Doxorubicin resistance in a small cell lung cancer cell line can be abolished by siRNA down-regulation of cox 1

Doxorubicin resistance in a small cell lung cancer cell line can be abolished by siRNA down-regulation of cox 1

Multidrug resistance (MDR) in small cell lung cancer is one of the major causes of failures of chemotherapy. MDR is a means of protection of tumor cells against chemotherapeutic drugs. Although the molecular basis of MDR is not fully understood, genes involved in apoptosis may be mutated. Recent fin...

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Bibliographic Details
Main Author: Aryal, Pratik
Other Authors: Vann, Carolyn N.
Format: Others
Published: 2011
Subjects:
Doxorubicin > Effectiveness.
Drug resistance in cancer cells.
Small cell lung cancer > Genetic aspects.
Cyclooxygenases > Inhibitors.
Gene silencing.
Online Access:http://cardinalscholar.bsu.edu/handle/handle/188277
http://liblink.bsu.edu/uhtbin/catkey/1371682
Description
Summary:Multidrug resistance (MDR) in small cell lung cancer is one of the major causes of failures of chemotherapy. MDR is a means of protection of tumor cells against chemotherapeutic drugs. Although the molecular basis of MDR is not fully understood, genes involved in apoptosis may be mutated. Recent finding of a link between over-expression of an apoptotic gene, cyclooxygenase 1 (cox 1), and MDR suggests that cox 1 is involved in the development of MDR phenotype. This research was an attempt to observe whether up-regulation of cox 1 contributes to the MDR phenotype in small cell lung cancer cells. This research ultimately may provide a mechanism to reverse the abberant up-regulation of apoptosis genes associated with multidrug resistance to either eliminate or control reproduction of cancer cells. Real time RT PCR was used to confirm the up-regulation of cox 1 in cultured MDR resistant small cell lung cancer cells (GLC4). The up-regulated cox 1 expression was down-regulated using RNA interference technology (RNAi) by transfection with an anti-cox 1 siRNA. More than 90% transfection of cells was confirmed using confocal microscopy. Down-regulation of cox 1 was validated as the protein expression significantly decreased (P=0.004) from multidrug resistant small cell lung cancer transfected cells compared to multidrug resistant nontransfected cells. There was decrease level of expression of cox 1 in multidrug resistant cells after the knockdown with siRNA specific to cox 1. The decreased level of cox 1 expression and, therefore, Cox 1 production increased the rate of apoptosis in small cell lung cancer cells as indicated by its sensitivity to the doxorubicin. === Department of Biology

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