Your search keyword '"Eag1"' showing total 6 results

1. Dronedarone blockage of the tumor-related Kv10.1 channel: a comparison with amiodarone.

Author

Meléndez, T. A., Huanosta-Gutiérrez, A., Barriga-Montoya, C., González-Andrade, M., and Gómez-Lagunas, F.

Subjects

*AMIODARONE, *DRUG interactions, *DRUG side effects, *POTASSIUM channels

Abstract

Kv10.1 (Eag1, or KCNH1) is a human potassium-selective channel associated with tumor development. In this work, we study the interaction of the drug dronedarone with Kv10.1. Dronedarone presents two chemical modifications aimed to lessen side effects produced by its parent molecule, the antiarrhythmic amiodarone. Hence, our observations are discussed within the framework of a previously reported interaction of amiodarone with Kv10.1. Additionally, we show new data regarding the interaction of amiodarone with the channels. We found that, unexpectedly, the effect of dronedarone on Kv10.1 differs both quantitatively and qualitatively to that of amiodarone. Among other observations, we found that dronedarone seems to be an open-pore blocker, in contrast to the reported behavior of amiodarone, which seems to inhibit from both open and closed states. Additionally, herein we provide evidence showing that, in spite of their chemical similarity, these molecules inhibit the K+ conductance by binding to non-overlapping, independent (non-allosterically related) sites. Also, we show that, while amiodarone inhibits the Cole-Moore shift, dronedarone is unable to inhibit this voltage-dependent characteristic of Kv10.1. [ABSTRACT FROM AUTHOR]

Published

2020

2. Eag1 Voltage-Dependent Potassium Channels: Structure, Electrophysiological Characteristics, and Function in Cancer.

Author

Wang, Xuzhao, Chen, Yafei, Zhang, Yuhong, Guo, Shuai, Mo, Li, An, Hailong, and Zhan, Yong

Subjects

*POTASSIUM channels, *ELECTROPHYSIOLOGY, *MOLECULAR structure, *ADRENAL glands, *CANCER cell proliferation, *MYOBLASTS, *POTASSIUM metabolism, *PROTEIN metabolism, *ANIMALS, *CARRIER proteins, *POTASSIUM, *TUMORS

Abstract

Eag1 (ether-à-go-go-1), a member of the voltage-dependent potassium channel family, is expressed mainly in the brain, and at low levels in placenta, testis, and adrenal gland, and only transiently in myoblasts. Recently, several studies have suggested that Eag1 is selectively expressed in various tumor tissues. Eag1 plays important roles in tumor proliferation, malignant transformation, invasion, metastasis, recurrence, and prognosis. Therefore, it has become a new molecular target for tumor diagnosis, prognosis evaluation, and tumor-targeted therapy. This review provides information about the current progress in understanding Eag1 structure, electrophysiological characteristics, and role in cancer. [ABSTRACT FROM AUTHOR]

Published

2017

3. Knockdown of Eag1 Expression by RNA Interference Increases Chemosensitivity to Cisplatin in Ovarian Cancer Cells.

Author

Hui, Chen, Lan, Zhang, Yue-li, Lin, Li-lin, Hong, and Li-lin, Huang

Subjects

*GENE expression, *RNA interference, *CISPLATIN, *CANCER cell analysis, *OVARIAN cancer, *HEALTH outcome assessment

Abstract

Ether á go-go 1 (Eag1) is frequently highly expressed in various malignant cancers and its excessive expression is correlated with poor prognosis in various cancers. However, the relationship of Eag1 expression with the clinical outcome of patients having ovarian cancer treated with cisplatin-based adjuvant chemotherapy is still unknown. In this study, we measured the expression of Eag1 in ovarian cancer and investigated the association between cisplatin chemosensitivity of ovarian cancer cells and Eag1 expression level. We demonstrate that decreased expression of Eag1 correlates with favorable prognosis in patients treated with cisplatin-based adjuvant chemotherapy and predicts higher cisplatin sensitivity in ovarian cancer cells. In vitro, knockdown of Eag1 by small interfering RNA facilitated the sensitivity of ovarian cancer cells (SKOV3 and TYK) to cisplatin-induced apoptosis via nuclear factor κ-light chain-enhancer of activated B cells (NF-κB) pathway. Furthermore, knockdown of Eag1 expression was associated with decreased expression of the P-glycoprotein without affecting multidrug resistance-associated protein 1 expression. Taken together, Eag1 may serve as a potential indicator to predict Eag1 chemosensitivity, and silencing Eag1 may represent a potential therapeutic strategy for ovarian cancer. [ABSTRACT FROM AUTHOR]

Published

2015

4. Astemizole-based anticancer therapy for hepatocellular carcinoma (HCC), and Eag1 channels as potential early-stage markers of HCC.

Author

Guadalupe Chávez-López, María, Pérez-Carreón, Julio, Zuñiga-García, Violeta, Díaz-Chávez, José, Herrera, Luis, Caro-Sánchez, Claudia, Acuña-Macías, Isabel, Gariglio, Patricio, Hernández-Gallegos, Elizabeth, Chiliquinga, Andrea, and Camacho, Javier

Abstract

Hepatocellular carcinoma (HCC) has very poor prognosis. Astemizole has gained great interest as a potential anticancer drug because it targets several proteins involved in cancer including the Eag1 ( ether à-go-go-1) potassium channel that is overexpressed in human HCC. Eag1 channels are regulated by cancer etiological factors and have been proposed as early tumor markers. Here, we found that HepG2 and HuH-7 HCC cells displayed Eag1 messenger RNA (mRNA) and protein expression, determined by real-time RT-PCR and immunochemistry, respectively. Astemizole inhibited human HCC cell proliferation (assessed by metabolic activity assay) and induced apoptosis (studied with flow cytometry) in both cell lines. The subcellular Eag1 protein localization was modified by astemizole in the HepG2 cells. The treatment with astemizole prevented diethylnitrosamine (DEN)-induced rat HCC development in vivo (followed by studying γ-glutamyl transpeptidase (GGT) activity). The Eag1 mRNA and protein levels were increased in most DEN-treated groups but decreased after astemizole treatment. GGT activity was decreased by astemizole. The Eag1 protein was detected in cirrhotic and dysplastic rat livers. Astemizole might have clinical utility for HCC prevention and treatment, and Eag1 channels may be potential early HCC biomarkers. These data provide significant basis to include astemizole in HCC clinical trials. [ABSTRACT FROM AUTHOR]

Published

2015

5. Ether- à- go- go 1 (Eag1) Potassium Channel Expression in Dopaminergic Neurons of Basal Ganglia is Modulated by 6-Hydroxydopamine Lesion.

Author

Ferreira, N., Mitkovski, M., Stühmer, W., Pardo, L., and Del Bel, E.

Subjects

*POTASSIUM channels, *ETHER (Anesthetic), *DOPAMINERGIC neurons, *BASAL ganglia, *6-Hydroxydopamine, *DOPAMINE, *NEUROTOXIC agents, *LABORATORY rats

Abstract

The ether à go- go (Eag) gene encodes the voltage-gated potassium (K) ion channel Kv10.1, whose function still remains unknown. As dopamine may directly affect K channels, we evaluated whether a nigrostriatal dopaminergic lesion induced by the neurotoxin 6-hydroxydopamine (6-OHDA) would alter Eag1-K channel expression in the rat basal ganglia and related brain regions. Male Wistar rats received a microinjection of either saline or 6-OHDA (unilaterally) into the medial forebrain bundle. The extent of the dopaminergic lesion induced by 6-OHDA was evaluated by apomorphine-induced rotational behavior and by tyrosine hydroxylase (TH) immunoreactivity. The 6-OHDA microinjection caused a partial or complete lesion of dopaminergic cells, as well as a reduction of Eag1+ cells in a manner proportional to the extent of the lesion. In addition, we observed a decrease in TH immunoreactivity in the ipsilateral striatum. In conclusion, the expression of the Eag1-K-channel throughout the nigrostriatal pathway in the rat brain, its co-localization with dopaminergic cells and its reduction mirroring the extent of the lesion highlight a physiological circuitry where the functional role of this channel can be investigated. The Eag1-K channel expression in dopaminergic cells suggests that these channels are part of the diversified group of ion channels that generate and maintain the electrophysiological activity pattern of dopaminergic midbrain neurons. [ABSTRACT FROM AUTHOR]

Published

2012

6. Tumor cell-selective apoptosis induction through targeting of KV10.1 via bifunctional TRAIL antibody

Author

Hartung, F., Stühmer, W., and Pardo, L.

Subjects

Cancer Research, Cell Survival, Recombinant Fusion Proteins, Gene Expression, Antineoplastic Agents, Apoptosis, lcsh:RC254-282, TNF-Related Apoptosis-Inducing Ligand, Cell Line, Tumor, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Humans, Cycloheximide, Eag1, Research, Cell Cycle, scFv62-TRAIL, KV10.1, Bystander Effect, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Ether-A-Go-Go Potassium Channels, Receptors, TNF-Related Apoptosis-Inducing Ligand, Oncology, Molecular Medicine, Single-Chain Antibodies

Abstract

Background The search for strategies to target ion channels for therapeutic applications has become of increasing interest. Especially, the potassium channel KV10.1 (Ether-á-go-go) is attractive as target since this surface protein is virtually not detected in normal tissue outside the central nervous system, but is expressed in approximately 70% of tumors from different origins. Methods We designed a single-chain antibody against an extracellular region of KV10.1 (scFv62) and fused it to the human soluble TRAIL. The KV10.1-specific scFv62 antibody -TRAIL fusion protein was expressed in CHO-K1 cells, purified by chromatography and tested for biological activity. Results Prostate cancer cells, either positive or negative for KV10.1 were treated with the purified construct. After sensitization with cytotoxic drugs, scFv62-TRAIL induced apoptosis only in KV10.1-positive cancer cells, but not in non-tumor cells, nor in tumor cells lacking KV10.1 expression. In co-cultures with KV10.1-positive cancer cells the fusion protein also induced apoptosis in bystander KV10.1-negative cancer cells, while normal prostate epithelial cells were not affected when present as bystander. Conclusions KV10.1 represents a novel therapeutic target for cancer. We could design a strategy that selectively kills tumor cells based on a KV10.1-specific antibody.