA MICHALAK
In Vivo Jan 2006, 20 (1) 109-113;
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