2014
DOI: 10.1124/mol.113.091439
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Long-Term Channel Block Is Required to Inhibit Cellular Transformation by Human Ether-à-Go-Go–Related Gene (hERG1) Potassium Channels

Abstract: Both human ether-à-go-go-related gene (hERG1) and the closely related human ether-à-go-go (hEAG1) channel are aberrantly expressed in a large proportion of human cancers. In the present study, we demonstrate that transfection of hERG1 into mouse fibroblasts is sufficient to induce many features characteristic of malignant transformation. An important finding of this work is that this transformation could be reversed by chronic incubation (for 2-3 weeks) with the hERG channel blocker dofetilide (100 nM), wherea… Show more

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Cited by 11 publications
(13 citation statements)
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“…Interestingly, altered motility was paralleled by a reduced capacity for cells to reorganize their actin cytoskeleton, to promote the formation of actin spike, and to change their shape following contact with ECM (46). This result is in line with previous observations showing that hERG expression contributes to morphology, actin cytoskeleton dynamics, and finally cell migration behavior (11). Together, these data reveal that Sig1R participates to cancer migration potency in response to ECM.…”
Section: Discussionsupporting
confidence: 81%
See 1 more Smart Citation
“…Interestingly, altered motility was paralleled by a reduced capacity for cells to reorganize their actin cytoskeleton, to promote the formation of actin spike, and to change their shape following contact with ECM (46). This result is in line with previous observations showing that hERG expression contributes to morphology, actin cytoskeleton dynamics, and finally cell migration behavior (11). Together, these data reveal that Sig1R participates to cancer migration potency in response to ECM.…”
Section: Discussionsupporting
confidence: 81%
“…9,10]. hERG expression is sufficient to induce transformation of fibroblasts (11), and in cancer cells, it forms membrane platforms with receptors of the tumor cell microenvironment, such as integrins [adhesion receptors of the extracellular matrix (ECM)], that deeply influences signaling pathways controlling in turn cancer cell spreading (12). Targeting proteins regulating ion channel activity in cancer cells appears as a promising way to control cancer cell behavior.…”
Section: Introductionmentioning
confidence: 99%
“…In these conditions, even 0.1 mM produced significant reduction of cell proliferation. This is also in agreement with recent results by Pier et al (2014) showing that nonsaturating concentrations of hERG1 blockers need to be applied for long periods of time to fully produce their antitransformation effects. Although different leukemia models and different administration schedules (e.g., twice per day) could be tested, our in vivo data indicate that CD-160130 is On the whole, K V 11.1 would seem an attractive target for antineoplastic therapy, particularly in leukemias.…”
Section: Discussionsupporting
confidence: 81%
“…NIH3T3-cells stably transfected with K v 11.1 (hERG1) channels show a loss of cell contact inhibition. In culture, these cells grow in multiple layers and at high density [31]. Interestingly, their morphology changes from fibroblast-like to spindle-shaped while both the degree of cell polarization and migration increase.…”
Section: Emt and Loss Of Cell-cell Contactsmentioning
confidence: 96%
“…Interestingly, their morphology changes from fibroblast-like to spindle-shaped while both the degree of cell polarization and migration increase. Furthermore, allogeneic transplantation of hERG1-expressing cells into nude mice leads to an increased incidence of tumors [31].…”
Section: Emt and Loss Of Cell-cell Contactsmentioning
confidence: 99%