Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.

Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.

Many cell lines derived from tumors as well as transformed cell lines are far more sensitive to V-ATPase inhibitors than normal counterparts. The molecular mechanisms underlying these differences in sensitivity are not known. Using global gene expression data, we show that the most sensitive respons...

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Main Authors: Sarah Straud, Iryna Zubovych, Jef K De Brabander, Michael G Roth
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-07-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2905441?pdf=render
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spelling doaj-19230cabd779487c980ebe8a0491b6712020-11-24T22:06:41ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-07-0157e1162910.1371/journal.pone.0011629Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.Sarah StraudIryna ZubovychJef K De BrabanderMichael G RothMany cell lines derived from tumors as well as transformed cell lines are far more sensitive to V-ATPase inhibitors than normal counterparts. The molecular mechanisms underlying these differences in sensitivity are not known. Using global gene expression data, we show that the most sensitive responses to HeLa cells to low doses of V-ATPase inhibitors involve genes responsive to decreasing intracellular iron or decreasing cholesterol and that sensitivity to iron uptake is an important determinant of V-ATPase sensitivity in several cancer cell lines. One of the most sensitive cell lines, melanoma derived SK-Mel-5, over-expresses the iron efflux transporter ferroportin and has decreased expression of proteins involved in iron uptake, suggesting that it actively suppresses cytoplasmic iron. SK-Mel-5 cells have increased production of reactive oxygen species and may be seeking to limit additional production of ROS by iron.http://europepmc.org/articles/PMC2905441?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Sarah Straud
Iryna Zubovych
Jef K De Brabander
Michael G Roth
spellingShingle Sarah Straud
Iryna Zubovych
Jef K De Brabander
Michael G Roth
Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.
PLoS ONE
author_facet Sarah Straud
Iryna Zubovych
Jef K De Brabander
Michael G Roth
author_sort Sarah Straud
title Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.
title_short Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.
title_full Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.
title_fullStr Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.
title_full_unstemmed Inhibition of iron uptake is responsible for differential sensitivity to V-ATPase inhibitors in several cancer cell lines.
title_sort inhibition of iron uptake is responsible for differential sensitivity to v-atpase inhibitors in several cancer cell lines.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2010-07-01
description Many cell lines derived from tumors as well as transformed cell lines are far more sensitive to V-ATPase inhibitors than normal counterparts. The molecular mechanisms underlying these differences in sensitivity are not known. Using global gene expression data, we show that the most sensitive responses to HeLa cells to low doses of V-ATPase inhibitors involve genes responsive to decreasing intracellular iron or decreasing cholesterol and that sensitivity to iron uptake is an important determinant of V-ATPase sensitivity in several cancer cell lines. One of the most sensitive cell lines, melanoma derived SK-Mel-5, over-expresses the iron efflux transporter ferroportin and has decreased expression of proteins involved in iron uptake, suggesting that it actively suppresses cytoplasmic iron. SK-Mel-5 cells have increased production of reactive oxygen species and may be seeking to limit additional production of ROS by iron.
url http://europepmc.org/articles/PMC2905441?pdf=render
work_keys_str_mv AT sarahstraud inhibitionofironuptakeisresponsiblefordifferentialsensitivitytovatpaseinhibitorsinseveralcancercelllines
AT irynazubovych inhibitionofironuptakeisresponsiblefordifferentialsensitivitytovatpaseinhibitorsinseveralcancercelllines
AT jefkdebrabander inhibitionofironuptakeisresponsiblefordifferentialsensitivitytovatpaseinhibitorsinseveralcancercelllines
AT michaelgroth inhibitionofironuptakeisresponsiblefordifferentialsensitivitytovatpaseinhibitorsinseveralcancercelllines
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