Your search keyword '"KCNE3"' showing total 135 results

1. The potassium channel Kcne3 is a VEGFA-inducible gene selectively expressed by vascular endothelial tip cells

Author

Chunxiang Tong, Nicholas W. Gale, Saathyaki Rajamani, George D. Yancopoulos, Jingtai Cao, Julia Lerner, Virginia Hughes, Zhe Li, Andrew J. Murphy, Eunice Cheung, Gavin Thurston, Carmelo Romano, Gabor Halasz, Ivan B. Lobov, Patricia Boland, Melissa G. Dominguez, and Ron A. Deckelbaum

Subjects

Vascular Endothelial Growth Factor A, VEGFA, 0301 basic medicine, Cancer Research, Cell type, Mice, 129 Strain, Physiology, Angiogenesis, Kcne3, Clinical Biochemistry, Neovascularization, Physiologic, Mice, Transgenic, Biology, Retina, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pregnancy, Morphogenesis, Animals, Allele, Cells, Cultured, Original Paper, Diabetic Retinopathy, Retinal angiogenesis, Neovascularization, Pathologic, Inducible gene, Endothelial Cells, Gene Expression Regulation, Developmental, Retinal Vessels, Cell Differentiation, KCNE3, Retinal, Embryo, Mammalian, Potassium channel, Cell biology, Mice, Inbred C57BL, Vascular endothelial growth factor A, 030104 developmental biology, Animals, Newborn, chemistry, Potassium Channels, Voltage-Gated, 030220 oncology & carcinogenesis, Female, Endothelial tip-cell

Abstract

Angiogenesis is largely driven by motile endothelial tip-cells capable of invading avascular tissue domains and enabling new vessel formation. Highly responsive to Vascular Endothelial Growth-Factor-A (VEGFA), endothelial tip-cells also suppress angiogenic sprouting in adjacent stalk cells, and thus have been a primary therapeutic focus in addressing neovascular pathologies. Surprisingly, however, there remains a paucity of specific endothelial tip-cell markers. Here, we employ transcriptional profiling and alacZreporter allele to identifyKcne3as an early and selective endothelial tip-cell marker in multiple angiogenic contexts. In development,Kcne3expression initiates during early phases of angiogenesis (E9) and remains specific to endothelial tip-cells, often adjacent to regions expressing VEGFA. Consistently,Kcne3activation is highly responsive to exogenous VEGFA but maintains tip-cell specificity throughout normal retinal angiogenesis. We also demonstrate endothelial tip-cell selectivity ofKcne3in several injury and tumor models. Together, our data show thatKcne3is a unique marker of sprouting angiogenic tip-cells and offers new opportunities for investigating and targeting this cell type.

Published

2019

2. Nr4a1 , Kcne3 and Dgkg Are Identified as Oxygen‐sensitive Genes in the Ductus Arteriosus

Author

Toru Akaike, Susumu Minamisawa, and Takako Yokota

Subjects

medicine.medical_specialty, chemistry.chemical_element, KCNE3, Biology, Biochemistry, Oxygen, medicine.anatomical_structure, chemistry, Internal medicine, Ductus arteriosus, Genetics, medicine, Cardiology, Molecular Biology, Gene, Biotechnology

Published

2021

3. Optimized tight binding between the S1 segment and KCNE3 is required for the constitutively open nature of the KCNQ1-KCNE3 channel complex

Author

Nakajo K and Go Kasuya

Subjects

medicine.anatomical_structure, Channel gating, Chemistry, Protein subunit, Voltage sensor, Biophysics, medicine, KCNE3, Triad (anatomy), Gating, Amino acid residue, Communication channel

Abstract

Tetrameric voltage-gated K+ channels have four identical voltage sensor domains, and they regulate channel gating. KCNQ1 (Kv7.1) is a voltage-gated K+ channel, and its auxiliary subunit KCNE proteins dramatically regulate its gating. For example, KCNE3 makes KCNQ1 a constitutively open channel at physiological voltages by affecting the voltage sensor movement. However, how KCNE proteins regulate the voltage sensor domain is largely unknown. In this study, by utilizing the KCNQ1-KCNE3-calmodulin complex structure, we thoroughly surveyed amino acid residues on KCNE3 and the S1 segment of the KCNQ1 voltage sensor facing each other. By changing the side-chain bulkiness of these interacting amino acid residues, we found that the distance between the S1 segment and KCNE3 is elaborately optimized to achieve the constitutive activity. In addition, we identified two pairs of KCNQ1 and KCNE3 mutants that partially restored constitutive activity by co-expression. Our work suggests that tight binding of the S1 segment and KCNE3 is crucial for controlling the voltage sensor domains.

Published

2021

4. Molecular expression and functional features of Kv7 channels in human prostate smooth muscle

Author

Hyun Hwan Sung, Joongwon Choi, Deok Hyun Han, Mee Ree Chae, Sung Won Lee, Su Jeong Kang, and Jimin Shin

Subjects

Male, medicine.medical_specialty, Urology, Endocrinology, Diabetes and Metabolism, In Vitro Techniques, Cell Line, 03 medical and health sciences, Bridged Bicyclo Compounds, 0302 clinical medicine, Endocrinology, Prostate, Internal medicine, medicine, Humans, Anilides, Membrane potential, 030219 obstetrics & reproductive medicine, biology, Chemistry, Colocalization, KCNE3, Muscle, Smooth, Voltage-gated potassium channel, KCNE4, Potassium channel, Electrophysiology, medicine.anatomical_structure, Reproductive Medicine, Potassium Channels, Voltage-Gated, biology.protein

Abstract

BACKGROUND Relaxation of prostate smooth muscle tone is a key strategy for the medical treatment of lower urinary tract symptoms (LUTS) in men. However, potassium channel's physiological role inhuman prostatic smooth muscle (HPrSM) has yet to be determined. OBJECTIVES In this study, we examined the molecular characteristics and physiological roles of Kv7 channels in HPrSM. MATERIALS AND METHODS The expressions of KCNQ1-5 (Kv7 channel pore-forming α-subunits) and KCNE1-5 (β-regulatory subunits) isoforms in HPrSM were examined using real-time PCR. The relaxation effect of ML213 was investigated by cumulatively adding ML213 to the prostate strips. Kv7 currents were recorded using an amphotericin-B perforated patch-clamp technique. RESULTS In HPrSM cells, KCNQ4, KCNQ5, and KCNE4 isoforms were predominantly expressed, while KCNQ1, KCNQ5, and KCNE3 isoforms were the most abundantly expressed in human prostatic tissues. Western blot analysis revealed the protein expression of the Kv7.1, 7.4, and 7.5 channel subtypes in human prostate tissues (n = 3). ML213 (an activator of Kv7.2/7.4/7.5) induced the concentration-dependent relaxation of HPrSM strips (n = 15, p = 0.001), and this effect was attenuated by pretreatment with XE991 (a Kv7.1-7.5 blocker). In electrophysiology studies, ML213 significantly increased the amplitude of whole-cell Kv7 currents in HPrSM cells. ML213-induced outward currents were greater than retigabine (a Kv7.2-7.5 channel activator). The subsequent addition of XE991 completely inhibited the ML213-induced currents (n = 9, p

Published

2020

5. Gating and Regulation of KCNQ1 and KCNQ1 + KCNE1 Channel Complexes

Author

David Fedida, Yundi Wang, and Jodene Eldstrom

Subjects

0301 basic medicine, calmodulin, Calmodulin, Physiology, Voltage clamp, Allosteric regulation, Review, Gating, IKs, lcsh:Physiology, 03 medical and health sciences, 0302 clinical medicine, Ion channel complex, Physiology (medical), single channels, PKA, lcsh:QP1-981, KCNQ1, biology, Chemistry, KCNE3, Potassium channel, Coupling (electronics), 030104 developmental biology, KCNE1, biology.protein, Biophysics, activation gating, 030217 neurology & neurosurgery

Abstract

The IKs channel complex is formed by the co-assembly of Kv7.1 (KCNQ1), a voltage-gated potassium channel, with its β-subunit, KCNE1 and the association of numerous accessory regulatory molecules such as PIP2, calmodulin, and yotiao. As a result, the IKs potassium current shows kinetic and regulatory flexibility, which not only allows IKs to fulfill physiological roles as disparate as cardiac repolarization and the maintenance of endolymph K+ homeostasis, but also to cause significant disease when it malfunctions. Here, we review new areas of understanding in the assembly, kinetics of activation and inactivation, voltage-sensor pore coupling, unitary events and regulation of this important ion channel complex, all of which have been given further impetus by the recent solution of cryo-EM structural representations of KCNQ1 alone and KCNQ1+KCNE3. Recently, the stoichiometric ratio of KCNE1 to KCNQ1 subunits has been confirmed to be variable up to a ratio of 4:4, rather than fixed at 2:4, and we will review the results and new methodologies that support this conclusion. Significant advances have been made in understanding differences between KCNQ1 and IKs gating using voltage clamp fluorimetry and mutational analysis to illuminate voltage sensor activation and inactivation, and the relationship between voltage sensor translation and pore domain opening. We now understand that the KCNQ1 pore can open with different permeabilities and conductance when the voltage sensor is in partially or fully activated positions, and the ability to make robust single channel recordings from IKs channels has also revealed the complicated pore subconductance architecture during these opening steps, during inactivation, and regulation by 1−4 associated KCNE1 subunits. Experiments placing mutations into individual voltage sensors to drastically change voltage dependence or prevent their movement altogether have demonstrated that the activation of KCNQ1 alone and IKs can best be explained using allosteric models of channel gating. Finally, we discuss how the intrinsic gating properties of KCNQ1 and IKs are highly modulated through the impact of intracellular signaling molecules and co-factors such as PIP2, protein kinase A, calmodulin and ATP, all of which modulate IKs current kinetics and contribute to diverse IKs channel complex function.

Published

2020

6. K2PTASK-2 and KCNQ1-KCNE3 K+channels are major players contributing to intestinal anion and fluid secretion

Author

Sandra Villanueva, L. Pablo Cid, Francisca Julio-Kalajzić, Thomas J. Jentsch, Francisco V. Sepúlveda, Margarita Ojeda, and Johanna Burgos

Subjects

0301 basic medicine, Membrane potential, Physiology, Conductance, chemistry.chemical_element, KCNE3, Biology, Calcium, Phenotype, Intestinal epithelium, Epithelium, Cell biology, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Biochemistry, chemistry, medicine, Secretion

Abstract

Key points K+ channels are important in intestinal epithelium as they ensure the ionic homeostasis and electrical potential of epithelial cells during anion and fluid secretion. Intestinal epithelium cAMP-activated anion secretion depends on the activity of the (also cAMP dependent) KCNQ1-KCNE3 K+ channel, but the secretory process survives after genetic inactivation of the K+ channel in the mouse. Here we use double mutant mice to investigate which alternative K+ channels come into action to compensate for the absence of KCNQ1-KCNE3 K+ channels. Our data establish that whilst Ca2+ -activated KCa 3.1 channels are not involved, K2P two-pore domain TASK-2 K+ channels are major players providing an alternative conductance to sustain the intestinal secretory process. Work with double mutant mice lacking both TASK-2 and KCNQ1-KCNE3 channels nevertheless points to yet-unidentified K+ channels that contribute to the robustness of the cAMP-activated anion secretion process. Abstract Anion and fluid secretion across the intestinal epithelium, a process altered in cystic fibrosis and secretory diarrhoea, is mediated by cAMP-activated CFTR Cl- channels and requires the simultaneous activity of basolateral K+ channels to maintain cellular ionic homeostasis and membrane potential. This function is fulfilled by the cAMP-activated K+ channel formed by the association of pore-forming KCNQ1 with its obligatory KCNE3 β-subunit. Studies using mice show sizeable cAMP-activated intestinal anion secretion in the absence of either KCNQ1 or KCNE3 suggesting that an alternative K+ conductance must compensate for the loss of KCNQ1-KCNE3 activity. We used double mutant mouse and pharmacological approaches to identify such a conductance. Ca2+ -dependent anion secretion can also be supported by Ca2+ -dependent KCa 3.1 channels after independent CFTR activation, but cAMP-dependent anion secretion is not further decreased in the combined absence of KCa 3.1 and KCNQ1-KCNE3 K+ channel activity. We show that the K2P K+ channel TASK-2 is expressed in the epithelium of the small and large intestine. Tetrapentylammonium, a TASK-2 inhibitor, abolishes anion secretory current remaining in the absence of KCNQ1-KCNE3 activity. A double mutant mouse lacking both KCNQ1-KCNE3 and TASK-2 showed a much reduced cAMP-mediated anion secretion compared to that observed in the single KCNQ1-KCNE3 deficient mouse. We conclude that KCNQ1-KCNE3 and TASK-2 play major roles in the intestinal anion and fluid secretory phenotype. The persistence of an, admittedly reduced, secretory activity in the absence of these two conductances suggests that further additional K+ channel(s) as yet unidentified contribute to the robustness of the intestinal anion secretory process.

Published

2017

7. Cellular mechanisms underlying the inhibitory effect of flufenamic acid on chloride secretion in human intestinal epithelial cells

Author

Vatcharin Rukachaisirikul, Chatchai Muanprasat, Varanuj Chatsudthipong, Chantapol Yimnual, and Pawin Pongkorpsakol

Subjects

Diarrhea, 0301 basic medicine, ATPase, AMP-Activated Protein Kinases, Potassium Channels, Calcium-Activated, 03 medical and health sciences, 0302 clinical medicine, Tolfenamic acid, Cholera, Chloride secretion, Chlorides, Chloride Channels, Cell Line, Tumor, Potassium Channel Blockers, medicine, Humans, Secretion, Intestinal Mucosa, Adenosine Triphosphatases, Pharmacology, Intestinal Secretions, biology, Chemistry, lcsh:RM1-950, Anti-Inflammatory Agents, Non-Steroidal, Sodium, NF-kappa B, Biological Transport, Epithelial Cells, KCNE3, Molecular biology, Flufenamic Acid, Intestines, Meclofenamic acid, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Flufenamic acid, Biochemistry, Chloride channel, biology.protein, Molecular Medicine, lipids (amino acids, peptides, and proteins), Cotransporter, 030217 neurology & neurosurgery, medicine.drug

Abstract

Intestinal Cl − secretion is involved in the pathogenesis of secretory diarrheas including cholera. We recently demonstrated that flufenamic acid (FFA) suppressed Vibrio cholerae El Tor variant-induced intestinal fluid secretion via mechanisms involving AMPK activation and NF-κB-suppression. The present study aimed to investigate the effect of FFA on transepithelial Cl − secretion in human intestinal epithelial (T84) cells. FFA inhibited cAMP-dependent Cl − secretion in T84 cell monolayers with IC 50 of ∼8 μM. Other fenamate drugs including tolfenamic acid, meclofenamic acid and mefenamic acid exhibited the same effect albeit with lower potency. FFA also inhibited activities of CFTR, a cAMP-activated apical Cl − channel, and KCNQ1/KCNE3, a cAMP-activated basolateral K + channel. Mechanisms of CFTR inhibition by FFA did not involve activation of its negative regulators. Interestingly, FFA inhibited Ca 2+ -dependent Cl − secretion with IC 50 of ∼10 μM. FFA inhibited activities of Ca 2+ -activated Cl − channels and K Ca 3.1, a Ca 2+ -activated basolateral K + channels, but had no effect on activities of Na + –K + –Cl − cotransporters and Na + –K + ATPases. These results indicate that FFA inhibits both cAMP and Ca 2+ -dependent Cl − secretion by suppressing activities of both apical Cl − channels and basolateral K + channels. FFA and other fenamate drugs may be useful in the treatment of secretory diarrheas.

Published

2017

8. Investigation of Structural Dynamics of the KCNE3 in a Lipid Bilayer Membrane using Site-Directed Spin Labeling EPR Spectroscopy

Author

William D. Carbo, Samuel Haralu, Gary A. Lorigan, Alberto Perez, Indra D. Sahu, and Matthew Scheyer

Subjects

Membrane, law, Chemistry, Dynamics (mechanics), Biophysics, KCNE3, Site-directed spin labeling, Electron paramagnetic resonance, Lipid bilayer, law.invention

Published

2021

9. Gating modulation of the KCNQ1 channel by KCNE proteins studied by voltage-clamp fluorometry

Author

Koichi Nakajo

Subjects

0301 basic medicine, endocrine system diseases, Voltage clamp, Gating, Review Article, lcsh:Physiology, 03 medical and health sciences, lcsh:QH301-705.5, Ion channel, 030102 biochemistry & molecular biology, lcsh:QP1-981, Chemistry, urogenital system, KCNE3, General Medicine, electrophysiology, Transmembrane protein, Potassium channel, lcsh:QC1-999, voltage sensor, Electrophysiology, 030104 developmental biology, Membrane protein, lcsh:Biology (General), auxiliary subunit, ion channel, Biophysics, lcsh:Physics, potassium channel

Abstract

The KCNQ1 channel is a voltage-dependent potassium channel and is ubiquitously expressed throughout the human body including the heart, lung, kidney, pancreas, intestine and inner ear. Gating properties of the KCNQ1 channel are modulated by KCNE auxiliary subunits. For example, the KCNQ1-KCNE1 channel produces a slowly-activating potassium current, while KCNE3 makes KCNQ1 a voltage-independent, constitutively open channel. Thus, physiological functions of KCNQ1 channels are greatly dependent on the type of KCNE protein that is co-expressed in that organ. It has long been debated how the similar single transmembrane KCNE proteins produce quite different gating behaviors. Recent applications of voltage-clamp fluorometry (VCF) for the KCNQ1 channel have shed light on this question. The VCF is a quite sensitive method to detect structural changes of membrane proteins and is especially suitable for tracking the voltage sensor domains of voltage-gated ion channels. In this short review, I will introduce how the VCF technique can be applied to detect structural changes and what have been revealed by the recent VCF applications to the gating modulation of KCNQ1 channels by KCNE proteins.

Published

2019

10. Association study in Mexican patients with thyrotoxic hypokalemic periodic paralysis

Author

Laura Elia Martinez‑Garza, Mario Arturo Bautista‑Medina, Hugo Leonid Gallardo‑Blanco, Jesús Zacarías Villarreal Pérez, Fernando J. Lavalle Gonzalez, and Ricardo Martín Cerda Flores

Subjects

genetic variant, medicine.medical_specialty, CACNA1s, hypokalemic periodic paralysis, Population, MUC1, association study, General Biochemistry, Genetics and Molecular Biology, Hypokalemic periodic paralysis, Internal medicine, Epidemiology, medicine, Genetic predisposition, General Pharmacology, Toxicology and Pharmaceutics, education, Genetic association, education.field_of_study, business.industry, General Neuroscience, Thyrotoxic periodic paralysis, Muscle weakness, Articles, General Medicine, Odds ratio, medicine.disease, thyrotoxic hypokalemic periodic paralysis, KCNE3, medicine.symptom, business, SCN4A

Abstract

Hypokalemic periodic paralysis type 1 (OMIM; HOKPP1) and type 2 (OMIM; HOKPP2) are diseases of the muscle characterized by episodes of painless muscle weakness, and is associated with low potassium blood levels. Hyperthyroidism has been associated with thyrotoxic periodic paralysis (TTPP) (OMIM; TTPP1 and TTPP2), and genetic susceptibility has been implicated. In the present study, the clinical and epidemiological characteristics of patients with TTPP are described, together with their association with genetic variants reported previously in other populations. A prospective and a retrospective search of the medical records of patients who attended the emergency department at the Hospital Universitario ‘Dr. Jose E. Gonzalez’ in Monterrey, Nuevo León, Mexico, and were diagnosed with TTPP was performed. A total of 16 gene variants in the genes MUC1, CACNA1S, KCNE3 and SCN4A, and nine ancestry informative markers (AIMs), were analysed by Multiplex TaqMan™ Open Array assay, and a genetic association study was performed. A total of 11 patients were recruited, comprising nine males and two females (age range, 19-52 years) and 64 control subjects. Only two cases (18%) had a previous diagnosis of hyperthyroidism; the rest were diagnosed subsequently with Graves' disease. Based on the analysis, two DNA variants were found to potentially confer an increased risk for TTPP: S1PR1 rs3737576 [odds ratio (OR), 4.38; 95% confidence interval (CI), 1.08-17.76] and AIM rs2330442 (OR, 4.50; 95% CI, 1.21-16.69), and one variant was suggested to be possibly associated with TTPP, namely MUC1 rs4072037 (OR, 3.08; 95% CI, 0.841-1.38). However, there were no statistically significant associations between any of the 24 DNA variants and TTPP in a population from northeast Mexico.

Published

2018

11. NMR resonance assignments and secondary structure of a mutant form of the human KCNE1 channel accessory protein that exhibits KCNE3-like function

Author

Charles R. Sanders and Cheryl L. Law

Subjects

chemistry.chemical_classification, 0303 health sciences, Nitrogen Isotopes, Chemical shift, 030303 biophysics, KCNE3, Voltage-gated potassium channel, Biochemistry, Transmembrane protein, Potassium channel, Protein Structure, Secondary, Article, Amino acid, 03 medical and health sciences, Ion homeostasis, chemistry, Structural Biology, Potassium Channels, Voltage-Gated, Biophysics, Humans, Mutant Proteins, Protons, Protein secondary structure, Nuclear Magnetic Resonance, Biomolecular, 030304 developmental biology

Abstract

KCNQ1 (Q1) is a voltage-gated potassium channel that is modulated by members of the KCNE family, the best-characterized being KCNE1 (E1) and KCNE3 (E3). The Q1/E1 complex generates a channel with delayed activation and increased conductance. This complex is expressed in cardiomyocytes where it provides the I(Ks) current that is critical for the repolarization phase of the cardiac action potential. The Q1/E3 complex, on the other hand, is expressed in epithelial cells of the colon and stomach, where it serves as a constitutively active leak channel to help maintain water and ion homeostasis. Studies show the single transmembrane segments (TMS) present in both E1 and E3 are essential to their distinct functions. More specifically, residues FTL located near the middle of the E1 TMS are essential for the delayed activation of Q1, while the corresponding TVG sites in E3 are critical for constitutive activation of the channel. Swapping these three residues leads to the switching of the functional properties for both Q1/E1(FTL➔TVG) and Q1/E3(TVG➔FTL) complexes. This work details the backbone assignments and chemical shifts for the E1(FTL➔TVG) mutant, as determined using a suite of 3D NMR experiments along with specific and inverse amino acid isotopic labeling. The completed assignments are being used, in conjunction with other NMR experiments, to generate a 3D structure of E1(FTL➔TVG). The results of TALOS-N analysis of the chemical shifts are reported here. The E1(FTL➔TVG) structure will be compared to the already available E1 and E3 structures to determine the roles that their TMS triplet motifs play in each protein to dictate their distinct channel-modulatory functions.

Published

2018

12. Role of SCN5A coding and non-coding sequences in Brugada syndrome onset: What’s behind the scenes?

Author

Khaldoun Ben Hamda, Diego Franco, Amelia Aránega, Amel Haj Khelil, Jemni Be. Chibani, Houria Daimi, Ali Neji, and Sabri Maaoui

Subjects

Genetics, Untranslated region, Candidate gene, Mutation, medicine.diagnostic_test, KCNE3, Biology, medicine.disease, Bioinformatics, medicine.disease_cause, SCN1B, medicine, Coding region, cardiovascular diseases, Genetic testing, Brugada syndrome

Abstract

Brugada syndrome (BrS) is a rare inherited cardiac arrhythmia associated with a high risk of sudden cardiac death (SCD) due to ventricular fibrillation (VF). BrS is characterized by coved-type ST-segment elevation in the right precordial leads (V1-V3) in the absence of structural heart disease. This pattern is spontaneous, or is unmasked by intravenous administration of Class I antiarrhythmic drugs. The SCN5A-encoded α-subunit of the NaV1.5 cardiac sodium channel has been linked to BrS, and mutations in SCN5A are identified in 15–30% of BrS cases. Genetic testing of BrS patients generally involves sequencing of protein-coding portions and flanking intronic regions of SCN5A, according to recent international guidelines. This excludes the regulatory untranslated regions (5’UTR and 3’UTR) from the routine genetic testing of BrS patients. We here screened the coding sequence, the flanking intronic regions as well as the 5’ and 3’UTR regions of SCN5A gene and further five candidate genes (GPD1L, SCN1B, KCNE3, SCN4B, and MOG1) in a Tunisian family diagnosed with Brugada syndrome.A new Q1000K mutation was identified on the SCN5A gene along with two common polymorphisms (H558R and D1819). Furthermore, multiple genetic variants were identified on the SCN5A 3’UTR, one of which is predicted to create additional microRNA (miRNAs) binding site for miR-1270. Additionally, we identified the hsa-miR-219a rs107822. No relevant coding sequence variant was identified in the remaining studied candidate genes. Although Q1000K is localized in the conserved binding site of MOG1 which predicts a functional consequence, this new mutation along with the additional variants were differentially distributed among the family members without any clear genotype-phenotype concordance. This gives extra evidences about the complexity of the disease and suggests that the occurrence and prognosis of BrS is most likely controlled by a combination of multiple genetic factors and exposures, rather than a single polymorphism/mutation. Most SCN5A polymorphisms were localized in non-coding regions hypothesizing an impact on the miRNA-target complementarities. In this regard, over-expression of miR-1270 led to a significant decrease of luciferase activity suggesting a direct role regulating SCN5A. Therefore, genetic variants that disrupt its binding affinity to SCN5A 3’UTR and/or its expression might cause loss of normal repression control and be associated to BrS.

Published

2017

13. KCNE1 and KCNE3 modulate KCNQ1 channels by affecting different gating transitions

Author

Rosamary Ramentol, Sara I. Liin, Rene Barro-Soria, Robert S. Kass, Marta E. Perez, and H. Peter Larsson

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Patch-Clamp Techniques, endocrine system diseases, Voltage clamp, Biophysics, Action Potentials, Gating, Membrane Potentials, Xenopus laevis, 03 medical and health sciences, chemistry.chemical_compound, Internal medicine, medicine, Animals, Humans, Repolarization, Phosphatidylinositol, Multidisciplinary, urogenital system, KCNE3, Cardiac action potential, Coupling (electronics), 030104 developmental biology, Endocrinology, PNAS Plus, chemistry, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, cardiovascular system, Mutagenesis, Site-Directed, Oocytes, Ion Channel Gating, AND gate

Abstract

KCNE β-subunits assemble with and modulate the properties of voltage-gated K+ channels. In the heart, KCNE1 associates with the α-subunit KCNQ1 to generate the slowly activating, voltage-dependent potassium current (IKs) in the heart that controls the repolarization phase of cardiac action potentials. By contrast, in epithelial cells from the colon, stomach, and kidney, KCNE3 coassembles with KCNQ1 to form K+ channels that are voltage-independent K+ channels in the physiological voltage range and important for controlling water and salt secretion and absorption. How KCNE1 and KCNE3 subunits modify KCNQ1 channel gating so differently is largely unknown. Here, we use voltage clamp fluorometry to determine how KCNE1 and KCNE3 affect the voltage sensor and the gate of KCNQ1. By separating S4 movement and gate opening by mutations or phosphatidylinositol 4,5-bisphosphate depletion, we show that KCNE1 affects both the S4 movement and the gate, whereas KCNE3 affects the S4 movement and only affects the gate in KCNQ1 if an intact S4-to-gate coupling is present. Further, we show that a triple mutation in the middle of the transmembrane (TM) segment of KCNE3 introduces KCNE1-like effects on the second S4 movement and the gate. In addition, we show that differences in two residues at the external end of the KCNE TM segments underlie differences in the effects of the different KCNEs on the first S4 movement and the voltage sensor-to-gate coupling.

Published

2017

14. Molecular Basis and Differentiation-Associated Alterations of Anion Secretion in Human Duodenal Enteroid Monolayers

Author

Jennifer Foulke-Abel, Mark Donowitz, Hugo R. de Jonge, Jianyi Yin, Chung Ming Tse, Leela Rani Avula, Varsha Singh, and Gastroenterology & Hepatology

Subjects

0301 basic medicine, Hepatology, biology, Ussing chamber, Chemistry, Gastroenterology, KCNE3, Molecular biology, Cystic fibrosis transmembrane conductance regulator, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Carbonic anhydrase, Extracellular, biology.protein, lcsh:Diseases of the digestive system. Gastroenterology, Secretion, Triphosphatase, lcsh:RC799-869, Ion transporter

Abstract

Background & Aims: Human enteroids present a novel tool to study human intestinal ion transport physiology and pathophysiology. The present study describes the contributions of Cl- and HCO3- secretion to total cyclic adenosine monophosphate (cAMP)-stimulated electrogenic anion secretion in human duodenal enteroid monolayers and the relevant changes after differentiation. Methods: Human duodenal enteroids derived from 4 donors were grown as monolayers and differentiated by a protocol that includes the removal of Wnt3A, R-spondin1, and SB202190 for 5 days. The messenger RNA level and protein expression of selected ion transporters and carbonic anhydrase isoforms were determined by quantitative real-time polymerase chain reaction and immunoblotting, respectively. Undifferentiated and differentiated enteroid monolayers were mounted in the Ussing chamber/voltage-current clamp apparatus, using solutions that contained as well as lacked Cl- and HCO3-/CO2, to determine the magnitude of forskolin-induced short-circuit current change and its sensitivity to specific inhibitors that target selected ion transporters and carbonic anhydrase(s). Results: Differentiation resulted in a significant reduction in the messenger RNA level and protein expression of cystic fibrosis transmembrane conductance regulator, (CFTR) Na+/K+/2Cl- co-transporter 1 (NKCC1), and potassium channel, voltage gated, subfamily E, regulatory subunit 3 (KCNE3); and, conversely, increase of down-regulated-in-adenoma (DRA), electrogenic Na+/HCO3- co-transporter 1 (NBCe1), carbonic anhydrase 2 (CA2), and carbonic anhydrase 4 (CA4). Both undifferentiated and differentiated enteroids showed active cAMP-stimulated anion secretion that included both Cl- and HCO3- secretion as the magnitude of total active anion secretion was reduced after the removal of extracellular Cl- or HCO3-/CO2. The magnitude of total anion secretion in differentiated enteroids was approximately 33% of that in undifferentiated enteroids, primarily owing to the reduction in Cl- secretion with no significant change in HCO3- secretion. Anion secretion was consistently lower but detectable in differentiated enteroids compared with undifferentiated enteroids in the absence of extracellular Cl- or HCO3-/CO2. Inhibiting CFTR, NKCC1, carbonic anhydrase(s), cAMP-activated K+ channel(s), and Na+/K+-adenosine triphosphatase reduced cAMP-stimulated anion secretion in both undifferentiated and differentiated enteroids. Conclusions: Human enteroids recapitulate anion secretion physiology of small intestinal epithelium. Enteroid differentiation is associated with significant alterations in the expression of several ion transporters and carbonic anhydrase isoforms, leading to a reduced but preserved anion secretory phenotype owing to markedly reduced Cl- secretion but no significant change in HCO3- secretion. Keywords: Chloride Secretion, Bicarbonate Secretion, DRA, Ion Transport

Published

2017

15. Structural Basis of Human KCNQ1 Modulation and Gating

Author

Ji Sun and Roderick MacKinnon

Subjects

Phosphatidylinositol 4,5-Diphosphate, Conformational change, Patch-Clamp Techniques, Gating, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Membrane Potentials, 03 medical and health sciences, 0302 clinical medicine, Humans, Glucose homeostasis, Inner membrane, Secretion, 030304 developmental biology, 0303 health sciences, Cryoelectron Microscopy, KCNE3, Membrane, Membrane protein, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, Biophysics, lipids (amino acids, peptides, and proteins), Ion Channel Gating, 030217 neurology & neurosurgery

Abstract

KCNQ1, also known as Kv7.1, is a voltage-dependent K+ channel that regulates gastric acid secretion, salt and glucose homeostasis, and heart rhythm. Its functional properties are regulated in a tissue-specific manner through co-assembly with beta subunits KCNE1-5. In non-excitable cells, KCNQ1 forms a complex with KCNE3, which suppresses channel closure at negative membrane voltages that otherwise would close it. Pore opening is regulated by the signaling lipid PIP2. Using cryoelectron microscopy (cryo-EM), we show that KCNE3 tucks its single-membrane-spanning helix against KCNQ1, at a location that appears to lock the voltage sensor in its depolarized conformation. Without PIP2, the pore remains closed. Upon addition, PIP2 occupies a site on KCNQ1 within the inner membrane leaflet, which triggers a large conformational change that leads to dilation of the pore's gate. It is likely that this mechanism of PIP2 activation is conserved among Kv7 channels.

Published

2020

16. Gain-of-function mutations in potassium channel subunit KCNE2 associated with early-onset lone atrial fibrillation

Author

Jonas B. Nielsen, Stig Haunsø, Nicole Schmitt, Jens-Peter David, Bo Hjorth Bentzen, Søren-Peter Olesen, Morten S. Olesen, and Jesper Hastrup Svendsen

Subjects

Adult, Male, Nonsynonymous substitution, medicine.medical_specialty, DNA Mutational Analysis, Clinical Biochemistry, Mutation, Missense, Blood Pressure, CHO Cells, Cricetulus, Cricetinae, Internal medicine, Atrial Fibrillation, Drug Discovery, medicine, Animals, Humans, Missense mutation, Genetic Predisposition to Disease, Amino Acid Sequence, Allele, Alleles, Microscopy, Confocal, Base Sequence, biology, business.industry, Biochemistry (medical), KCNE2, Cardiac arrhythmia, KCNE3, Atrial fibrillation, medicine.disease, Potassium channel, Endocrinology, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, biology.protein, Cardiology, Female, business

Abstract

Aims: Atrial fibrillation (AF) is the most common cardiac arrhythmia. Disturbances in cardiac potassium conductance are considered as one of the disease mechanisms in AF. We aimed to investigate if mutations in potassium-channel β-subunits KCNE2 and KCNE3 are associated with early-onset lone AF. Methods & results: The coding regions of KCNE2 and KCNE3 were bidirectionally sequenced in 192 unrelated patients diagnosed with early-onset lone AF (V7.1, KV11.1, KV4.3 and KV1.5. A significant gain-of-function effect was observed upon coexpression with KV7.1 and KV7.1 + KCNE1. Confocal imaging found no differences in subcellular localization. No disease-suspected mutations were identified in KCNE3. Conclusion: We identified two KCNE2 gain-of-function missense mutations that seem to increase the susceptibility of early-onset lone AF. These results confirm previous findings indicating that gain-of-function in the slow delayed rectifier potassium current might be involved in the pathogenesis of AF.

Published

2014

17. Kcne3 deletion initiates extracardiac arrhythmogenesis in mice

Author

Ritu Kant, Zhaoyang Hu, Shawn M. Crump, Geoffrey W. Abbott, Marie Anand, and Roberto Levi

Subjects

Male, medicine.medical_specialty, Potassium Channels, Microarray, Long QT syndrome, Biology, Real-Time Polymerase Chain Reaction, Biochemistry, Research Communications, Pathogenesis, Electrocardiography, Mice, chemistry.chemical_compound, Internal medicine, Gene expression, Genetics, medicine, Animals, Aldosterone, Molecular Biology, medicine.diagnostic_test, Arrhythmias, Cardiac, KCNE3, medicine.disease, Mice, Mutant Strains, Potassium channel, Endocrinology, chemistry, Potassium Channels, Voltage-Gated, cardiovascular system, Female, Biotechnology

Abstract

Mutations in the human KCNE3 potassium channel ancillary subunit gene are associated with life-threatening ventricular arrhythmias. Most genes underlying inherited cardiac arrhythmias, including KCNE3, are not exclusively expressed in the heart, suggesting potentially complex disease etiologies. Here we investigated mechanisms of KCNE3-linked arrhythmogenesis in Kcne3−/− mice using real-time qPCR, echo- and electrocardiography, ventricular myocyte patch-clamp, coronary artery ligation/reperfusion, blood analysis, cardiac synaptosome exocytosis, microarray and pathway analysis, and multitissue histology. Kcne3 transcript was undetectable in adult mouse atria, ventricles, and adrenal glands, but Kcne3−/− mice exhibited 2.3-fold elevated serum aldosterone (P=0.003) and differentially expressed gene networks consistent with an adrenal-targeted autoimmune response. Furthermore, 8/8 Kcne3−/− mice vs. 0/8 Kcne3+/+ mice exhibited an activated-lymphocyte adrenal infiltration (P=0.0002). Kcne3 deletion also caused aldosterone-dependent ventricular repolarization delay (19.6% mean QTc prolongation in females; P

Published

2013

18. KCNQ and KCNE potassium channel subunit expression in bovine retinal pigment epithelium

Author

Bret A. Hughes and Xiaoming Zhang

Subjects

Retina, Retinal pigment epithelium, Protein subunit, KCNE3, Retinal, KCNE4, Biology, Molecular biology, eye diseases, Sensory Systems, Blot, Cellular and Molecular Neuroscience, Ophthalmology, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, medicine, biology.protein, sense organs, Outer nuclear layer

Abstract

Human, monkey, and bovine retinal pigment epithelial (RPE) cells exhibit an M-type K+ current, which in many other cell types is mediated by channels composed of KCNQ α-subunits and KCNE auxiliary subunits. Recently, we demonstrated the expression of KCNQ1, KCNQ4, and KCNQ5 in the monkey RPE. Here, we investigated the expression of KCNQ and KCNE subunits in native bovine RPE. RT-PCR analysis revealed the expression of KCNQ1, KCNQ4, and KCNQ5 transcripts in the RPE, but, in Western blot analysis of RPE plasma membranes, only KCNQ5 was detected. Among the five members of the KCNE gene family, transcripts for KCNE1, KCNE2, KCNE3, and KCNE4 were detected in bovine RPE, but only KCNE1 and KCNE2 proteins were detected. Immunohistochemistry of frozen bovine retinal sections revealed KCNE1 expression near the apical and basal membranes of the RPE, in cone outer segments, in the outer nuclear layer, and throughout the inner retina. The localization of KCNE1 in the RPE basal membrane, where KCNQ5 was previously found to be present, suggests that this β-subunit may contribute to M-type K(+) channels in this membrane.

Published

2013

19. Dynamic subunit stoichiometry confers a progressive continuum of pharmacological sensitivity by KCNQ potassium channels

Author

Haibo Yu, Cecile Terrenoire, Beiyan Zou, Meng Wu, Zhihong Lin, Hongkang Zhang, Robert S. Kass, Min Li, Craig W. Lindsley, Margrith E. Mattmann, Owen B. McManus, and Corey R. Hopkins

Subjects

endocrine system diseases, Protein subunit, Action Potentials, Muscle Proteins, CHO Cells, Gating, Tosyl Compounds, Cricetulus, Piperidines, Tetramer, Cricetinae, Animals, Humans, Myocytes, Cardiac, Ion transporter, Ion Transport, Multidisciplinary, urogenital system, Chemistry, HEK 293 cells, KCNE3, Biological Sciences, Potassium channel, Transmembrane protein, Thiazoles, HEK293 Cells, Biochemistry, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, Potassium, Biophysics, Protein Multimerization

Abstract

Voltage-gated KCNQ1 (Kv7.1) potassium channels are expressed abundantly in heart but they are also found in multiple other tissues. Differential coassembly with single transmembrane KCNE beta subunits in different cell types gives rise to a variety of biophysical properties, hence endowing distinct physiological roles for KCNQ1–KCNEx complexes. Mutations in either KCNQ1 or KCNE1 genes result in diseases in brain, heart, and the respiratory system. In addition to complexities arising from existence of five KCNE subunits, KCNE1 to KCNE5, recent studies in heterologous systems suggest unorthodox stoichiometric dynamics in subunit assembly is dependent on KCNE expression levels. The resultant KCNQ1–KCNE channel complexes may have a range of zero to two or even up to four KCNE subunits coassembling per KCNQ1 tetramer. These findings underscore the need to assess the selectivity of small-molecule KCNQ1 modulators on these different assemblies. Here we report a unique small-molecule gating modulator, ML277, that potentiates both homomultimeric KCNQ1 channels and unsaturated heteromultimeric (KCNQ1) 4 (KCNE1) n ( n < 4) channels. Progressive increase of KCNE1 or KCNE3 expression reduces efficacy of ML277 and eventually abolishes ML277-mediated augmentation. In cardiomyocytes, the slowly activating delayed rectifier potassium current, or I Ks , is believed to be a heteromultimeric combination of KCNQ1 and KCNE1, but it is not entirely clear whether I Ks is mediated by KCNE-saturated KCNQ1 channels or by channels with intermediate stoichiometries. We found ML277 effectively augments I Ks current of cultured human cardiomyocytes and shortens action potential duration. These data indicate that unsaturated heteromultimeric (KCNQ1) 4 (KCNE1) n channels are present as components of I Ks and are pharmacologically distinct from KCNE-saturated KCNQ1–KCNE1 channels.

Published

2013

20. Regulation of human cardiac potassium channels by full-length KCNE3 and KCNE4

Author

Geoffrey W. Abbott

Subjects

0301 basic medicine, Potassium Channels, Xenopus, Action Potentials, 030204 cardiovascular system & hematology, Cardiovascular, Xenopus laevis, Mice, 0302 clinical medicine, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Protein Isoforms, 2.1 Biological and endogenous factors, Myocytes, Cardiac, Transgenes, Aetiology, Multidisciplinary, biology, Chemistry, Voltage-Gated, KCNE3, Cardiac action potential, Kv Channel-Interacting Proteins, KCNE4, Potassium channel, Cell biology, Other Physical Sciences, Shal Potassium Channels, Heart Disease, Potassium Channels, Voltage-Gated, cardiovascular system, Cardiac, Signal Transduction, Protein subunit, Heart Ventricles, hERG, Primary Cell Culture, CHO Cells, Article, 03 medical and health sciences, Cricetulus, Animals, Humans, Heart Atria, Kv1.1 Potassium Channel, Myocytes, biology.organism_classification, Protein Subunits, 030104 developmental biology, Gene Expression Regulation, biology.protein, Oocytes, Biochemistry and Cell Biology

Abstract

Voltage-gated potassium (Kv) channels comprise pore-forming α subunits and a multiplicity of regulatory proteins, including the cardiac-expressed and cardiac arrhythmia-linked transmembrane KCNE subunits. After recently uncovering novel, N-terminally extended (L) KCNE3 and KCNE4 isoforms and detecting their transcripts in human atrium, reported here are their functional effects on human cardiac Kv channel α subunits expressed in Xenopus laevis oocytes. As previously reported for short isoforms KCNE3S and KCNE4S, KCNE3L inhibited hERG; KCNE4L inhibited Kv1.1; neither form regulated the HCN1 pacemaker channel. Unlike KCNE4S, KCNE4L was a potent inhibitor of Kv4.2 and Kv4.3; co-expression of cytosolic β subunit KChIP2, which regulates Kv4 channels in cardiac myocytes, partially relieved Kv4.3 but not Kv4.2 inhibition. Inhibition of Kv4.2 and Kv4.3 by KCNE3L was weaker, and its inhibition of Kv4.2 abolished by KChIP2. KCNE3L and KCNE4L also exhibited subunit-specific effects on Kv4 channel complex inactivation kinetics, voltage dependence and recovery. Further supporting the potential physiological significance of the robust functional effects of KCNE4L on Kv4 channels, KCNE4L protein was detected in human atrium, where it co-localized with Kv4.3. The findings establish functional effects of novel human cardiac-expressed KCNE isoforms and further contribute to our understanding of the potential mechanisms influencing cardiomyocyte repolarization.

Published

2016

21. Structural basis for KCNE3 modulation of potassium recycling in epithelia

Author

Carlos G. Vanoye, Jarrod A. Smith, Brett M. Kroncke, Alfred L. George, Keenan C. Taylor, Charles R. Sanders, Richard Welch, Nicholas J. Sisco, CongBao Kang, Wade D. Van Horn, D.P. Nannemann, Jens Meiler, and Yuanli Song

Subjects

0301 basic medicine, Cystic Fibrosis, Protein domain, channel, Biochemistry, 03 medical and health sciences, Protein Domains, Chloride Channels, estrogen, integrative modeling, Animals, Humans, Research Articles, Ion channel, Multidisciplinary, KCNQ1, Kv7.1, 030102 biochemistry & molecular biology, Chemistry, potassium, Computational Biology, SciAdv r-articles, Epithelial Cells, KCNE3, NMR, Electrophysiological Phenomena, Transmembrane domain, Electrophysiology, 030104 developmental biology, Membrane protein, Structural biology, Potassium Channels, Voltage-Gated, Multiprotein Complexes, KCNQ1 Potassium Channel, Chloride channel, Biophysics, Research Article

Abstract

KCNE3 modulates the KCNQ1 K+ channel in epithelia by directly stabilizing the voltage-sensor S4 segment in its activated state., The single-span membrane protein KCNE3 modulates a variety of voltage-gated ion channels in diverse biological contexts. In epithelial cells, KCNE3 regulates the function of the KCNQ1 potassium ion (K+) channel to enable K+ recycling coupled to transepithelial chloride ion (Cl−) secretion, a physiologically critical cellular transport process in various organs and whose malfunction causes diseases, such as cystic fibrosis (CF), cholera, and pulmonary edema. Structural, computational, biochemical, and electrophysiological studies lead to an atomically explicit integrative structural model of the KCNE3-KCNQ1 complex that explains how KCNE3 induces the constitutive activation of KCNQ1 channel activity, a crucial component in K+ recycling. Central to this mechanism are direct interactions of KCNE3 residues at both ends of its transmembrane domain with residues on the intra- and extracellular ends of the KCNQ1 voltage-sensing domain S4 helix. These interactions appear to stabilize the activated “up” state configuration of S4, a prerequisite for full opening of the KCNQ1 channel gate. In addition, the integrative structural model was used to guide electrophysiological studies that illuminate the molecular basis for how estrogen exacerbates CF lung disease in female patients, a phenomenon known as the “CF gender gap.”

Published

2016

22. Mechanisms of KCNE Beta Subunit Modulation of Voltage Sensing and Gating in KCNQ1 Channels

Author

Peter Larsson

Subjects

endocrine system diseases, biology, urogenital system, Chemistry, Voltage clamp, Analytical chemistry, Biophysics, KCNE2, KCNE3, Gating, Potassium channel, Coupling (electronics), biology.protein, Beta (finance), ATP synthase alpha/beta subunits

Abstract

KCNQ1 (Kv7.1) channels are expressed in different tissues and exhibit different gating behaviors in these different tissues. In the heart, KCNQ1 channels are coexpressed with KCNE1 beta subunits and form slowly activating, voltage-gated potassium channels, whereas in epithelial cells KCNQ1 are coexpressed with KCNE2 or KCNE3 beta subunits and form potassium channels that appear voltage-independent. We have used voltage clamp fluorometry (VCF) to elucidate the gating mechanism in KCNQ1 channels and the effects of KCNE beta subunits on KCNQ1 gating. Voltage clamp fluorometry allows us to follow both voltage sensor movement and gate opening simultaneously, thereby better understand the relationship of voltage sensor movement and channel opening in these channels. We show that the voltage sensor S4 moves and the gate closes in KCNQ1/KCNE3 channels, but only at very negative voltages. By decoupling the voltage sensor and the gate, we show that KCNE3 mainly affects the voltage sensor and only indirectly affects the pore through the voltage-sensor-to-gate coupling. The KCNE3 seems to affect the voltage sensor S4 via an electrostatic interactions between negatively charged KCNE3 residues and positively charged S4 residues. Our data suggests that KCNE1 and KCNE3 affect different domains of KCNQ1, thereby resulting in very different modulations of KCNQ1 voltage gating. KCNE1 affects both the voltage-sensing domain and the pore-gate domain, whereas KCNE3 affects mainly the voltage-sensing domain. That different KCNE beta subunits affect different domains of KCNQ1 explains how two highly similar KCNE beta subunits have so different effects on KCNQ1 gating.

Published

2016

23. Structural Analysis of KCNE1 Transmembrane Mutant Yielding KCNE3-Like Function

Author

Cheryl L. Law and Charles R. Sanders

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Chemistry, Mutant, Biophysics, Conductance, Pulse sequence, KCNE3, Nuclear magnetic resonance spectroscopy, Transmembrane protein, Potassium channel, Crystallography, Docking (molecular), cardiovascular system

Abstract

The KCNE family contains five single transmembrane-spanning proteins that modulate the voltage-gated potassium channel, KCNQ1 and provide functional diversity to the KCNQ1 channel. For example, KCNE1 modulates the KCNQ1 channel by slowing its activation and increasing its conductance. The KCNE3 protein also increases the conductance, but induces constitutive activation of the channel. In 2001, Melman et al made a series of KCNE1 and KCNE3 chimeras, and identified the transmembrane region as key to distinct functions of KCNE1 and KCNE3. They showed that by swapping three transmembrane residues, T71V72G73, of KCNE3 for KCNE1, F57T58L59, to create a KCNE1/3 chimera they could create a current trace similar to KCNE3 and eliminate KCNE1's ability to delay opening. Thus, KCNE1 with TVG from KCNE3 yields a constitutively active channel without a delay in opening. We hypothesize that this is due to changes in flexibility of the transmembrane-helix of KCNE1 when TVG triple mutation is present. By using NMR spectroscopy, biochemical studies, and computational docking, we aim to look at structural and conformational differences between KCNE1 and KCNE1TVG. We have expressed and purified KCNE1TVG for NMR studies and collected 2D-NMR spectra using a TROSY-based pulse sequence. Partial backbone assignments of KCNE1TVG have been determined by aligning and transfer assignments of the WT KCNE1 previous determined in our lab. Further 3D experiments have been carried out to complete assignments. Further NMR studied will be done to structurally determine KCNE1TVG. Computational models of KCNE1TVG/KCNQ1 in the open and closed state will be created. These models, along with working models for KCNQ1/KCNE1 will provide insight into how KCNE1TVG interacts with the channel differently and similarly than both KCNE1 and KCNE3. This will provide insight into how KCNE1TVG interacts with the channel differently and similarly than both KCNE1 and KCNE3.

Published

2016

24. Increased aldosterone-dependent Kv1.5 recycling predisposes to pacing-induced atrial fibrillation in Kcne3-/- mice

Author

Nicola Wilck, Burkert Pieske, Clemens Koehncke, Ulrike Lisewski, Bastian Buschmeyer, and Torsten K. Roepke

Subjects

0301 basic medicine, medicine.medical_specialty, Patch-Clamp Techniques, 030204 cardiovascular system & hematology, Spironolactone, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Kv1.5 Potassium Channel, Mice, 0302 clinical medicine, Internal medicine, Adrenal Glands, Atrial Fibrillation, Hyperaldosteronism, Genetics, medicine, Animals, Myocytes, Cardiac, Molecular Biology, Protein kinase B, Aldosterone, Mice, Knockout, business.industry, GTPase-Activating Proteins, Membrane Proteins, Atrial fibrillation, KCNE3, medicine.disease, Electrophysiological Phenomena, Electrophysiology, 030104 developmental biology, Endocrinology, chemistry, Gene Expression Regulation, Potassium Channels, Voltage-Gated, rab GTP-Binding Proteins, Phosphorylation, business, Proto-Oncogene Proteins c-akt, Biotechnology

Abstract

Hyperaldosteronism is associated with an increased prevalence of atrial fibrillation (AF). Mutations in KCNE3 have been associated with AF, and Kcne3(-/-) mice exhibit hyperaldosteronism. In this study, we used recently developed Kcne3(-/-) mice to study atrial electrophysiology with respect to development of aldosterone-dependent AF. In invasive electrophysiology studies, Kcne3(-/-) mice displayed a reduced atrial effective refractory period (AERP) and inducible episodes of paroxysmal AF. The cellular arrhythmogenic correlate for AF predisposition was a significant increase in atrial Kv currents generated by the micromolar 4-aminopyridine-sensitive Kv current encoded by Kv1.5. Electrophysiological alterations in Kcne3(-/-) mice were aldosterone dependent and were associated with increased Rab4, -5, and -9-dependent recycling of Kv1.5 channels to the Z-disc/T-tubulus region and lateral membrane via activation of the Akt/AS160 pathway. Treatment with spironolactone inhibited Akt/AS160 phosphorylation, reduced Rab-dependent Kv1.5 recycling, normalized AERP and atrial Kv currents to the wild-type level, and reduced arrhythmia induction in Kcne3(-/-) mice. Kcne3 deletion in mice predisposes to AF by a heretofore unrecognized mechanism-namely, increased aldosterone-dependent Kv1.5 recycling via Rab GTPases. The findings uncover detailed molecular mechanisms underpinning a channelopathy-linked form of AF and emphasize the inevitability of considering extracardiac mechanisms in genetic arrhythmia syndromes.-Lisewski, U., Koehncke, C., Wilck, N., Buschmeyer, B., Pieske, B., Roepke, T. K. Increased aldosterone-dependent Kv1.5 recycling predisposes to pacing-induced atrial fibrillation in Kcne3(-/-) mice.

Published

2016

25. Targeting of Kv7.5 (KCNQ5)/KCNE channels to surface microdomains of cell membranes

Author

Meritxell Roura-Ferrer, Laura Solé, Antonio Felipe, Núria Comes, Anna Oliveras, and Alvaro Villarroel

Subjects

Physiology, HEK 293 cells, Fluorescence recovery after photobleaching, Skeletal muscle, KCNE3, Biology, Potassium channel, law.invention, Cell biology, Cellular and Molecular Neuroscience, Membrane, medicine.anatomical_structure, Confocal microscopy, law, Physiology (medical), medicine, Neurology (clinical), Lipid raft

Abstract

Background: Kv7.5 (KCNQ5) channels conduct M-type potassium currents in the brain, are expressed in skeletal muscle, and contribute to vascular muscle tone. Methods: We coexpressed Kv7.5 and KCNE1–3 peptides in HEK293 cells and then analyzed their association using electrophysiology and co-immunoprecipitation, assessed localization using confocal microscopy, examined targeting of the oligomeric channels to cholesterol-rich membrane surface microdomains using lipid raft isolation, and evaluated their membrane dynamics using fluorescence recovery after photobleaching (FRAP). Results: Kv7.5 forms oligomeric channels specifically with KCNE1 and KCNE3. The expression of Kv7.5 targeted to cholesterol-rich membrane surface microdomains was very low. Oligomeric Kv7.5/KCNE1 and Kv7.5/KCNE3 channels did not localize to lipid rafts. However, Kv7.5 association impaired KCNE3 expression in lipid raft microdomains. Conclusions: Our results indicate that Kv7.5 contributes to the spatial regulation of KCNE3. This new scenario could greatly assist in determining the physiological relevance of putative KCNE3 interactions in nerve and muscle. Muscle Nerve 45: 48–54, 2012

Published

2011

26. Sexual dimorphism and oestrogen regulation of KCNE3 expression modulates the functional properties of KCNQ1 K+channels

Author

Fiona O'Mahony, Rodrigo Alzamora, Francisco V. Sepúlveda, Raphael Rapetti-Mauss, Brian J. Harvey, Valerie Urbach, Viviana Bustos, and L. Pablo Cid

Subjects

0303 health sciences, Messenger RNA, medicine.medical_specialty, endocrine system diseases, biology, urogenital system, Physiology, KCNE2, KCNE3, Gating, Epithelium, Potassium channel, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, medicine.anatomical_structure, Intestinal mucosa, Internal medicine, medicine, biology.protein, Patch clamp, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The KCNQ1 potassium channel associates with various KCNE ancillary subunits that drastically affect channel gating and pharmacology. Co-assembly with KCNE3 produces a current with nearly instantaneous activation, some time-dependent activation at very positive potentials, a linear current-voltage relationship and a 10-fold higher sensitivity to chromanol 293B. KCNQ1:KCNE3 channels are expressed in colonic crypts and mediate basolateral K(+) recycling required for Cl(-) secretion. We have previously reported the female-specific anti-secretory effects of oestrogen via KCNQ1:KCNE3 channel inhibition in colonic crypts. This study was designed to determine whether sex and oestrogen regulate the expression and function of KCNQ1 and KCNE3 in rat distal colon. Colonic crypts were isolated from Sprague-Dawley rats and used for whole-cell patch-clamp and to extract total RNA and protein. Sheets of epithelium were used for short-circuit current recordings. KCNE1 and KCNE3 mRNA and protein abundance were significantly higher in male than female crypts. No expression of KCNE2 was found and no difference was observed in KCNQ1 expression between male and female (at oestrus) colonic crypts. Male crypts showed a 2.2-fold higher level of association of KCNQ1 and KCNE3 compared to female cells. In female colonic crypts, KCNQ1 and KCNE3 protein expression fluctuated throughout the oestrous cycle and 17β-oestradiol (E2 10 nM) produced a rapid (

Published

2011

27. Impact of KCNE subunits on KCNQ1 (Kv7.1) channel membrane surface targeting

Author

Antonio Felipe, Núria Comes, Rinat Dahan, Alvaro Villarroel, Meritxell Roura-Ferrer, Laura Solé, Anna Oliveras, and Joanna Bielanska

Subjects

endocrine system diseases, Physiology, Recombinant Fusion Proteins, Protein subunit, Clinical Biochemistry, Context (language use), Biology, Transfection, Cell Line, Membrane Microdomains, Humans, Lipid raft, Microscopy, Confocal, urogenital system, Fluorescence recovery after photobleaching, KCNE2, KCNE3, Cell Biology, Cell biology, Transport protein, Kinetics, Protein Subunits, Protein Transport, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, biology.protein, lipids (amino acids, peptides, and proteins), Fluorescence Recovery After Photobleaching

Abstract

The KCNQ1 (Kv7.1) channel plays an important role in cardiovascular physiology. Cardiomyocytes co-express KCNQ1 with KCNE1-5 proteins. KCNQ1 may co-associate with multiple KCNE regulatory subunits to generate different biophysically and pharmacologically distinct channels. Increasing evidence indicates that the location and targeting of channels are important determinants of their function. In this context, the presence of K(+) channels in sphingolipid-cholesterol-enriched membrane microdomains (lipid rafts) is under investigation. Lipid rafts are important for cardiovascular functioning. We aimed to determine whether KCNE subunits modify the localization and targeting of KCNQ1 channels in lipid rafts microdomains. HEK-293 cells were transiently transfected with KCNQ1 and KCNE1-5, and their traffic and presence in lipid rafts were analyzed. Only KCNQ1 and KCNE3, when expressed alone, co-localized in raft fractions. In addition, while KCNE2 and KCNE5 notably stained the cell surface, KCNQ1 and the rest of the KCNEs showed strong intracellular retention. KCNQ1 targets multiple membrane surface microdomains upon association with KCNE peptides. Thus, while KCNQ1/KCNE1 and KCNQ1/KCNE2 channels target lipid rafts, KCNQ1 associated with KCNE3-5 did not. Channel membrane dynamics, analyzed by fluorescence recovery after photobleaching (FRAP) experiments, further supported these results. In conclusion, the trafficking and targeting pattern of KCNQ1 can be influenced by its association with KCNEs. Since KCNQ1 is crucial for cardiovascular physiology, the temporal and spatial regulations that different KCNE subunits may confer to the channels could have a dramatic impact on membrane electrical activity and putative endocrine regulation.

Published

2010

28. Increased KCNJ18 promoter activity as a mechanism in atypical normokalemic periodic paralysis

Author

Richard C Dodel, Guenter F. Pilz, Susanne Rinné, Bilgen Kurt, Andreas Maieron, Muhidien Soufi, Juergen R. Schaefer, Tobias Mueller, Niels Decher, and Volker Ruppert

Subjects

0301 basic medicine, Candidate gene, Chemistry, HEK 293 cells, Periodic paralysis, KCNE3, Transfection, medicine.disease, Molecular biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Extracellular, medicine, Luciferase, Neurology (clinical), Gene, 030217 neurology & neurosurgery, Genetics (clinical)

Abstract

ObjectiveTo identify the genetic basis of a patient with symptoms of normokalemic sporadic periodic paralysis (PP) and to study the effect of KCNJ18 mutations.MethodsA candidate gene approach was used to identify causative gene mutations, using Sanger sequencing. KCNJ18 promoter activity was analyzed in transfected HEK293 cells with a luciferase assay, and functional analysis of Kir2.6 channels was performed with the two-electrode voltage-clamp technique.ResultsAlthough we did not identify harmful mutations in SCN4A, CACNA1S, KCNJ2 and KCNE3, we detected a monoallelic four-fold variant in KCNJ18 (R39Q/R40H/A56E/I249V), together with a variant in the respective promoter of this channel (c.-542T/A). The exonic variants in Kir2.6 did not alter the channel function; however, luciferase assays revealed a 10-fold higher promoter activity of the c.-542A promoter construct, which is likely to cause a gain-of-function by increased expression of Kir2.6. We found that reducing extracellular K+ levels causes a paradoxical reduction in outward currents, similar to that described for other inward rectifying K+ channels. Thus, reducing the extracellular K+ levels might be a therapeutic strategy to antagonize the transcriptionally increased KCNJ18 currents. Consistently, treatment of the patient with K+ reducing drugs dramatically improved the health situation and prevented PP attacks.ConclusionsWe show that a promoter defect in the KCNJ18 gene is likely to cause periodic paralysis, as the observed transcriptional upregulation will be linked to increased Kir2.6 function. This concept is further supported by our observation that most of the PP attacks in our patient disappeared on medical treatment with K+ reducing drugs.

Published

2018

29. Effect of the Ito activator NS5806 on cloned Kv4 channels depends on the accessory protein KChIP2

Author

Kirstine Calloe, Søren-Peter Olesen, Morten Grunnet, Thomas Jespersen, Nicole Schmitt, Alicia Lundby, and Jonathan M. Cordeiro

Subjects

Pharmacology, Membrane potential, Cardiac transient outward potassium current, biology, Shal Potassium Channels, Chemistry, Protein subunit, Xenopus, KCNE2, KCNE3, biology.organism_classification, Potassium channel, Biochemistry, Biophysics, biology.protein

Abstract

Background and purpose The compound NS5806 increases the transient outward current (I(to)) in canine ventricular cardiomyocytes and slows current decay. In human and canine ventricle, I(to) is thought to be mediated by K(V)4.3 and various ancillary proteins, yet, the exact subunit composition of I(to) channels is still debated. Here we characterize the effect of NS5806 on heterologously expressed putative I(to) channel subunits and other potassium channels. Experimental approach Cloned K(V)4 channels were co-expressed with KChIP2, DPP6, DPP10, KCNE2, KCNE3 and K(V)1.4 in Xenopus laevis oocytes or CHO-K1 cells. Key results NS5806 increased K(V)4.3/KChIP2 peak current amplitudes with an EC(50) of 5.3 +/- 1.5microM and significantly slowed current decay. KCNE2, KCNE3, DPP6 and DPP10 modulated K(V)4.3 currents and the response to NS5806, but current decay was slowed only in complexes containing KChIP2. The effect of NS5806 on K(V)4.2 was similar to that on K(V)4.3, and current decay was only slowed in presence of KChIP2. However, for K(V)4.1, the slowing of current decay by NS5806 was independent of KChIP2. K(V)1.4 was strongly inhibited by 10 microM NS5806 and K(V)1.5 was inhibited to a smaller extent. Effects of NS5806 on kinetics of currents generated by K(V)4.3/KChIP2/DPP6 with K(V)1.4 in oocytes could reproduce those on cardiac I(to) in canine ventricular myocytes. K(V)7.1, K(V)11.1 and K(ir)2 currents were unaffected by NS5806. Conclusion and implications NS5806 modulated K(V)4 channel gating depending on the presence of KChIP2, suggesting that NS5806 can potentially be used to address the molecular composition as well as the physiological role of cardiac I(to).

Published

2010

30. Disruption of the K+ Channel β-Subunit KCNE3 Reveals an Important Role in Intestinal and Tracheal Cl− Transport

Author

Thomas J. Jentsch, Lena Wartosch, Michael Fromm, Jacques Barhanin, Karl Kunzelmann, Patricia Preston, Patthara Kongsuphol, Richard Warth, Jiraporn Ousingsawat, and Dorothee Günzel

Subjects

medicine.medical_specialty, Patch-Clamp Techniques, Chloride Transport, Gene Knock-out, KvLQT1, CFTR, MiRP2, KCNN4, Ussing Chamber, Intestine, Potassium Channels, Epithelium, Gating, Biology, Biochemistry, Cell Line, Mice, Chlorides, Membrane Biology, Internal medicine, medicine, Animals, Humans, Tissue Distribution, Patch clamp, Intestinal Mucosa, Muscle, Skeletal, Protein Structure, Quaternary, Molecular Biology, Mice, Knockout, Ussing chamber, Stomach, Skeletal muscle, Periodic paralysis, KCNE3, Cell Biology, medicine.disease, Potassium channel, Cell biology, Intestines, Trachea, Protein Subunits, medicine.anatomical_structure, Endocrinology, Gastric Mucosa, Potassium Channels, Voltage-Gated, Rotarod Performance Test, KCNQ1 Potassium Channel

Abstract

The KCNE3 beta-subunit constitutively opens outwardly rectifying KCNQ1 (Kv7.1) K(+) channels by abolishing their voltage-dependent gating. The resulting KCNQ1/KCNE3 heteromers display enhanced sensitivity to K(+) channel inhibitors like chromanol 293B. KCNE3 was also suggested to modify biophysical properties of several other K(+) channels, and a mutation in KCNE3 was proposed to underlie forms of human periodic paralysis. To investigate physiological roles of KCNE3, we now disrupted its gene in mice. kcne3(-/-) mice were viable and fertile and displayed neither periodic paralysis nor other obvious skeletal muscle abnormalities. KCNQ1/KCNE3 heteromers are present in basolateral membranes of intestinal and tracheal epithelial cells where they might facilitate transepithelial Cl(-) secretion through basolateral recycling of K(+) ions and by increasing the electrochemical driving force for apical Cl(-) exit. Indeed, cAMP-stimulated electrogenic Cl(-) secretion across tracheal and intestinal epithelia was drastically reduced in kcne3(-/-) mice. Because the abundance and subcellular localization of KCNQ1 was unchanged in kcne3(-/-) mice, the modification of biophysical properties of KCNQ1 by KCNE3 is essential for its role in intestinal and tracheal transport. Further, these results suggest KCNE3 as a potential modifier gene in cystic fibrosis.

Published

2010

31. KCNQ1 K+ Channels are Involved in Lipopolysaccharide-induced Apoptosis of Distal Kidney Cells

Author

Philippe Poujeol, Marc Cougnon, Jacques Barhanin, Christophe Duranton, Sebastien L'hoste, Isabelle Rubera, and Michel Tauc

Subjects

0303 health sciences, Kidney, Lipopolysaccharide, Charybdotoxin, Physiology, 030232 urology & nephrology, KCNE3, Biology, Molecular biology, Potassium channel, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine.anatomical_structure, chemistry, Apoptosis, Immunology, medicine, Patch clamp, Intracellular, 030304 developmental biology

Abstract

Most bacteria initiate host inflammatory responses through interactions with epithelial cells. Lipopolysaccharide (LPS), a component of the bacterial cell wall is a major cause of septic shock in emergency care units and in the pathogenesis of acute renal failure. Kidney cells exposed to LPS undergo apoptotic changes, including cell volume decrease, phosphatidylserine exposure, caspase-3- and membrane K+ conductance -activation. Whole-cell configuration was used to identify K+ channels in primary and immortalized culture of mice distal convoluted tubules. LPS exposure induced a 3 fold increase in intracellular cAMP concentration and the activation of an outwardly rectifying K+ conductance in both immortalized and primary culture of distal cells. This LPS-induced current exhibited KCNQ1 K+ channel characteristics, i.e. inhibition by quinidine, chromanol293B and low dose of HMR1556 (IC50

Published

2010

32. The genetic basis of Brugada syndrome: A mutation update

Author

Paula L. Hedley, Poul Jørgensen, Michael Christiansen, Valerie A. Corfield, Johanna C. Moolman-Smook, Sarah Schlamowitz, and Jørgen K. Kanters

Subjects

medicine.medical_specialty, Potassium Channels, Calcium Channels, L-Type, Long QT syndrome, Biology, Sudden death, Sodium Channels, SCN1B, Internal medicine, NAV1.3 Voltage-Gated Sodium Channel, Genetics, medicine, Humans, Genetics (clinical), Brugada Syndrome, Brugada syndrome, Voltage-Gated Sodium Channel beta-3 Subunit, Sodium channel, fungi, KCNE3, Short QT syndrome, Voltage-Gated Sodium Channel beta-1 Subunit, medicine.disease, Potassium channel, Endocrinology, Potassium Channels, Voltage-Gated, Mutation

Abstract

Brugada syndrome (BrS) is a condition characterized by a distinct ST-segment elevation in the right precordial leads of the electrocardiogram and, clinically, by an increased risk of cardiac arrhythmia and sudden death. The condition predominantly exhibits an autosomal dominant pattern of inheritance with an average prevalence of 5:10,000 worldwide. Currently, more than 100 mutations in seven genes have been associated with BrS. Loss-of-function mutations in SCN5A, which encodes the α-subunit of the Nav1.5 sodium ion channel conducting the depolarizing INa current, causes 15–20% of BrS cases. A few mutations have been described in GPD1L, which encodes glycerol-3-phosphate dehydrogenase-1 like protein; CACNA1C, which encodes the α-subunit of the Cav1.2 ion channel conducting the depolarizing IL,Ca current; CACNB2, which encodes the stimulating β2-subunit of the Cav1.2 ion channel; SCN1B and SCN3B, which, in the heart, encodes β-subunits of the Nav1.5 sodium ion channel, and KCNE3, which encodes the ancillary inhibitory β-subunit of several potassium channels including the Kv4.3 ion channel conducting the repolarizing potassium Ito current. BrS exhibits variable expressivity, reduced penetrance, and “mixed phenotypes,” where families contain members with BrS as well as long QT syndrome, atrial fibrillation, short QT syndrome, conduction disease, or structural heart disease, have also been described. Hum Mutat 30:1–11, 2009. © 2009 Wiley-Liss, Inc.

Published

2009

33. Distinct subdomains of the KCNQ1 S6 segment determine channel modulation by different KCNE subunits

Author

Lauren J. Manderfield, Carlos G. Vanoye, Melissa A. Daniels, Richard C. Welch, Alfred L. George, Charles R. Sanders, and Andrew R. Tapper

Subjects

endocrine system diseases, Physiology, Protein subunit, Amino Acid Motifs, Molecular Sequence Data, CHO Cells, Article, 03 medical and health sciences, Cricetulus, 0302 clinical medicine, Protein structure, Cricetinae, Animals, Amino Acid Sequence, Peptide sequence, 030304 developmental biology, 0303 health sciences, biology, urogenital system, KCNE3, Dipeptides, KCNE4, biology.organism_classification, Transmembrane protein, Protein Structure, Tertiary, Cell biology, Biochemistry, KCNQ1 Potassium Channel, biology.protein, 030217 neurology & neurosurgery, KCNQ4

Abstract

Modulation of voltage-gated potassium (KV) channels by the KCNE family of single transmembrane proteins has physiological and pathophysiological importance. All five KCNE proteins (KCNE1–KCNE5) have been demonstrated to modulate heterologously expressed KCNQ1 (KV7.1) with diverse effects, making this channel a valuable experimental platform for elucidating structure–function relationships and mechanistic differences among members of this intriguing group of accessory subunits. Here, we specifically investigated the determinants of KCNQ1 inhibition by KCNE4, the least well-studied KCNE protein. In CHO-K1 cells, KCNQ1, but not KCNQ4, is strongly inhibited by coexpression with KCNE4. By studying KCNQ1-KCNQ4 chimeras, we identified two adjacent residues (K326 and T327) within the extracellular end of the KCNQ1 S6 segment that determine inhibition of KCNQ1 by KCNE4. This dipeptide motif is distinct from neighboring S6 sequences that enable modulation by KCNE1 and KCNE3. Conversely, S6 mutations (S338C and F340C) that alter KCNE1 and KCNE3 effects on KCNQ1 do not abrogate KCNE4 inhibition. Further, KCNQ1-KCNQ4 chimeras that exhibited resistance to the inhibitory effects of KCNE4 still interact biochemically with this protein, implying that accessory subunit binding alone is not sufficient for channel modulation. These observations indicate that the diverse functional effects observed for KCNE proteins depend, in part, on structures intrinsic to the pore-forming subunit, and that distinct S6 subdomains determine KCNQ1 responses to KCNE1, KCNE3, and KCNE4.

Published

2009

34. NovelKCNE3mutation reduces repolarizing potassium current and associated with long QT syndrome

Author

Toru Kita, Keiko Tsuji, Takeru Makiyama, Hidetada Yoshida, Kazuhiko Obayashi, Hiroshi Matsuura, Shiro Kamakura, Wataru Shimizu, Futoshi Toyoda, Toshihiro Honda, Minoru Horie, Hisao Ueyama, Yoshihiro Miyamoto, Dimitar P. Zankov, and Seiko Ohno

Subjects

Adult, Male, Proband, congenital, hereditary, and neonatal diseases and abnormalities, Patch-Clamp Techniques, Adolescent, Long QT syndrome, Mutation, Missense, Single-nucleotide polymorphism, Torsades de pointes, CHO Cells, Biology, Transfection, medicine.disease_cause, Membrane Potentials, Cricetulus, Cricetinae, Chlorocebus aethiops, Genetics, medicine, Animals, Humans, Missense mutation, Amino Acid Sequence, Genetics (clinical), Aged, Mutation, Base Sequence, KCNE2, KCNE3, medicine.disease, Long QT Syndrome, Potassium Channels, Voltage-Gated, COS Cells, KCNQ1 Potassium Channel, biology.protein, Female, Protein Binding

Abstract

Long QT syndrome (LQTS) is an inherited disease involving mutations in the genes encoding a number of cardiac ion channels and a membrane adaptor protein. Among the genes that are responsible for LQTS, KCNE1 and KCNE2 are members of the KCNE family of genes, and function as ancillary subunits of Kv channels. The third KCNE gene, KCNE3, is expressed in cardiac myocytes and interacts with KCNQ1 to change the channel properties. However, KCNE3 has never been linked to LQTS. To investigate the association between KCNE3 and LQTS, we conducted a genetic screening of KCNE3 mutations and single nucleotide polymorphisms (SNPs) in 485 Japanese LQTS probands using DHPLC-WAVE system and direct sequencing. Consequently, we identified two KCNE3 missense mutations, located in the N- and C-terminal domains. The functional effects of these mutations were examined by heterologous expression systems using CHO cells stably expressing KCNQ1. One mutation, p.R99lambdaH was identified in a 76-year-old woman who suffered torsades de pointes (TdP) after administration of disopyramide. Another mutation, p.T4A was identified in a 16-year-old boy and 67-year-old woman. Although the boy carried another KCNH2 mutation, he was asymptomatic. On the other hand, the woman suffered from hypokalemia-induced TdP. In a series of electrophysiological analyses, the KCNQ1(Q1)+KCNE3(E3)-R99lambdaH channel significantly reduced outward current compared to Q1+E3-WT, though the current density of the Q1+E3-T4A channel displayed no statistical significance. This is the first report of KCNE3 mutations associated with LQTS. Screening for variants in the KCNE3 gene is of clinical importance for LQTS patients.

Published

2009

35. KCNE4 domains required for inhibition of KCNQ1

Author

Lauren J. Manderfield, Melissa A. Daniels, Alfred L. George, and Carlos G. Vanoye

Subjects

endocrine system diseases, biology, urogenital system, Physiology, Chemistry, KCNE3, KCNE4, Plasma protein binding, Tripeptide, Fusion protein, Transmembrane protein, Cell biology, Transmembrane domain, Biochemistry, biology.protein, Peptide sequence

Abstract

Voltage-gated potassium (Kv) channels are modulated in distinct ways by members of the KCNE family of single transmembrane domain accessory subunits. KCNE4 has a dramatic inhibitory effect on KCNQ1 that differs substantially from the activating effects of KCNE1 and KCNE3. The structural features of KCNE4 that enable this behaviour are unknown. We exploited chimeras of KCNE1, KCNE3 and KCNE4 to identify specific domains responsible for the inhibitory effects on heterologously expressed KCNQ1. Previous structure–function analysis of KCNE1 and KCNE3 identified a critical tripeptide motif within the transmembrane domain that accounts for the differences in KCNQ1 modulation evoked by these two KCNE proteins. Swapping the transmembrane tripeptide motif of KCNE4 with the corresponding amino acid sequence of KCNE1 did not influence the behaviour of either protein. Similarly, exchanging the tripeptide regions of KCNE3 and KCNE4 further demonstrated that this transmembrane motif does not explain the activity of KCNE4. Using a more systematic approach, we demonstrated that the KCNE4 C-terminus was critical for KCNQ1 modulation. Replacement of the KCNE1 or KCNE3 C-termini with that of KCNE4 created chimeric proteins that strongly inhibited KCNQ1. Additional evidence supported a cooperative role of the KCNE4 transmembrane domain. Although the C-terminus was necessary for KCNE4 activity, we demonstrated that a surrogate transmembrane domain derived from the cytokine receptor CD8 did not enable inhibition of KCNQ1, indicating that the KCNE4 C-terminus alone was not sufficient for KCNQ1 modulation. We further demonstrated that the KCNE4 C-terminus interacts with KCNQ1. Our data reveal important structure–function relationships for KCNE4 that help advance our understanding of potassium channel modulation by KCNE proteins.

Published

2009

36. KCNE variants reveal a critical role of the beta subunit carboxyl terminus in PKA-dependent regulation of the IKspotassium channel

Author

Robert S. Kass, Asami Kaihara, Bankston, Chen L, Junko Kurokawa, and Tetsushi Furukawa

Subjects

Time Factors, Molecular Sequence Data, Biophysics, A Kinase Anchor Proteins, CHO Cells, Transfection, Biochemistry, Article, Membrane Potentials, Dephosphorylation, Cricetulus, Cricetinae, Okadaic Acid, Cyclic AMP, Animals, Humans, Amino Acid Sequence, Phosphorylation, Protein kinase A, G alpha subunit, Cyclic AMP-Dependent Protein Kinase Catalytic Subunits, biology, KCNE2, KCNE3, Receptor-mediated endocytosis, Potassium channel, Protein Structure, Tertiary, Cell biology, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, Mutagenesis, Site-Directed, biology.protein, ATP synthase alpha/beta subunits

Abstract

Co-assembly of KCNQ1 with different accessory, or beta, subunits that are members of the KCNE family results in potassium (K+) channels that conduct functionally distinct currents. The alpha subunit KCNQ1 conducts a slowly activated delayed rectifier K+ current (IKs), a major contributor to cardiac repolarization, when co-assembled with KCNE1 and channels that favor the open state when co-assembled with either KCNE2 or KCNE3. In the heart, stimulation of the sympathetic nervous system enhances IKs. A macromolecular signaling complex of the IKs channel including the targeting protein Yotiao coordinates up or downregulation of channel activity by protein kinase A (PKA) phosphorylation and dephosphorylation of molecules in the complex. beta-adrenergic receptor mediated IKs upregulation, a functional consequence of PKA phosphorylation of the KCNQ1 amino terminus (N-T), requires co-expression of KCNQ1/Yotiao with KCNE1. Here, we report that co-expression of KCNE2, like KCNE1, confers a functional channel response to KCNQ1 phosphorylation, but co-expression of KCNE3 does not. Amino acid sequence comparison among the KCNE peptides, and KCNE1 truncation experiments, reveal a segment of the predicted intracellular KCNE1 carboxyl terminus (C-T) that is necessary for functional transduction of PKA phosphorylated KCNQ1. Moreover, chimera analysis reveals a region of KCNE1 sufficient to confer cAMP-dependent functional regulation upon the KCNQ1_KCNE3_Yotiao channel. The property of specific beta subunits to transduce post-translational regulation of alpha subunits of ion channels adds another dimension to our understanding molecular mechanisms underlying the diversity of regulation of native K+ channels.

Published

2009

37. Functional Effects of KCNE3 Mutation and Its Role in the Development of Brugada Syndrome

Author

Yuesheng Wu, Jonathan M. Cordeiro, Charles Antzelevitch, Michael Christiansen, Carsten Toftager Larsen, Lucía Núñez, Alejandra Guerchicoff, Jacob Hofman-Bang, Eva Delpón, Poul Erik Bloch Thomsen, Elena Burashnikov, Jørgen K. Kanters, and Guido D. Pollevick

Subjects

Adult, Male, Proband, medicine.medical_specialty, Patch-Clamp Techniques, Adolescent, DNA Mutational Analysis, Mutant, Mutation, Missense, Action Potentials, Gene mutation, Biology, medicine.disease_cause, Article, Young Adult, Physiology (medical), Internal medicine, medicine, Humans, Immunoprecipitation, Missense mutation, Genetic Predisposition to Disease, Child, Cells, Cultured, Aged, Brugada Syndrome, Brugada syndrome, Cardiac transient outward potassium current, Mutation, Myocardium, KCNE3, DNA, Middle Aged, medicine.disease, Pedigree, Endocrinology, Potassium Channels, Voltage-Gated, Female, Cardiology and Cardiovascular Medicine, Follow-Up Studies

Abstract

Background— The Brugada syndrome, an inherited syndrome associated with a high incidence of sudden cardiac arrest, has been linked to mutations in 4 different genes, leading to a loss of function in sodium and calcium channel activity. Although the transient outward current ( I to ) is thought to play a prominent role in the expression of the syndrome, mutations in I to -related genes have not been identified as yet. Methods and Results— One hundred five probands with the Brugada syndrome were screened for ion channel gene mutations using single-strand conformation polymorphism electrophoresis and direct sequencing. A missense mutation (R99H) in KCNE3 ( MiRP2 ) was detected in 1 proband. The R99H mutation was found 4/4 phenotype-positive and 0/3 phenotype-negative family members. Chinese hamster ovary-K1 cells were cotransfected using wild-type (WT) or mutant KCNE3 and either WT KCND3 or KCNQ1. Whole-cell patch clamp studies were performed after 48 hours. Interactions between Kv4.3 and KCNE3 were analyzed in coimmunoprecipitation experiments in human atrial samples. Cotransfection of R99H- KCNE3 with KCNQ1 produced no alteration in tail current magnitude or kinetics. However, cotransfection of R99H KCNE3 with KCND3 resulted in a significant increase in the I to intensity compared with WT KCNE3 +KCND3. Using tissues isolated from the left atrial appendages of human hearts, we also demonstrate that K v 4.3 and KCNE3 can be coimmunoprecipitated. Conclusions— These results provide definitive evidence for a functional role of KCNE3 in the modulation of I to in the human heart and suggest that mutations in KCNE3 can underlie the development of the Brugada syndrome.

Published

2008

38. Autonomously Functioning Thyroid Nodule Associated with Thyrotoxic Periodic Paralysis

Author

Kouki Mori, Sadayoshi Ito, Hiroshi Ozaki, Yoshinori Nakagawa, Katsumi Yoshida, and Saeko Hoshikawa

Subjects

Adult, Male, Periodicity, endocrine system, medicine.medical_specialty, Calcium Channels, L-Type, Endocrinology, Diabetes and Metabolism, DNA Mutational Analysis, Thyrotropin receptor, Pathogenesis, Endocrinology, Internal medicine, Humans, Paralysis, Medicine, Thyroid Nodule, Ultrasonography, Voltage-dependent calcium channel, business.industry, Calcium channel, Thyroid, Thyrotoxic periodic paralysis, KCNE3, medicine.disease, Potassium channel, Thyrotoxicosis, medicine.anatomical_structure, Calcium Channels, business

Abstract

Thyrotoxic periodic paralysis (TPP) is mainly associated with Graves' disease but rarely with autonomously functioning thyroid nodule (AFTN). We herein report a case of AFTN associated with TPP in which the latter resolved after (131) I therapy for the former. We analyzed the genes encoding thyrotropin receptor (TSHR), the alpha-subunit of the stimulatory G protein (Gsalpha), calcium channel CACNA1S and potassium channel KCNE3, and found that the patient does not carry the known mutations in these genes. Whereas the pathogenesis of TPP and AFTN remains to be understood, the present case suggests that ion channel defects responsible for familial hypokalemic periodic paralysis may not be associated with TPP, and that mutations in TSHR and Gs alpha genes may be less frequent in AFTN patients in the Japanese population.

Published

2008

39. KCNE Peptides Differently Affect Voltage Sensor Equilibrium and Equilibration Rates in KCNQ1 K+ Channels

Author

William R. Kobertz and Jessica M. Rocheleau

Subjects

Patch-Clamp Techniques, Physiology, Xenopus, Genetic Vectors, Kinetics, Analytical chemistry, Gating, Article, Membrane Potentials, Animals, Humans, Cysteine, Patch clamp, Membrane potential, urogenital system, Chemistry, Cell Membrane, Depolarization, KCNE3, Articles, Electrophysiology, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, Oocytes, Biophysics, Female, Ion Channel Gating

Abstract

KCNQ1 voltage-gated K(+) channels assemble with the family of KCNE type I transmembrane peptides to afford membrane-embedded complexes with diverse channel gating properties. KCNQ1/KCNE1 complexes generate the very slowly activating cardiac I(Ks) current, whereas assembly with KCNE3 produces a constitutively conducting complex involved in K(+) recycling in epithelia. To determine whether these two KCNE peptides influence voltage sensing in KCNQ1 channels, we monitored the position of the S4 voltage sensor in KCNQ1/KCNE complexes using cysteine accessibility experiments. A panel of KCNQ1 S4 cysteine mutants was expressed in Xenopus oocytes, treated with the membrane-impermeant cysteine-specific reagent 2-(trimethylammonium) ethyl methanethiosulfonate (MTSET), and the voltage-dependent accessibility of each mutant was determined. Of these S4 cysteine mutants, three (R228C, G229C, I230C) were modified by MTSET only when KCNQ1 was depolarized. We then employed these state-dependent residues to determine how assembly with KCNE1 and KCNE3 affects KCNQ1 voltage sensor equilibrium and equilibration rates. In the presence of KCNE1, MTSET modification rates for the majority of the cysteine mutants were approximately 10-fold slower, as was recently reported to indicate that the kinetics of the KCNQ1 voltage sensor are slowed by KCNE1 (Nakajo, K., and Y. Kubo. 2007 J. Gen. Physiol. 130:269-281). Since MTS modification rates reflect an amalgam of reagent accessibility, chemical reactivity, and protein conformational changes, we varied the depolarization pulse duration to determine whether KCNE1 slows the equilibration rate of the voltage sensors. Using the state-dependent cysteine mutants, we determined that MTSET modification rates were essentially independent of depolarization pulse duration. These results demonstrate that upon depolarization the voltage sensors reach equilibrium quickly in the presence of KCNE1 and the slow gating of the channel complex is not due to slowly moving voltage sensors. In contrast, all cysteine substitutions in the S4 of KCNQ1/KCNE3 complexes were freely accessible to MTSET independent of voltage, which is consistent with KCNE3 shifting the voltage sensor equilibrium to favor the active state at hyperpolarizing potentials. In total, these results suggest that KCNE peptides differently modulate the voltage sensor in KCNQ1 K(+) channels.

Published

2007

40. A Derivatized Scorpion Toxin Reveals the Functional Output of Heteromeric KCNQ1–KCNE K + Channel Complexes

Author

William R. Kobertz and Trevor J. Morin

Subjects

chemistry.chemical_classification, Patch-Clamp Techniques, Scorpion toxin, biology, Xenopus, Scorpion Venoms, Peptide, KCNE3, General Medicine, KCNE4, Biochemistry, Transmembrane protein, chemistry, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, Mutagenesis, Site-Directed, biology.protein, Biophysics, Animals, Molecular Medicine, Homomeric, Amino Acid Sequence, Patch clamp, Peptide sequence

Abstract

KCNE transmembrane peptides are a family of modulatory beta-subunits that assemble with voltage-gated K+ channels, producing the diversity of potassium currents needed for proper function in a variety of tissues. Although all five KCNE transcripts have been found in cardiac and other tissues, it is unclear whether two different KCNE peptides can assemble with the same K+ channel to form a functional complex. Here, we describe the derivatization of a scorpion toxin that irreversibly inhibits KCNQ1 (Q1) K+ channel complexes that contain a specific KCNE peptide. Using this KCNE sensor, we show that heteromeric complexes form, and the functional output from these complexes reveals a hierarchy in KCNE modulation of Q1 channels: KCNE3 > KCNE1 >> KCNE4. Furthermore, our results demonstrate that Q1/KCNE1/KCNE4 complexes also generate a slowly activating current that has been previously attributed to homomeric Q1/KCNE1 complexes, providing a potential functional role for KCNE4 peptides in the heart.

Published

2007

41. KCNE3 acts by promoting voltage sensor activation in KCNQ1

Author

H. Peter Larsson, Rene Barro-Soria, and Marta E. Perez

Subjects

endocrine system diseases, Voltage clamp, Analytical chemistry, Plasma protein binding, Arginine, Models, Biological, Membrane Potentials, Xenopus laevis, Voltage sensor, Animals, Humans, Electrostatic interaction, Membrane potential, Aspartic Acid, Multidisciplinary, Binding Sites, Voltage-gated ion channel, Chemistry, urogenital system, KCNE3, PNAS Plus, Potassium Channels, Voltage-Gated, KCNQ1 Potassium Channel, Mutation, Biophysics, Oocytes, Female, Ion Channel Gating, AND gate, Protein Binding

Abstract

KCNE β-subunits assemble with and modulate the properties of voltage-gated K(+) channels. In the colon, stomach, and kidney, KCNE3 coassembles with the α-subunit KCNQ1 to form K(+) channels important for K(+) and Cl(-) secretion that appear to be voltage-independent. How KCNE3 subunits turn voltage-gated KCNQ1 channels into apparent voltage-independent KCNQ1/KCNE3 channels is not completely understood. Different mechanisms have been proposed to explain the effect of KCNE3 on KCNQ1 channels. Here, we use voltage clamp fluorometry to determine how KCNE3 affects the voltage sensor S4 and the gate of KCNQ1. We find that S4 moves in KCNQ1/KCNE3 channels, and that inward S4 movement closes the channel gate. However, KCNE3 shifts the voltage dependence of S4 movement to extreme hyperpolarized potentials, such that in the physiological voltage range, the channel is constitutively conducting. By separating S4 movement and gate opening, either by a mutation or PIP2 depletion, we show that KCNE3 directly affects the S4 movement in KCNQ1. Two negatively charged residues of KCNE3 (D54 and D55) are found essential for the effect of KCNE3 on KCNQ1 channels, mainly exerting their effects by an electrostatic interaction with R228 in S4. Our results suggest that KCNE3 primarily affects the voltage-sensing domain and only indirectly affects the gate.

Published

2015

42. Ancillary subunits and stimulation frequency determine the potency of chromanol 293B block of the KCNQ1 potassium channel

Author

Randall L. Rasmusson, Michael E. Duffey, Glenna C.L. Bett, Derek L. Beahm, and Michael J. Morales

Subjects

endocrine system diseases, biology, urogenital system, Physiology, Xenopus, KCNE3, Stimulation, Gating, Pharmacology, biology.organism_classification, Potassium channel, Biophysics, biology.protein, Potency, KvLQT1, IC50

Abstract

KCNQ1 (Kv7.1 or KvLQT1) encodes the alpha-subunit of a voltage-gated potassium channel found in tissues including heart, brain, epithelia and smooth muscle. Tissue-specific characteristics of KCNQ1 current are diverse, due to modification by ancillary subunits. In heart, KCNQ1 associates with KCNE1 (MinK), producing a slowly activating voltage-dependent channel. In epithelia, KCNQ1 co-assembles with KCNE3 (Mirp2) producing a constitutively open channel. Chromanol 293B is a selective KCNQ1 blocker. We studied drug binding and frequency dependence of 293B on KCNQ1 and ancillary subunits expressed in Xenopus oocytes. Ancillary subunits altered 293B potency up to 100-fold (IC50 for KCNQ1 = 65.4 ± 1.7 μm; KCNQ1/KCNE1 = 15.1 ± 3.3 μm; KCNQ1/KCNE3 = 0.54 ± 0.18 μm). Block of KCNQ1 and KCNQ1/KCNE3 was time independent, but 293B altered KCNQ1/KCNE1 activation. We therefore studied frequency-dependent block of KCNQ1/KCNE1. Repetitive rapid stimulation increased KCNQ1/KCNE1 current biphasically, and 293B abolished the slow component. KCNQ1/KCNE3[V72T] activates slowly with a KCNQ1/KCNE1-like phenotype, but retains the high affinity binding of KCNQ1/KCNE3, demonstrating that subunit-mediated changes in gating can be dissociated from subunit-mediated changes in affinity. This study demonstrates the KCNQ1 pharmacology is significantly altered by ancillary subunits. The response of KCNQ1 to specific blockers will therefore be critically dependent on the electrical stimulation pattern of the target organ. Furthermore, the dissociation between gating and overall affinity suggests that mutations in ancillary subunits can potentially strongly alter drug sensitivity without obvious functional changes in gating behaviour, giving rise to unexpected side-effects such as a predisposition to acquired long QT syndrome.

Published

2006

43. Functional modulation of the transient outward current Ito by KCNE β-subunits and regional distribution in human non-failing and failing hearts

Author

Gea-Ny Tseng, András Varró, Norbert Jost, Erich Wettwer, Susanne Radicke, Eva M. Graf, Diego Cotella, Ulrich Banse, and Ursula Ravens

Subjects

Male, medicine.medical_specialty, Patch-Clamp Techniques, Physiology, Protein subunit, CHO Cells, Membrane Potentials, Cricetulus, Cricetinae, Physiology (medical), Internal medicine, medicine, Animals, Humans, Myocyte, RNA, Messenger, Patch clamp, Heart Failure, Cardiac transient outward potassium current, biology, Reverse Transcriptase Polymerase Chain Reaction, Myocardium, KCNE2, Kv Channel-Interacting Proteins, KCNE3, KCNE4, Cell biology, Shal Potassium Channels, Endocrinology, Gene Expression Regulation, Potassium Channels, Voltage-Gated, Case-Control Studies, cardiovascular system, biology.protein, Female, Heterologous expression, Cardiology and Cardiovascular Medicine

Abstract

Objectives The function of Kv4.3 (KCND3) channels, which underlie the transient outward current I to in human heart, can be modulated by several accessory subunits such as KChIP2 and KCNE1–KCNE5. Here we aimed to determine the regional expression of Kv4.3, KChIP2, and KCNE mRNAs in non-failing and failing human hearts and to investigate the functional consequences of subunit coexpression in heterologous expression systems. Methods We quantified mRNA levels for two Kv4.3 isoforms, Kv4.3-S and Kv4.3-L, and for KChIP2 as well as KCNE1–KCNE5 with real-time RT-PCR. We also studied the effects of KCNEs on Kv4.3+KChIP2 current characteristics in CHO cells with the whole-cell voltage-clamp method. Results: In non-failing hearts, low expression was found for KCNE1, KCNE3, and KCNE5, three times higher expression for KCNE2, and 60 times higher for KCNE4. Transmural gradients were detected only for KChIP2 in left and right ventricles. Compared to non-failing tissue, failing hearts showed higher expression of Kv4.3-L and KCNE1 and lower of Kv4.3-S, KChIP2, KCNE4, and KCNE5. In CHO cells, Kv4.3+KChIP2 currents were differentially modified by co-expressed KCNEs: time constants of inactivation were shorter with KCNE1 and KCNE3-5 while time-to-peak was decreased, and V 0.5 of steady-state inactivation was shifted to more negative potentials by all KCNE subunits. Importantly, KCNE2 induced a unique and prominent 'overshoot' of peak current during recovery from inactivation similar to that described for human I to while other KCNE subunits induced little (KCNE4,5) or no overshoot. Conclusions: All KCNEs are expressed in the human heart at the transcript level. Compared to I to in native human myocytes, none of the combination of KChIP2 and KCNE produced an ideal congruency in current characteristics, suggesting that additional factors contribute to the regulation of the native I to channel.

Published

2006

44. The Cdc42 inhibitor secramine B prevents cAMP-induced K+ conductance in intestinal epithelial cells

Author

Wayne I. Lencer, William P. Ciesla, Matthew D. Shair, Nori Tanaka, Tomas Kirchhausen, Henry E. Pelish, and Krishna P. Reddy

Subjects

Pharmacology, Membrane potential, Ion Transport, KCNE3, GTPase, Benzazepines, Biology, Biochemistry, Article, Cell Line, Cell biology, Intestinal mucosa, Cdc42 GTP-Binding Protein, Cyclic AMP, Potassium, Humans, Secretion, Intestinal Mucosa, cdc42 GTP-Binding Protein, Ion Channel Gating, Ion transporter, Epithelial polarity

Abstract

Cyclic AMP- (cAMP) and calcium-dependent agonists stimulate chloride secretion through the coordinated activation of distinct apical and basolateral membrane channels and ion transporters in mucosal epithelial cells. Defects in the regulation of Cl- transport across mucosal surfaces occur with cystic fibrosis and V. cholerae infection and can be life threatening. Here we report that secramine B, a small molecule that inhibits activation of the Rho GTPase Cdc42, reduced cAMP-stimulated chloride secretion in the human intestinal cell line T84. Secramine B interfered with a cAMP-gated and Ba2+-sensitive K+ channel, presumably KCNQ1/KCNE3. This channel is required to maintain the membrane potential that sustains chloride secretion. In contrast, secramine B did not affect the Ca2+-mediated chloride secretion pathway, which requires a separate K+ channel activity from that of cAMP. Pirl1, another small molecule structurally unrelated to secramine B that also inhibits Cdc42 activation in vitro, similarly inhibited cAMP-dependent but not Ca2+-dependent chloride secretion. These results suggest that Rho GTPases may be involved in the regulation of the chloride secretory response and identify secramine B an inhibitor of cAMP-dependent K+ conductance in intestinal epithelial cells.

Published

2006

45. Phosphorylation and protonation of neighboring MiRP2 sites: function and pathophysiology of MiRP2‐Kv3.4 potassium channels in periodic paralysis

Author

Geoffrey W. Abbott, Steve A.N. Goldstein, and Margaret H. Butler

Subjects

Intracellular pH, Molecular Sequence Data, PKC Phosphorylation Site, Biochemistry, Cell Line, Paralyses, Familial Periodic, Serine, Cricetinae, Genetics, medicine, Animals, Humans, Genetic Predisposition to Disease, Amino Acid Sequence, Phosphorylation, Molecular Biology, Conserved Sequence, Protein kinase C, Binding Sites, Chemistry, KCNE3, Periodic paralysis, medicine.disease, Potassium channel, Protein Structure, Tertiary, Shaw Potassium Channels, Potassium Channels, Voltage-Gated, Mutation, Biophysics, Protons, Ion Channel Gating, Biotechnology

Abstract

MinK-related peptide 2 (MiRP2) and Kv3.4 subunits assemble in skeletal muscle to create subthreshold, voltage-gated potassium channels. MiRP2 acts on Kv3.4 to shift the voltage dependence of activation, speed recovery from inactivation, suppress cumulative inactivation and increase unitary conductance. We previously found an R83H missense mutation in MiRP2 that segregated with periodic paralysis in two families and diminished the effects of MiRP2 on Kv3.4. Here we show that MiRP2 has a single, functional PKC phosphorylation site at serine 82 and that normal MiRP2-Kv3.4 function requires phosphorylation of the site. The R83H variant does not prevent PKC phosphorylation of neighboring S82; rather, the change shifts the voltage dependence of activation and endows MiRP2-Kv3.4 channels with sensitivity to changes in intracellular pH across the physiological range. Thus, current passed by single R83H channels decreases as internal pH is lowered (pK(a) approximately 7.3, consistent with histidine protonation) whereas wild-type channels are largely insensitive. These findings identify a key regulatory domain in MiRP2 and suggest a mechanistic link between acidosis and episodes of periodic paralysis.

Published

2006

46. Interaction of KCNE subunits with the KCNQ1 K+channel pore

Author

Kwok-Keung Tai, Geoffrey W. Abbott, and Gianina Panaghie

Subjects

Genetics, endocrine system diseases, urogenital system, Physiology, KCNE3, Gating, Biology, Transmembrane protein, Potassium channel, Protein structure, biology.animal, Biophysics, Patch clamp, Mink, G alpha subunit

Abstract

KCNQ1 alpha subunits form functionally distinct potassium channels by coassembling with KCNE ancillary subunits MinK and MiRP2. MinK-KCNQ1 channels generate the slowly activating, voltage-dependent cardiac IKs current. MiRP2-KCNQ1 channels form a constitutively active current in the colon. The structural basis for these contrasting channel properties, and the mechanisms of alpha subunit modulation by KCNE subunits, are not fully understood. Here, scanning mutagenesis located a tryptophan-tolerant region at positions 338-340 within the KCNQ1 pore-lining S6 domain, suggesting an exposed region possibly amenable to interaction with transmembrane ancillary subunits. This hypothesis was tested using concomitant mutagenesis in KCNQ1 and in the membrane-localized 'activation triplet' regions of MinK and MiRP2 to identify pairs of residues that interact to control KCNQ1 activation. Three pairs of mutations exerted dramatic effects, ablating channel function or either removing or restoring control of KCNQ1 activation. The results place KCNE subunits close to the KCNQ1 pore, indicating interaction of MiRP2-72 with KCNQ1-338; and MinK-59,58 with KCNQ1-339, 340. These data are consistent either with perturbation of the S6 domain by MinK or MiRP2, dissimilar positioning of MinK and MiRP2 within the channel complex, or both. Further, the results suggest specifically that two of the interactions, MiRP2-72/KCNQ1-338 and MinK-58/KCNQ1-340, are required for the contrasting gating effects of MinK and MiRP2.

Published

2006

47. Expression and transcriptional control of human KCNE genes

Author

Andrew L. Lundquist, Leomar Y. Ballester, Alfred L. George, and Candice L. Turner

Subjects

Transcription, Genetic, Transcription (biology), Gene expression, Genetics, Transcriptional regulation, Humans, Potassium channel, Promoter Regions, Genetic, Gene, KCNQ1, biology, Promoter, KCNE2, KCNE3, KCNE4, Gene Expression Regulation, KCNE5, Organ Specificity, Potassium Channels, Voltage-Gated, KCNE1, biology.protein, Transcription Factors

Abstract

Potassium channels are essential for a variety of cellular processes ranging from membrane excitability to cellular proliferation. The KCNE genes (KCNE1–5) encode a family of single-transmembrane-domain proteins that modulate the properties of several potassium channels, suggesting a physiologic role for these accessory subunits in many human tissues. To investigate the expression and transcriptional control of KCNE genes we mapped transcription start sites, delineated 5′ genomic structure, and characterized functional promoter elements for each gene. We identified alternatively spliced transcripts for both KCNE1 and KCNE3, including a cardiac-specific KCNE1 transcript. Analysis of relative expression levels of KCNE1–5 in a panel of human tissues revealed distinct, but overlapping, expression patterns. The coexpression of multiple functionally distinct KCNE genes in some tissues infers complex accessory subunit modification of potassium channels. Identification of the core promoter elements necessary for transcriptional control of the KCNE genes facilitates future work investigating factors responsible for tissue-specific expression as well as the discovery of promoter variants associated with disease.

Published

2006

48. In vitro molecular interactions and distribution of KCNE family with KCNQ1 in the human heart

Author

Karinne Haurogne, Marie Madeleine Larroque, Viktoria Szuts, Denis Escande, Renaud Derand, Sophie Demolombe, Jacques Barhanin, Saïd Bendahhou, Céline Marionneau, Institut de pharmacologie moléculaire et cellulaire (IPMC), Université Nice Sophia Antipolis (... - 2019) (UNS), and COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Centre National de la Recherche Scientifique (CNRS)

Subjects

medicine.medical_specialty, endocrine system diseases, Physiology, 030204 cardiovascular system & hematology, Transfection, 03 medical and health sciences, 0302 clinical medicine, Cricetinae, Physiology (medical), Internal medicine, Chlorocebus aethiops, medicine, Animals, Humans, Repolarization, Heart Atria, RNA, Messenger, KvLQT1, 030304 developmental biology, 0303 health sciences, COS cells, biology, Atrium (architecture), Reverse Transcriptase Polymerase Chain Reaction, urogenital system, Myocardium, KCNE2, KCNE3, KCNE4, Endocrinology, medicine.anatomical_structure, Potassium Channels, Voltage-Gated, Ventricle, COS Cells, KCNQ1 Potassium Channel, cardiovascular system, biology.protein, Biophysics, Cardiology and Cardiovascular Medicine, Ion Channel Gating

Abstract

Objective : The voltage-gated K+ channel KCNQ1 associates with the small KCNE1 β subunit to underlie the IKs repolarizing current in the heart. Based on sequence homology, the KCNE family is recognized to comprise five members. Controversial data have indicated their participation in several K+ channel protein complexes, including KCNQ1. The expression level and the putative functions of the different KCNE subunits in the human heart still require further investigation. Methods : We have carried out a comparative study of all KCNE subunits with KCNQ1 using the patch-clamp technique in mammalian cells. Real-time RT-PCR absolute quantification was performed on human atrial and ventricular tissue. Results : While KCNQ1/KCNE1 heteromultimer reached high current density with slow gating kinetics and pronounced voltage dependence, KCNQ1/KCNE2 and KCNQ1/KCNE3 complexes produced instantaneous voltage-independent currents with low and high current density, respectively. Co-expression of KCNE4 or KCNE5 with KCNQ1 induced small currents in the physiological range of voltages, with kinetics similar to those of the KCNQ1/KCNE1 complex. However, co-expression of these inhibitory subunits with a disease-associated mutation (S140G-KCNQ1) led to currents that were almost undistinguishable from the KCNQ1/KCNE1 canonical complex. Absolute cDNA quantification revealed a relatively homogeneous distribution of each transcript, except for KCNE4, inside left atria and endo- and epicardia of left ventricular wall with the following abundance: KCNQ1 ![Graphic][1] KCNE4 ≥ KCNE1>KCNE3>KCNE2>KCNE5. KCNE4 expression was twice as high in atrium compared to ventricle. Conclusions : Our data show that KCNQ1 forms a channel complex with 5 KCNE subunits in a specific manner but only interactions with KCNE1, KCNE2, and KCNE3 may have physiological relevance in the human heart. [1]: /embed/inline-graphic-1.gif

Published

2005

49. Expression of multiple KCNE genes in human heart may enable variable modulation of

Author

Christopher S. Rogers, Carlos G. Vanoye, Alfred L. George, Lauren J. Manderfield, Paul Chang, Katherine T. Murray, Andrew L. Lundquist, Davis C. Drinkwater, and Brian S. Donahue

Subjects

Adult, Male, Patch-Clamp Techniques, Transcription, Genetic, CHO Cells, In situ hybridization, Cricetinae, Animals, Humans, Gene family, RNA, Messenger, Molecular Biology, Gene, In Situ Hybridization, Aged, Regulation of gene expression, Ion Transport, biology, Myocardium, KCNE2, KCNE3, KCNE4, Middle Aged, Molecular biology, Potassium channel, Electrophysiology, Protein Subunits, Gene Expression Regulation, Potassium Channels, Voltage-Gated, Potassium, cardiovascular system, biology.protein, Cardiomyopathies, Cardiology and Cardiovascular Medicine

Abstract

Voltage-gated potassium (K(V)) channels are modulated by at least three distinct classes of proteins including the KCNE family of single transmembrane accessory subunits. In the human genome, KCNE proteins are encoded by five genes designated KCNE1 through KCNE5. KCNE1 associates with KCNQ1 in vitro to generate a potassium current closely resembling the slowly activating delayed rectifier (I(Ks)). Other KCNE proteins also affect the activity of heterologously expressed KCNQ1. To investigate the potential physiological relevance of this gene family in human heart, we examined the relative expression of KCNQ1 and all five KCNE genes in samples derived from normal tissues representing major regions of human heart by real-time, quantitative RT-PCR. KCNE genes are expressed in human heart with a relative abundance ranking of KCNE1 > KCNE4 > KCNE5 approximately KCNE3 >> KCNE2. In situ hybridization revealed prominent expression of KCNE1 and KCNE3-5 in human atrial myocytes. In cardiomyopathic hearts, expression of KCNE1, KCNE3, KCNE4, and KCNQ1 was significantly increased, while KCNE2 and KCNE5 exhibited reduced expression. In a cell line stably expressing KCNQ1 and KCNE1, transient expression of KCNE3, KCNE4, or KCNE5 significantly altered I(Ks) current profiles. Even in the presence of additional KCNE1, KCNE4 and KCNE5 exert dominant effects on I(Ks). Although KCNE1 is the predominant KCNE family member expressed in human heart, the abundance of other KCNE transcripts including potential KCNQ1 suppressors (KCNE4 and KCNE5) and their altered expression patterns in disease lead us to speculate that a balance of KCNE accessory subunits may be important for cardiac K(V) channel function.

Published

2005

50. Ménière’s Disease Is Associated with Single Nucleotide Polymorphisms in the Human Potassium Channel Genes, KCNE1 and KCNE3

Author

Toshihiro Kuramasu, Hiroshi Hibino, Takashi Sato, Takeshi Kubo, Yuka Fuse, Katsumi Doi, Tadashi Kitahara, Arata Horii, and Naoki Matsushiro

Subjects

Genetics, medicine.medical_specialty, Candidate gene, Single-nucleotide polymorphism, KCNE3, Biology, Endocrinology, Otorhinolaryngology, Internal medicine, medicine, Genetic predisposition, SNP, Gene, Genotyping, Genetic association

Abstract

Although the bases for both the sporadic and inherited forms of Ménière’s disease (MD) remain undefined, it is likely to be multifactorial, one of the factors being a genetic predisposition. Recently, genetic association studies on complex diseases have become very popular and most of them are case-control studies using single nucleotide polymorphisms (SNPs) as markers. Mutations/polymorphisms in KCNE potassium channel genes might play a causative role in MD, because KCNE potassium channels have been suggested to be present and active in transmembrane ion and water transports in the inner ear. In the present study, to identify MD susceptibility genes, we have conducted a genetic association study with optimized sampling, optimized phenotyping/genotyping, and a selection of KCNE genes as the candidate genes. The SNPs analyses identified 112G/A SNP in the KCNE1 gene and 198T/C SNP in the KCNE3 gene in 63 definite MD cases as well as 205 and 237 non-MD control subjects. For both KCNE1 and KCNE3 genes, a significant difference in frequency of each SNP was confirmed between MD cases and non-MD control subjects. The result indicates that 112G/A SNP in the KCNE1 gene and 198T/C SNP in the KCNE3 gene could determine an increased susceptibility to develop MD.

Published

2005