BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Response to oxidative stress, Breast Cancer, Heart, DNA fingerprint, Prozac, CYP51)
Bookmark Forward

Dual inhibition of sodium-mediated proton and calcium efflux triggers non-apoptotic cell death in malignant gliomas.

William Harley, Candace Floyd, Tamara Dunn, Xiao-Dong Zhang, Tsung-Yu Chen, Manu Hegde, Hasan Palandoken, Michael H Nantz, Leonardo Leon, K L Carraway, Bruce Lyeth, Fredric A Gorin

Department of Neurology, University of California, Davis, USA.

Brain research 2010 Dec 2


filter terms:
  • 2 4'- dichlorobenzamil (1)
  • amiloride (8)
  • aniline compounds (2)
  • animals (1)
  • astrocytes (3)
  • brain neoplasms (1)
  • calcium (6)
  • cariporide (4)
  • caspase (1)
  • cell (9)
  • cell death (4)
  • cytosol (1)
  • cytostatic (1)
  • dichlorobenzamil (5)
  • gliomas (13)
  • guanidines (2)
  • human cell (1)
  • humans (1)
  • hypoxia (1)
  • hypoxia brain (1)
  • intracellular (1)
  • ionomycin (2)
  • ionophores (2)
  • ischemia (1)
  • isoform (2)
  • levels sodium (1)
  • NCX1 (5)
  • NHE1 (7)
  • personal space (1)
  • phenyl ethers (2)
  • protons (2)
  • rats (1)
  • rats sprague- dawley (2)
  • sea0400 (4)
  • slc9a1 protein, rat (1)
  • sodium (6)
  • sodium calcium exchange (1)
  • sodium calcium exchanger (3)
  • sodium calcium exchanger 1 (1)
  • sodium hydrogen antiporter (2)
  • sulfones (2)
  • transport (1)
    • Sizes of these terms reflect their relevance to your search.

    Malignant glioma cells maintain an elevated intracellular pH (pH(i)) within hypoxic-ischemic tumor microenvironments through persistent activation of sodium-proton transport (McLean et al., 2000). Amiloride has been reported to selectively kill human malignant glioma cell lines but not primary astrocytes (Hegde et al., 2004). While amiloride reduces pH(i) of malignant gliomas by inhibiting isoform 1 of sodium-proton exchange (NHE1), direct acidification was shown to be cytostatic rather than cytotoxic. At cytotoxic concentrations, amiloride has multiple drug targets including inhibition of NHE1 and sodium-calcium exchange. Amiloride's glioma cytotoxicity can be explained, at least in part, by dual inhibition of NHE1 and of Na(+)-dependent calcium efflux by isoform 1.1 of the sodium-calcium exchanger (NCX1.1), which increases [Ca(2+)](i) and initiates glioma cell demise. As a result of persistent NHE1 activity, cytosolic free levels of sodium ([Na(+)](i)) in U87 and C6 glioma cells are elevated 3-fold, as compared with normal astrocytes. Basal cytosolic free calcium levels ([Ca(2+)](i)) also are increased 5-fold. 2', 4'-dichlorobenzamil (DCB) inhibits the sodium-dependent calcium transporter (NCX1.1) much more potently than NHE1. DCB was employed in a concentration-dependent fashion in glioma cells to selectively inhibit the forward mode of NCX1.1 at ≤1μM, while dually inhibiting both NHE1 and NCX1.1 at ≥20μM. DCB (1μM) was not cytotoxic to glioma cells, while DCB (20μM) further increased basal elevated levels of [Ca(2+)](i) in glioma cells that was followed by cell demise. Cariporide and SEA0400 are more selective inhibitors of NHE1 and NCX1.1 than amiloride or DCB, respectively. Individually, Cariporide and SEA0400 are not cytotoxic, but in combination induced glioma cell death. Like amiloride, the combination of Cariporide and SEA0400 produced glioma cell death in the absence of demonstrable caspase activation. Copyright © 2010 Elsevier B.V. All rights reserved.

    Citation

    William Harley, Candace Floyd, Tamara Dunn, Xiao-Dong Zhang, Tsung-Yu Chen, Manu Hegde, Hasan Palandoken, Michael H Nantz, Leonardo Leon, K L Carraway, Bruce Lyeth, Fredric A Gorin. Dual inhibition of sodium-mediated proton and calcium efflux triggers non-apoptotic cell death in malignant gliomas. Brain research. 2010 Dec 2;1363:159-69

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 20869350

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.