Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.

Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.

Dysregulated PI3K/Akt signaling occurs commonly in breast cancers and is due to HER2 amplification, PI3K mutation or PTEN inactivation. The objective of this study was to determine the role of Akt activation in breast cancer as a function of mechanism of activation and whether inhibition of Akt sign...

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Main Authors: Qing-Bai She, Sarat Chandarlapaty, Qing Ye, Jose Lobo, Kathleen M Haskell, Karen R Leander, Deborah DeFeo-Jones, Hans E Huber, Neal Rosen
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2008-08-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2516933?pdf=render
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spelling doaj-b5b859fcec964286a6785e18f0e5d4e22020-11-24T20:45:52ZengPublic Library of Science (PLoS)PLoS ONE1932-62032008-08-0138e306510.1371/journal.pone.0003065Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.Qing-Bai SheSarat ChandarlapatyQing YeJose LoboKathleen M HaskellKaren R LeanderDeborah DeFeo-JonesHans E HuberNeal RosenDysregulated PI3K/Akt signaling occurs commonly in breast cancers and is due to HER2 amplification, PI3K mutation or PTEN inactivation. The objective of this study was to determine the role of Akt activation in breast cancer as a function of mechanism of activation and whether inhibition of Akt signaling is a feasible approach to therapy.A selective allosteric inhibitor of Akt kinase was used to interrogate a panel of breast cancer cell lines characterized for genetic lesions that activate PI3K/Akt signaling: HER2 amplification or PI3K or PTEN mutations in order to determine the biochemical and biologic consequences of inhibition of this pathway. A variety of molecular techniques and tissue culture and in vivo xenograft models revealed that tumors with mutational activation of Akt signaling were selectively dependent on the pathway. In sensitive cells, pathway inhibition resulted in D-cyclin loss, G1 arrest and induction of apoptosis, whereas cells without pathway activation were unaffected. Most importantly, the drug effectively inhibited Akt kinase and its downstream effectors in vivo and caused complete suppression of the growth of breast cancer xenografts with PI3K mutation or HER2 amplification, including models of the latter selected for resistance to Herceptin. Furthermore, chronic administration of the drug was well-tolerated, causing only transient hyperglycemia without gross toxicity to the host despite the pleiotropic normal functions of Akt.These data demonstrate that breast cancers with PI3K mutation or HER2 amplification are selectively dependent on Akt signaling, and that effective inhibition of Akt in tumors is feasible and effective in vivo. These findings suggest that direct inhibition of Akt may represent a therapeutic strategy for breast and other cancers that are addicted to the pathway including tumors with resistant to Herceptin.http://europepmc.org/articles/PMC2516933?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Qing-Bai She
Sarat Chandarlapaty
Qing Ye
Jose Lobo
Kathleen M Haskell
Karen R Leander
Deborah DeFeo-Jones
Hans E Huber
Neal Rosen
spellingShingle Qing-Bai She
Sarat Chandarlapaty
Qing Ye
Jose Lobo
Kathleen M Haskell
Karen R Leander
Deborah DeFeo-Jones
Hans E Huber
Neal Rosen
Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.
PLoS ONE
author_facet Qing-Bai She
Sarat Chandarlapaty
Qing Ye
Jose Lobo
Kathleen M Haskell
Karen R Leander
Deborah DeFeo-Jones
Hans E Huber
Neal Rosen
author_sort Qing-Bai She
title Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.
title_short Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.
title_full Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.
title_fullStr Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.
title_full_unstemmed Breast tumor cells with PI3K mutation or HER2 amplification are selectively addicted to Akt signaling.
title_sort breast tumor cells with pi3k mutation or her2 amplification are selectively addicted to akt signaling.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2008-08-01
description Dysregulated PI3K/Akt signaling occurs commonly in breast cancers and is due to HER2 amplification, PI3K mutation or PTEN inactivation. The objective of this study was to determine the role of Akt activation in breast cancer as a function of mechanism of activation and whether inhibition of Akt signaling is a feasible approach to therapy.A selective allosteric inhibitor of Akt kinase was used to interrogate a panel of breast cancer cell lines characterized for genetic lesions that activate PI3K/Akt signaling: HER2 amplification or PI3K or PTEN mutations in order to determine the biochemical and biologic consequences of inhibition of this pathway. A variety of molecular techniques and tissue culture and in vivo xenograft models revealed that tumors with mutational activation of Akt signaling were selectively dependent on the pathway. In sensitive cells, pathway inhibition resulted in D-cyclin loss, G1 arrest and induction of apoptosis, whereas cells without pathway activation were unaffected. Most importantly, the drug effectively inhibited Akt kinase and its downstream effectors in vivo and caused complete suppression of the growth of breast cancer xenografts with PI3K mutation or HER2 amplification, including models of the latter selected for resistance to Herceptin. Furthermore, chronic administration of the drug was well-tolerated, causing only transient hyperglycemia without gross toxicity to the host despite the pleiotropic normal functions of Akt.These data demonstrate that breast cancers with PI3K mutation or HER2 amplification are selectively dependent on Akt signaling, and that effective inhibition of Akt in tumors is feasible and effective in vivo. These findings suggest that direct inhibition of Akt may represent a therapeutic strategy for breast and other cancers that are addicted to the pathway including tumors with resistant to Herceptin.
url http://europepmc.org/articles/PMC2516933?pdf=render
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