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1. Development of new Kir2.1 channel openers from propafenone analogues.

Author

Li, Encan, Boujeddaine, Najla, Houtman, Marien J. C., Maas, Renee G. C., Sluijter, Joost P. G., Ecker, Gerhard F., Stary‐Weinzinger, Anna, van Ham, Willem B., and van der Heyden, Marcel A. G.

Subjects
ACTION potentials, SODIUM channel blockers, DRUG discovery, WESTERN immunoblotting, VENTRICULAR arrhythmia, POTASSIUM channels
Abstract

Background and Purposes: Reduced inward rectifier potassium channel (Kir2.1) functioning is associated with heart failure and may cause Andersen‐Tawil Syndrome, among others characterized by ventricular arrhythmias. Most heart failure or Andersen–Tawil Syndrome patients are treated with β‐adrenoceptor antagonists (β‐blockers) or sodium channel blockers; however, these do not specifically address the inward rectifier current (IK1) nor aim to improve resting membrane potential stability. Consequently, additional pharmacotherapy for heart failure and Andersen–Tawil Syndrome treatment would be highly desirable. Acute propafenone treatment at low concentrations enhances IK1 current, but it also exerts many off‐target effects. Therefore, discovering and exploring new IK1‐channel openers is necessary. Experimental Approach: Effects of propafenone and 10 additional propafenone analogues were analysed. Currents were measured by single‐cell patch‐clamp electrophysiology. Kir2.1 protein expression levels were determined by western blot analysis and action potential characteristics were further validated in human‐induced pluripotent stem cells–derived cardiomyocytes (hiPSC‐CMCs). Molecular docking was performed to obtain detailed information on drug‐channel interactions. Key Results: Analogues GPV0019, GPV0057 and GPV0576 strongly increased the outward component of IK1 while not affecting the Kir2.1 channel expression levels. GPV0057 did not block IKr at concentrations below 0.5 μmol L−1 nor NaV1.5 current below 1 μmol L−1. Moreover, hiPSC‐CMC action potential duration was also not affected by GPV0057 at 0.5 and 1 μmol L−1. Structure analysis indicates a mechanism by which GPV0057 might enhance Kir2.1 channel activation. Conclusion and Implications: GPV0057 has a strong efficiency towards increasing IK1, which makes it a good candidate to address IK1 deficiency‐associated diseases. [ABSTRACT FROM AUTHOR]

Published
2025
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3. Development of IKATP Ion Channel Blockers Targeting Sulfonylurea Resistant Mutant KIR6.2 Based Channels for Treating DEND Syndrome

Author

Medische Fysiologie, Circulatory Health, Houtman, Marien J C, Friesacher, Theres, Chen, Xingyu, Zangerl-Plessl, Eva-Maria, van der Heyden, Marcel A G, Stary-Weinzinger, Anna, Medische Fysiologie, Circulatory Health, Houtman, Marien J C, Friesacher, Theres, Chen, Xingyu, Zangerl-Plessl, Eva-Maria, van der Heyden, Marcel A G, and Stary-Weinzinger, Anna

Published
2022

4. Development of IKATP Ion Channel Blockers Targeting Sulfonylurea Resistant Mutant KIR6.2 Based Channels for Treating DEND Syndrome

Author

Houtman, Marien J. C., Friesacher, Theres, Chen, Xingyu, Zangerl-Plessl, Eva-Maria, van der Heyden, Marcel A. G., and Stary-Weinzinger, Anna

Subjects
Pharmacology, DEND syndrome, SUR2, KIR6.2, Therapeutics. Pharmacology, RM1-950, travoprost, betaxolol, patch clamp, molecular dynamics, Original Research
Abstract

Introduction: DEND syndrome is a rare channelopathy characterized by a combination of developmental delay, epilepsy and severe neonatal diabetes. Gain of function mutations in the KCNJ11 gene, encoding the KIR6.2 subunit of the IKATP potassium channel, stand at the basis of most forms of DEND syndrome. In a previous search for existing drugs with the potential of targeting Cantú Syndrome, also resulting from increased IKATP, we found a set of candidate drugs that may also possess the potential to target DEND syndrome. In the current work, we combined Molecular Modelling including Molecular Dynamics simulations, with single cell patch clamp electrophysiology, in order to test the effect of selected drug candidates on the KIR6.2 WT and DEND mutant channels. Methods: Molecular dynamics simulations were performed to investigate potential drug binding sites. To conduct in vitro studies, KIR6.2 Q52R and L164P mutants were constructed. Inside/out patch clamp electrophysiology on transiently transfected HEK293T cells was performed for establishing drug-channel inhibition relationships. Results: Molecular Dynamics simulations provided insight in potential channel interaction and shed light on possible mechanisms of action of the tested drug candidates. Effective IKIR6.2/SUR2a inhibition was obtained with the pore-blocker betaxolol (IC50 values 27–37 μM). Levobetaxolol effectively inhibited WT and L164P (IC50 values 22 μM) and Q52R (IC50 55 μM) channels. Of the SUR binding prostaglandin series, travoprost was found to be the best blocker of WT and L164P channels (IC50 2–3 μM), while Q52R inhibition was 15–20% at 10 μM. Conclusion: Our combination of MD and inside-out electrophysiology provides the rationale for drug mediated IKATP inhibition, and will be the basis for 1) screening of additional existing drugs for repurposing to address DEND syndrome, and 2) rationalized medicinal chemistry to improve IKATP inhibitor efficacy and specificity.

Published
2022
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9. Selective late sodium current inhibitor GS-458967 suppresses Torsades de Pointes by mostly affecting perpetuation but not initiation of the arrhythmia

Author

Bossu, Alexandre, Houtman, Marien J C, Meijborg, Veronique M F, Varkevisser, Rosanne, Beekman, Henriette D M, Dunnink, Albert, de Bakker, Jacques M T, Mollova, Nevena, Rajamani, Sridharan, Belardinelli, Luiz, van der Heyden, Marcel A G, Vos, Marc A, Cardiology, Amsterdam Cardiovascular Sciences, and ACS - Heart failure & arrhythmias

Subjects
Sulfonamides, Dogs, Dose-Response Relationship, Drug, Pyridines, Torsades de Pointes, Phenethylamines, Animals, Arrhythmias, Cardiac, Myocytes, Cardiac, Triazoles, Research Papers, Anti-Arrhythmia Agents, Research Paper
Abstract

BACKGROUND AND PURPOSE: Enhanced late sodium current (late INa ) in heart failure and long QT syndrome type 3 is proarrhythmic. This study investigated the antiarrhythmic effect and mode of action of the selective and potent late INa inhibitor GS-458967 (GS967) against Torsades de Pointes arrhythmias (TdP) in the chronic atrioventricular block (CAVB) dog. EXPERIMENTAL APPROACH: Electrophysiological and antiarrhythmic effects of GS967 were evaluated in isolated canine ventricular cardiomyocytes and CAVB dogs with dofetilide-induced early afterdepolarizations (EADs) and TdP, respectively. Mapping of intramural cardiac electrical activity in vivo was conducted to study effects of GS967 on spatial dispersion of repolarization. KEY RESULTS: GS967 (IC50 ~200nM) significantly shortened repolarization in canine ventricular cardiomyocytes and sinus rhythm (SR) dogs, in a concentration and dose-dependent manner. In vitro, despite addition of 1μM GS967, dofetilide-induced EADs remained present in 42% and 35% of cardiomyocytes from SR and CAVB dogs, respectively. Nonetheless, GS967 (787±265nM) completely abolished dofetilide-induced TdP in CAVB dogs (10/14 after dofetilide to 0/14 dogs after GS967), while single ectopic beats (sEB) persisted in 9 animals. In vivo mapping experiments showed that GS967 significantly reduced spatial dispersion of repolarization: cubic dispersion was significantly decreased from 237±54ms after dofetilide to 123±34ms after GS967. CONCLUSION AND IMPLICATIONS: GS967 terminated all dofetilide-induced TdP without completely suppressing EADs and sEB in vitro and in vivo, respectively. The antiarrhythmic mode of action of GS967, through the reduction of spatial dispersion of repolarization, seems to predominantly impede the perpetuation of arrhythmic events into TdP rather than their initiating trigger.

Published
2018

10. LUF7244 plus Dofetilide Rescues Aberrant Kv11.1 Trafficking and Produces Functional IKv11.1

Author

Medische Fysiologie, TN groep Adan, Circulatory Health, Qile, Muge, Ji, Yuan, Golden, Tyona D, Houtman, Marien J C, Romunde, Fee, Fransen, Doreth, van Ham, Willem B, IJzerman, Ad P, January, Craig T, Heitman, Laura H, Stary-Weinzinger, Anna, Delisle, Brian P, van der Heyden, Marcel A G, Medische Fysiologie, TN groep Adan, Circulatory Health, Qile, Muge, Ji, Yuan, Golden, Tyona D, Houtman, Marien J C, Romunde, Fee, Fransen, Doreth, van Ham, Willem B, IJzerman, Ad P, January, Craig T, Heitman, Laura H, Stary-Weinzinger, Anna, Delisle, Brian P, and van der Heyden, Marcel A G

Published
2020

11. Development of IKATP Ion Channel Blockers Targeting Sulfonylurea Resistant Mutant KIR6.2 Based Channels for Treating DEND Syndrome.

Author

Houtman, Marien J. C., Friesacher, Theres, Chen, Xingyu, Zangerl-Plessl, Eva-Maria, Heyden, Marcel A. G. van der, and Stary-Weinzinger, Anna

Subjects
ION channels, PATCH-clamp techniques (Electrophysiology), GAIN-of-function mutations, POTASSIUM channels, MOLECULAR dynamics, SULFONYLUREAS, PHARMACEUTICAL chemistry
Abstract

Introduction: DEND syndrome is a rare channelopathy characterized by a combination of developmental delay, epilepsy and severe neonatal diabetes. Gain of function mutations in the KCNJ11 gene, encoding the KIR6.2 subunit of the IKATP potassium channel, stand at the basis of most forms of DEND syndrome. In a previous search for existing drugs with the potential of targeting Cantú Syndrome, also resulting from increased IKATP, we found a set of candidate drugs that may also possess the potential to target DEND syndrome. In the current work, we combined Molecular Modelling including Molecular Dynamics simulations, with single cell patch clamp electrophysiology, in order to test the effect of selected drug candidates on the KIR6.2 WT and DEND mutant channels. Methods: Molecular dynamics simulations were performed to investigate potential drug binding sites. To conduct in vitro studies, KIR6.2 Q52R and L164P mutants were constructed. Inside/out patch clamp electrophysiology on transiently transfected HEK293T cells was performed for establishing drug-channel inhibition relationships. Results: Molecular Dynamics simulations provided insight in potential channel interaction and shed light on possible mechanisms of action of the tested drug candidates. Effective IKIR6.2/SUR2a inhibition was obtained with the pore-blocker betaxolol (IC50 values 27–37 μM). Levobetaxolol effectively inhibited WT and L164P (IC50 values 22 μM) and Q52R (IC50 55 μM) channels. Of the SUR binding prostaglandin series, travoprost was found to be the best blocker of WT and L164P channels (IC50 2–3 μM), while Q52R inhibition was 15–20% at 10 μM. Conclusion: Our combination of MD and inside-out electrophysiology provides the rationale for drug mediated IKATP inhibition, and will be the basis for 1) screening of additional existing drugs for repurposing to address DEND syndrome, and 2) rationalized medicinal chemistry to improve IKATP inhibitor efficacy and specificity. [ABSTRACT FROM AUTHOR]

Published
2022
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17. LUF7244, an allosteric modulator/activator of K v11.1 channels, counteracts dofetilide-induced torsades de pointes arrhythmia in the chronic atrioventricular block dog model

Author

Qile, Muge, Beekman, Henriette D M, Sprenkeler, David J, Houtman, Marien J C, van Ham, W B, Stary-Weinzinger, Anna, Beyl, Stanislav, Hering, Steffen, van den Berg, Dirk-Jan, de Lange, Elizabeth C M, Heitman, Laura H, IJzerman, Ad P, Vos, Marc A, van der Heyden, Marcel A G, Qile, Muge, Beekman, Henriette D M, Sprenkeler, David J, Houtman, Marien J C, van Ham, W B, Stary-Weinzinger, Anna, Beyl, Stanislav, Hering, Steffen, van den Berg, Dirk-Jan, de Lange, Elizabeth C M, Heitman, Laura H, IJzerman, Ad P, Vos, Marc A, and van der Heyden, Marcel A G

Published
2019

18. Computational Identification of Novel Kir6 Channel Inhibitors

Author

Chen, Xingyu, Garon, Arthur, Wieder, Marcus, Houtman, Marien J C, Zangerl-Plessl, Eva-Maria, Langer, Thierry, van der Heyden, Marcel A G, Stary-Weinzinger, Anna, Chen, Xingyu, Garon, Arthur, Wieder, Marcus, Houtman, Marien J C, Zangerl-Plessl, Eva-Maria, Langer, Thierry, van der Heyden, Marcel A G, and Stary-Weinzinger, Anna

Published
2019

19. Identification of a PEST Sequence in Vertebrate KIR2.1 That Modifies Rectification

Author

Medische Fysiologie, Circulatory Health, Qile, Muge, Ji, Yuan, Houtman, Marien J C, Veldhuis, Marlieke, Romunde, Fee, Kok, Bart, van der Heyden, Marcel A G, Medische Fysiologie, Circulatory Health, Qile, Muge, Ji, Yuan, Houtman, Marien J C, Veldhuis, Marlieke, Romunde, Fee, Kok, Bart, and van der Heyden, Marcel A G

Published
2019

20. LUF7244, an allosteric modulator/activator of K v11.1 channels, counteracts dofetilide-induced torsades de pointes arrhythmia in the chronic atrioventricular block dog model

Author

Medische Fysiologie, Circulatory Health, Arts Assistenten Cardiologie, TN groep Adan, Qile, Muge, Beekman, Henriette D M, Sprenkeler, David J, Houtman, Marien J C, van Ham, W B, Stary-Weinzinger, Anna, Beyl, Stanislav, Hering, Steffen, van den Berg, Dirk-Jan, de Lange, Elizabeth C M, Heitman, Laura H, IJzerman, Ad P, Vos, Marc A, van der Heyden, Marcel A G, Medische Fysiologie, Circulatory Health, Arts Assistenten Cardiologie, TN groep Adan, Qile, Muge, Beekman, Henriette D M, Sprenkeler, David J, Houtman, Marien J C, van Ham, W B, Stary-Weinzinger, Anna, Beyl, Stanislav, Hering, Steffen, van den Berg, Dirk-Jan, de Lange, Elizabeth C M, Heitman, Laura H, IJzerman, Ad P, Vos, Marc A, and van der Heyden, Marcel A G

Published
2019

21. Computational Identification of Novel Kir6 Channel Inhibitors

Author

Medische Fysiologie, Circulatory Health, Chen, Xingyu, Garon, Arthur, Wieder, Marcus, Houtman, Marien J C, Zangerl-Plessl, Eva-Maria, Langer, Thierry, van der Heyden, Marcel A G, Stary-Weinzinger, Anna, Medische Fysiologie, Circulatory Health, Chen, Xingyu, Garon, Arthur, Wieder, Marcus, Houtman, Marien J C, Zangerl-Plessl, Eva-Maria, Langer, Thierry, van der Heyden, Marcel A G, and Stary-Weinzinger, Anna

Published
2019

22. Glibenclamide and HMR1098 normalize Cantú syndrome-associated gain-of-function currents

Author

Genetica Groep Van Haaften, Child Health, CMM Sectie Genomics and Bioinformatics, Cancer, Medische Fysiologie, Circulatory Health, Houtman, Marien J C, Chen, Xingyu, Qile, Muge, Duran, Karen, van Haaften, Gijs, Stary-Weinzinger, Anna, van der Heyden, Marcel A G, Genetica Groep Van Haaften, Child Health, CMM Sectie Genomics and Bioinformatics, Cancer, Medische Fysiologie, Circulatory Health, Houtman, Marien J C, Chen, Xingyu, Qile, Muge, Duran, Karen, van Haaften, Gijs, Stary-Weinzinger, Anna, and van der Heyden, Marcel A G

Published
2019

25. Selective late sodium current inhibitor GS-458967 suppresses Torsades de Pointes by mostly affecting perpetuation but not initiation of the arrhythmia

Author

Medische Fysiologie, Circulatory Health, Bossu, Alexandre, Houtman, Marien J C, Meijborg, Veronique M F, Varkevisser, Rosanne, Beekman, Henriette D M, Dunnink, Albert, de Bakker, Jacques M T, Mollova, Nevena, Rajamani, Sridharan, Belardinelli, Luiz, van der Heyden, Marcel A G, Vos, Marc A, Medische Fysiologie, Circulatory Health, Bossu, Alexandre, Houtman, Marien J C, Meijborg, Veronique M F, Varkevisser, Rosanne, Beekman, Henriette D M, Dunnink, Albert, de Bakker, Jacques M T, Mollova, Nevena, Rajamani, Sridharan, Belardinelli, Luiz, van der Heyden, Marcel A G, and Vos, Marc A

Published
2018

26. PA-6 inhibits inward rectifier currents carried by V93I and D172N gain-of-function KIR2.1 channels, but increases channel protein expression

Author

Ji, Yuan, primary, Veldhuis, Marlieke G., additional, Zandvoort, Jantien, additional, Romunde, Fee L., additional, Houtman, Marien J. C., additional, Duran, Karen, additional, van Haaften, Gijs, additional, Zangerl-Plessl, Eva-Maria, additional, Takanari, Hiroki, additional, Stary-Weinzinger, Anna, additional, and van der Heyden, Marcel A. G., additional

Published
2017
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28. Identification of a PEST Sequence in Vertebrate KIR2.1 That Modifies Rectification.

Author

Qile, Muge, Ji, Yuan, Houtman, Marien J. C., Veldhuis, Marlieke, Romunde, Fee, Kok, Bart, and van der Heyden, Marcel A. G.

Subjects
AMINO acid sequence, WESTERN immunoblotting, MEMBRANE potential, LONG QT syndrome, GLUTAMIC acid
Abstract

KIR2.1 potassium channels, producing inward rectifier potassium current (I K1 ), are important for final action potential repolarization and a stable resting membrane potential in excitable cells like cardiomyocytes. Abnormal KIR2.1 function, either decreased or increased, associates with diseases such as Andersen-Tawil syndrome, long and short QT syndromes. KIR2.1 ion channel protein trafficking and subcellular anchoring depends on intrinsic specific short amino acid sequences. We hypothesized that combining an evolutionary based sequence comparison and bioinformatics will identify new functional domains within the C-terminus of the KIR2.1 protein, which function could be determined by mutation analysis. We determined PEST domain signatures, rich in proline (P), glutamic acid (E), serine (S), and threonine (T), within KIR2.1 sequences using the "epestfind" webtool. WT and ΔPEST KIR2.1 channels were expressed in HEK293T and COS-7 cells. Patch-clamp electrophysiology measurements were performed in the inside-out mode on excised membrane patches and the whole cell mode using AxonPatch 200B amplifiers. KIR2.1 protein expression levels were determined by western blot analysis. Immunofluorescence microscopy was used to determine KIR2.1 subcellular localization. An evolutionary conserved PEST domain was identified in the C-terminus of the KIR2.1 channel protein displaying positive PEST scores in vertebrates ranging from fish to human. No similar PEST domain was detected in KIR2.2, KIR2.3, and KIR2.6 proteins. Deletion of the PEST domain in California kingsnake and human KIR2.1 proteins (ΔPEST), did not affect plasma membrane localization. Co-expression of WT and ΔPEST KIR2.1 proteins resulted in heterotetrameric channel formation. Deletion of the PEST domain did not increase protein stability in cycloheximide assays [T½ from 2.64 h (WT) to 1.67 h (ΔPEST), n.s.]. WT and ΔPEST channels, either from human or snake, produced typical I K1 , however, human ΔPEST channels displayed stronger intrinsic rectification. The current observations suggest that the PEST sequence of KIR2.1 is not associated with rapid protein degradation, and has a role in the rectification behavior of I K1 channels. [ABSTRACT FROM AUTHOR]

Published
2019
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29. PA-6 inhibits inward rectifier currents carried by V93I and D172N gain-of-function KIR2.1 channels, but increases channel protein expression

Author

Ji, Yuan, Veldhuis, Marlieke G., Zandvoort, Jantien, Romunde, Fee L, Houtman, Marien J C, Duran, Karen, Van Haaften, Gijs, Zangerl-Plessl, Eva Maria, Takanari, Hiroki, Stary-Weinzinger, Anna, Van Der Heyden, Marcel A.G., Ji, Yuan, Veldhuis, Marlieke G., Zandvoort, Jantien, Romunde, Fee L, Houtman, Marien J C, Duran, Karen, Van Haaften, Gijs, Zangerl-Plessl, Eva Maria, Takanari, Hiroki, Stary-Weinzinger, Anna, and Van Der Heyden, Marcel A.G.

Published
2017

31. Short-term variability of repolarization is superior to other repolarization parameters in the evaluation of diverse antiarrhythmic interventions in the chronic atrioventricular block dog

Author

Medische Fysiologie, Circulatory Health, Bossu, Alexandre, Varkevisser, Rosanne, Beekman, Henriette D.M., Houtman, Marien J C, Van Der Heyden, Marcel A.G., Vos, Marc A., Medische Fysiologie, Circulatory Health, Bossu, Alexandre, Varkevisser, Rosanne, Beekman, Henriette D.M., Houtman, Marien J C, Van Der Heyden, Marcel A.G., and Vos, Marc A.

Published
2017

32. PA-6 inhibits inward rectifier currents carried by V93I and D172N gain-of-function KIR2.1 channels, but increases channel protein expression

Author

Medische Fysiologie, CMM, Genetica Groep Van Haaften, Child Health, CMM Sectie Genomics and Bioinformatics, Circulatory Health, Ji, Yuan, Veldhuis, Marlieke G., Zandvoort, Jantien, Romunde, Fee L, Houtman, Marien J C, Duran, Karen, Van Haaften, Gijs, Zangerl-Plessl, Eva Maria, Takanari, Hiroki, Stary-Weinzinger, Anna, Van Der Heyden, Marcel A.G., Medische Fysiologie, CMM, Genetica Groep Van Haaften, Child Health, CMM Sectie Genomics and Bioinformatics, Circulatory Health, Ji, Yuan, Veldhuis, Marlieke G., Zandvoort, Jantien, Romunde, Fee L, Houtman, Marien J C, Duran, Karen, Van Haaften, Gijs, Zangerl-Plessl, Eva Maria, Takanari, Hiroki, Stary-Weinzinger, Anna, and Van Der Heyden, Marcel A.G.

Published
2017

34. Calcium release near l-type calcium channels promotes beat-to-beat variability in ventricular myocytes from the chronic AV block dog

Author

Medische Fysiologie, Circulatory Health, Antoons, G., Johnson, Daniel M, Dries, Eef, Santiago, Demetrio J, Ozdemir, Semir, Lenaerts, Ilse, Beekman, Jet D M, Houtman, Marien J C, Sipido, Karin R, Vos, Marc A, Medische Fysiologie, Circulatory Health, Antoons, G., Johnson, Daniel M, Dries, Eef, Santiago, Demetrio J, Ozdemir, Semir, Lenaerts, Ilse, Beekman, Jet D M, Houtman, Marien J C, Sipido, Karin R, and Vos, Marc A

Published
2015

35. PA-6 inhibits inward rectifier currents carried by V93I and D172N gain-of-function KIR2.1 channels, but increases channel protein expression.

Author

Yuan Ji, Veldhuis, Marlieke G., Zandvoort, Jantien, Romunde, Fee L., Houtman, Marien J. C., Duran, Karen, van Haaften, Gijs, Zangerl-Plessl, Eva-Maria, Hiroki Takanari, Stary-Weinzinger, Anna, and van der Heyden, Marcel A. G.

Subjects
PROTEIN genetics, ATRIAL fibrillation, PROTEIN expression, MEMBRANE potential, BIOPOTENTIALS (Electrophysiology)
Abstract

Background: The inward rectifier potassium current IK1 contributes to a stable resting membrane potential and phase 3 repolarization of the cardiac action potential. KCNJ2 gain-of-function mutations V93I and D172N associate with increased IK1, short QT syndrome type 3 and congenital atrial fibrillation. Pentamidine-Analogue 6 (PA-6) is an efficient (IC50 = 14 nM with inside-out patch clamp methodology) and specific IK1 inhibitor that interacts with the cytoplasmic pore region of the KIR2.1 ion channel, encoded by KCNJ2. At 10 μM, PA-6 increases wild-type (WT) KIR2. 1 expression in HEK293T cells upon chronic treatment. We hypothesized that PA-6 will interact with and inhibit V93I and D172N KIR2.1 channels, whereas impact on channel expression at the plasma membrane requires higher concentrations. Methods: Molecular modelling was performed with the human KIR2.1 closed state homology model using FlexX. WT and mutant KIR2.1 channels were expressed in HEK293 cells. Patch-clamp single cell electrophysiology measurements were performed in the whole cell and inside-out mode of the patch clamp method. KIR2.1 expression level and localization were determined by western blot analysis and immunofluorescence microscopy, respectively. Results: PA-6 docking in the V93I/D172N double mutant homology model of KIR2.1 demonstrated that mutations and drug-binding site are >30 Å apart. PA-6 inhibited WT and V93I outward currents with similar potency (IC50 = 35.5 and 43.6 nM at +50 mV for WT and V93I), whereas D172N currents were less sensitive (IC50 = 128.9 nM at +50 mV) using inside-out patch-clamp electrophysiology. In whole cell mode, 1 μM of PA-6 inhibited outward IK1 at -50 mV by 28 ± 36%, 18 ± 20% and 10 ± 6%, for WT, V93I and D172N channels respectively. Western blot analysis demonstrated that PA-6 (5 μM, 24 h) increased KIR2.1 expression levels of WT (6.3 ± 1.5 fold), and V93I (3.9 ± 0.9) and D172N (4.8 ± 2. 0) mutants. Immunofluorescent microscopy demonstrated dose-dependent intracellular KIR2.1 accumulation following chronic PA-6 application (24 h, 1 and 5 μM). Conclusions: 1) KCNJ2 gain-of-function mutations V93I and D172N in the KIR2.1 ion channel do not impair PA-6 mediated inhibition of IK1, 2) PA-6 elevates KIR2.1 protein expression and induces intracellular KIR2.1 accumulation, 3) PA-6 is a strong candidate for further preclinical evaluation in treatment of congenital SQT3 and AF. [ABSTRACT FROM AUTHOR]

Published
2017
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36. Experimental mapping of the canine KCNJ2 and KCNJ12 gene structures and functional analysis of the canine KIR2.2 ion channel

Author

Houtman, Marien J. C., Takanari, Hiroki, Kok, Bart G. J. M., van Eck, Margot, Montagne, Denise R., Vos, Marc A., de Boer, Teun P., van der Heyden, Marcel A. G., Houtman, Marien J. C., Takanari, Hiroki, Kok, Bart G. J. M., van Eck, Margot, Montagne, Denise R., Vos, Marc A., de Boer, Teun P., and van der Heyden, Marcel A. G.

Abstract

For many model organisms traditionally in use for cardiac electrophysiological studies, characterization of ion channel genes is lacking. We focused here on two genes encoding the inward rectifier current, KCNJ2 and KCNJ12, in the dog heart. A combination of RT-PCR, 5′-RACE, and 3′-RACE demonstrated the status of KCNJ2 as a two exon gene. The complete open reading frame (ORF) was located on the second exon. One transcription initiation site was mapped. Four differential transcription termination sites were found downstream of two consensus polyadenylation signals. The canine KCNJ12 gene was found to consist of three exons, with its ORF located on the third exon. One transcription initiation and one termination site were found. No alternative splicing was observed in right ventricle or brain cortex. The gene structure of canine KCNJ2 and KCNJ12 was conserved amongst other vertebrates, while current GenBank gene annotation was determined as incomplete. In silico translation of KCN12 revealed a non-conserved glycine rich stretch located near the carboxy-terminus of the KIR2.2 protein. However, no differences were observed when comparing dog with human KIR2.2 protein upon ectopic expression in COS-7 or HEK293 cells with respect to subcellular localization or electrophysiological properties.

Published
2012

40. Reduction of fibrosis-related arrhythmias by chronic renin-angiotensin-aldosterone system inhibitors in an aged mouse model

Author

Stein, Mera, primary, Boulaksil, Mohamed, additional, Jansen, John A., additional, Herold, Eva, additional, Noorman, Maartje, additional, Joles, Jaap A., additional, van Veen, Toon A. B., additional, Houtman, Marien J. C., additional, Engelen, Markus A., additional, Hauer, Richard N. W., additional, de Bakker, Jacques M. T., additional, and van Rijen, Harold V. M., additional

Published
2010
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41. Inhibition of Cardiomyocyte Automaticity by Electrotonic Application of Inward Rectifier Current from Kir2.1 Expressing Cells.

Author

Nagel, Joachim H., Spaan, J. A. E, Coronel, Ruben, de Bakker, Jacques M. T., Zaza, Antonio, de Boer, Teun P., van Veen, Toon A. B., Houtman, Marien J. C., Jansen, John A., van Amersfoorth, Shirley C. M., Doevendans, Pieter A., Vos, Marc A., and van der Heyden, Marcel A. G.

Abstract

A biological pacemaker might be created by generation of a cellular construct consisting of cardiac cells that display spontaneous membrane depolarization, and that are electrotonically coupled to surrounding myocardial cells by means of gap junctions. Depending on the frequency of the spontaneously beating cells, frequency regulation might be required. We hypothesized that application of Kir2.1 expressing non-cardiac cells, which provide IK1 to spontaneously active neonatal cardiomyocytes (NCMs) by electrotonic coupling in such a cellular construct, would generate an opportunity for pacemaker frequency control. Non-cardiac Kir2.1 expressing cells were co-cultured with spontaneously active rat NCMs. Electrotonic coupling between the two cell types resulted in hyperpolarization of the cardiomyocyte membrane potential and silencing of spontaneous activity. Either blocking of gap-junctional communication by halothane or inhibition of IK1 by BaCl2 restored the original membrane potential and spontaneous activity of the NCMs. Our results demonstrate the power of electrotonic coupling for the application of specific ion currents into an engineered cellular construct such as a biological pacemaker. [ABSTRACT FROM AUTHOR]

Published
2007
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42. Increased sarcolemmal Na /H exchange activity in hypertrophied myocytes from dogs with chronic atrioventricular block.

Author

van Borren, Marcel M. G. J., Vos, Marc A., Houtman, Marien J. C., Antoons, Gudrun, and Ravesloot, Jan H.

Subjects
SODIUM-hydrogen antiporter, SODIUM in the body, ACID-base equilibrium, MUSCLE cells, HYDROGEN-ion concentration, CARDIAC hypertrophy
Abstract

Dogs with compensated biventricular hypertrophy due to chronic atrioventricular block (cAVB), are more susceptible to develop drug-induced Torsade-de-Pointes arrhythmias and sudden cardiac death. It has been suggested that the increased Na+ influx in hypertrophied cAVB ventricular myocytes contribute to these lethal arrhythmias. The increased Na+ influx was not mediated by Na+ channels, in fact the Na+ current proved reduced in cAVB myocytes. Here we tested the hypothesis that increased activity of the Na+/H+ exchanger type 1 (NHE-1), commonly observed in hypertrophic hearts, causes the elevated Na+ influx. Cardiac acid-base transport was studied with a pH-sensitive fluorescent dye in ventricular myocytes isolated from control and hypertrophied cAVB hearts; the H+ equivalent flux through NHE-1, Na+-HCO- 3 cotransport (NBC), Cl-/OH- exchange (CHE), and Cl-/HCO- 3 exchange (AE) were determined and normalized per liter cell water and corrected for surface-to-volume ratio. In cAVB, sarcolemmal NHE-1 flux was increased by 65 ± 6.3% in the pHi interval 6.3-7.2 and NBC, AE, and CHE fluxes remained unchanged. Accordingly, at steady-state intracellular pH the total sarcolemmal Na+ influx by NHE-1 + NBC increased from 8.5 ± 1.5 amol/μm2/min in normal myocytes to 15 ± 2.4 amol/μm2/min in hypertrophied cAVB myocytes. We conclude that compensated cardiac hypertrophy in cAVB dogs is accompanied with an increased sarcolemmal NHE-1 activity. This in conjunction with unchanged activity of the other acid-base transporters will raise the intracellular Na+ in hypertrophied cAVB myocytes. [ABSTRACT FROM AUTHOR]

Published
2013
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43. Late na(+) current inhibition by ranolazine reduces torsades de pointes in the chronic atrioventricular block dog model.

Author

Antoons G, Oros A, Beekman JD, Engelen MA, Houtman MJ, Belardinelli L, Stengl M, Vos MA, Antoons, Gudrun, Oros, Avram, Beekman, Jet D M, Engelen, Markus A, Houtman, Marien J C, Belardinelli, Luiz, Stengl, Milan, and Vos, Marc A

Abstract

Objectives: This study investigated whether ranolazine reduces dofetilide-induced torsades de pointes (TdP) in a model of long QT syndrome with down-regulated K(+) currents due to hypertrophic remodeling in the dog with chronic atrioventricular block (cAVB).Background: Ranolazine inhibits the late Na(+) current (I(NaL)) and is effective against arrhythmias in long QT3 syndromes despite its blocking properties of the rapid component of delayed rectifying potassium current.Methods: Ranolazine was administered to cAVB dogs before or after TdP induction with dofetilide and electrophysiological parameters were determined including beat-to-beat variability of repolarization (BVR). In single ventricular myocytes, effects of ranolazine were studied on I(NaL), action potential duration, and dofetilide-induced BVR and early afterdepolarizations.Results: After dofetilide, ranolazine reduced the number of TdP episodes from 10 +/- 3 to 3 +/- 1 (p < 0.05) and partially reversed the increase of BVR with no abbreviation of the dofetilide-induced QT prolongation. Likewise, pre-treatment with ranolazine, or using lidocaine as a specific Na(+) channel blocker, attenuated TdP, but failed to prevent dofetilide-induced increases in QT, BVR, and ectopic activity. In cAVB myocytes, ranolazine suppressed dofetilide-induced early afterdepolarizations in 25% of cells at 5 micromol/l, in 75% at 10 micromol/l, and in 100% at 15 micromol/l. At 5 micromol/l, ranolazine blocked 26 +/- 3% of tetrodotoxin-sensitive I(NaL), and 49 +/- 3% at 15 micromol/l. Despite a 54% reduction of I(NaL) amplitude in cAVB compared with control cells, I(NaL) inhibition by 5 micromol/l tetrodotoxin equally shortened relative action potential duration and completely abolished dofetilide-induced early afterdepolarizations.Conclusions: Despite down-regulation of I(NaL) in remodeled cAVB hearts, ranolazine is antiarrhythmic against drug-induced TdP. The antiarrhythmic effects are reflected in concomitant changes of BVR. [ABSTRACT FROM AUTHOR]

Published
2010
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44. LUF7244 plus Dofetilide Rescues Aberrant K v 11.1 Trafficking and Produces Functional I Kv11.1 .

Author

Qile M, Ji Y, Golden TD, Houtman MJC, Romunde F, Fransen D, van Ham WB, IJzerman AP, January CT, Heitman LH, Stary-Weinzinger A, Delisle BP, and van der Heyden MAG

Subjects
Action Potentials drug effects, Anti-Arrhythmia Agents chemistry, Blotting, Western, Computer Simulation, Drug Synergism, ERG1 Potassium Channel physiology, HEK293 Cells, Humans, Microscopy, Fluorescence, Models, Molecular, Myocytes, Cardiac drug effects, Myocytes, Cardiac physiology, Organic Chemicals chemistry, Phenethylamines chemistry, Potassium Channel Blockers chemistry, Pyridines, Sulfonamides chemistry, Anti-Arrhythmia Agents pharmacology, ERG1 Potassium Channel drug effects, Organic Chemicals pharmacology, Phenethylamines pharmacology, Potassium Channel Blockers pharmacology, Sulfonamides pharmacology
Abstract

Voltage-gated potassium 11.1 (K v 11.1) channels play a critical role in repolarization of cardiomyocytes during the cardiac action potential (AP). Drug-mediated K v 11.1 blockade results in AP prolongation, which poses an increased risk of sudden cardiac death. Many drugs, like pentamidine, interfere with normal K v 11.1 forward trafficking and thus reduce functional K v 11.1 channel densities. Although class III antiarrhythmics, e.g., dofetilide, rescue congenital and acquired forward trafficking defects, this is of little use because of their simultaneous acute channel blocking effect. We aimed to test the ability of a combination of dofetilide plus LUF7244, a K v 11.1 allosteric modulator/activator, to rescue K v 11.1 trafficking and produce functional K v 11.1 current. LUF7244 treatment by itself did not disturb or rescue wild type (WT) or G601S-K v 11.1 trafficking, as shown by Western blot and immunofluorescence microcopy analysis. Pentamidine-decreased maturation of WT K v 11.1 levels was rescued by 10 μM dofetilide or 10 μM dofetilide + 5 μM LUF7244. In trafficking defective G601S-K v 11.1 cells, dofetilide (10 μM) or dofetilide + LUF7244 (10 + 5 μM) also restored K v 11.1 trafficking, as demonstrated by Western blot and immunofluorescence microscopy. LUF7244 (10 μM) increased I Kv 11.1 despite the presence of dofetilide (1 μM) in WT K v 11.1 cells. In G601S-expressing cells, long-term treatment (24-48 hour) with LUF7244 (10 μM) and dofetilide (1 μM) increased I Kv11.1 compared with nontreated or acutely treated cells. We conclude that dofetilide plus LUF7244 rescues K v 11.1 trafficking and produces functional I Kv11.1 Thus, combined administration of LUF7244 and an I Kv11.1 trafficking corrector could serve as a new pharmacological therapy of both congenital and drug-induced K v 11.1 trafficking defects. SIGNIFICANCE STATEMENT: Decreased levels of functional K v 11.1 potassium channel at the plasma membrane of cardiomyocytes prolongs action potential repolarization, which associates with cardiac arrhythmia. Defective forward trafficking of K v 11.1 channel protein is an important factor in acquired and congenital long QT syndrome. LUF7244 as a negative allosteric modulator/activator in combination with dofetilide corrected both congenital and acquired K v 11.1 trafficking defects, resulting in functional K v 11.1 current., (Copyright © 2020 by The American Society for Pharmacology and Experimental Therapeutics.)

Published
2020
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45. LUF7244, an allosteric modulator/activator of K v 11.1 channels, counteracts dofetilide-induced torsades de pointes arrhythmia in the chronic atrioventricular block dog model.

Author

Qile M, Beekman HDM, Sprenkeler DJ, Houtman MJC, van Ham WB, Stary-Weinzinger A, Beyl S, Hering S, van den Berg DJ, de Lange ECM, Heitman LH, IJzerman AP, Vos MA, and van der Heyden MAG

Subjects
Allosteric Regulation drug effects, Animals, Anti-Arrhythmia Agents administration & dosage, Anti-Arrhythmia Agents chemistry, Atrioventricular Block metabolism, Atrioventricular Block pathology, Cells, Cultured, Dogs, HEK293 Cells, Humans, Models, Molecular, Myocytes, Cardiac drug effects, Myocytes, Cardiac metabolism, Myocytes, Cardiac pathology, Phenethylamines, Pyridines administration & dosage, Pyridines chemistry, Sulfonamides, Torsades de Pointes chemically induced, Torsades de Pointes pathology, Anti-Arrhythmia Agents pharmacology, Atrioventricular Block drug therapy, Disease Models, Animal, ERG1 Potassium Channel metabolism, Pyridines pharmacology, Torsades de Pointes drug therapy
Abstract

Background and Purpose: K v 11.1 (hERG) channel blockade is an adverse effect of many drugs and lead compounds, associated with lethal cardiac arrhythmias. LUF7244 is a negative allosteric modulator/activator of K v 11.1 channels that inhibits early afterdepolarizations in vitro. We tested LUF7244 for antiarrhythmic efficacy and potential proarrhythmia in a dog model., Experimental Approach: LUF7244 was tested in vitro for (a) increasing human I Kv11.1 and canine I Kr and (b) decreasing dofetilide-induced action potential lengthening and early afterdepolarizations in cardiomyocytes derived from human induced pluripotent stem cells and canine isolated ventricular cardiomyocytes. In vivo, LUF7244 was given intravenously to anaesthetized dogs in sinus rhythm or with chronic atrioventricular block., Key Results: LUF7244 (0.5-10 μM) concentration dependently increased I Kv11.1 by inhibiting inactivation. In vitro, LUF7244 (10 μM) had no effects on I KIR2.1 , I Nav1.5 , I Ca-L , and I Ks , doubled I Kr , shortened human and canine action potential duration by approximately 50%, and inhibited dofetilide-induced early afterdepolarizations. LUF7244 (2.5 mg·kg -1 ·15 min -1 ) in dogs with sinus rhythm was not proarrhythmic and shortened, non-significantly, repolarization parameters (QTc: -6.8%). In dogs with chronic atrioventricular block, LUF7244 prevented dofetilide-induced torsades de pointes arrhythmias in 5/7 animals without normalization of the QTc. Peak LUF7244 plasma levels were 1.75 ± 0.80 during sinus rhythm and 2.34 ± 1.57 μM after chronic atrioventricular block., Conclusions and Implications: LUF7244 counteracted dofetilide-induced early afterdepolarizations in vitro and torsades de pointes in vivo. Allosteric modulators/activators of K v 11.1 channels might neutralize adverse cardiac effects of existing drugs and newly developed compounds that display QTc lengthening., (© 2019 The Authors. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published
2019
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46. Identification of a PEST Sequence in Vertebrate K IR 2.1 That Modifies Rectification.

Author

Qile M, Ji Y, Houtman MJC, Veldhuis M, Romunde F, Kok B, and van der Heyden MAG

Abstract

K IR 2.1 potassium channels, producing inward rectifier potassium current ( I K1 ), are important for final action potential repolarization and a stable resting membrane potential in excitable cells like cardiomyocytes. Abnormal K IR 2.1 ion channel protein trafficking and subcellular anchoring depends on intrinsic specific short amino acid sequences. We hypothesized that combining an evolutionary based sequence comparison and bioinformatics will identify new functional domains within the C-terminus of the K IR 2.1 ion channel protein trafficking and subcellular anchoring depends on intrinsic specific short amino acid sequences. We hypothesized that combining an evolutionary based sequence comparison and bioinformatics will identify new functional domains within the C-terminus of the K IR 2.1 protein, which function could be determined by mutation analysis. We determined PEST domain signatures, rich in proline (P), glutamic acid (E), serine (S), and threonine (T), within K IR 2.1 sequences using the "epestfind" webtool. WT and ΔPEST K IR 2.1 channels were expressed in HEK293T and COS-7 cells. Patch-clamp electrophysiology measurements were performed in the inside-out mode on excised membrane patches and the whole cell mode using AxonPatch 200B amplifiers. K IR 2.1 subcellular localization. An evolutionary conserved PEST domain was identified in the C-terminus of the K IR 2.1 subcellular localization. An evolutionary conserved PEST domain was identified in the C-terminus of the K IR 2.1 channel protein displaying positive PEST scores in vertebrates ranging from fish to human. No similar PEST domain was detected in K IR 2.2, K IR 2.3, and K IR 2.6 proteins. Deletion of the PEST domain in California kingsnake and human K IR 2.1 proteins (ΔPEST), did not affect plasma membrane localization. Co-expression of WT and ΔPEST K IR 2.1 proteins resulted in heterotetrameric channel formation. Deletion of the PEST domain did not increase protein stability in cycloheximide assays [T½ from 2.64 h (WT) to 1.67 h (ΔPEST), n.s.]. WT and ΔPEST channels, either from human or snake, produced typical I K1 , however, human ΔPEST channels displayed stronger intrinsic rectification. The current observations suggest that the PEST sequence of K IR 2.1 is not associated with rapid protein degradation, and has a role in the rectification behavior of I K1 channels.

Published
2019
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47. Istaroxime, a positive inotropic agent devoid of proarrhythmic properties in sensitive chronic atrioventricular block dogs.

Author

Bossu A, Kostense A, Beekman HDM, Houtman MJC, van der Heyden MAG, and Vos MA

Subjects
Animals, Atrioventricular Block, Dogs, Etiocholanolone therapeutic use, Female, Myocytes, Cardiac drug effects, Myocytes, Cardiac physiology, Phenethylamines, Sulfonamides, Torsades de Pointes chemically induced, Anti-Arrhythmia Agents therapeutic use, Cardiotonic Agents therapeutic use, Etiocholanolone analogs & derivatives, Sodium-Potassium-Exchanging ATPase antagonists & inhibitors, Torsades de Pointes drug therapy
Abstract

Current inotropic agents in heart failure therapy associate with low benefit and significant adverse effects, including ventricular arrhythmias. Istaroxime, a novel Na + /K + -transporting ATPase inhibitor, also stimulates SERCA2a activity, which would confer improved inotropic and lusitropic properties with less proarrhythmic effects. We investigated hemodynamic, electrophysiological and potential proarrhythmic and antiarrhythmic effects of istaroxime in control and chronic atrioventricular block (CAVB) dogs sensitive to drug-induced Torsades de Pointes arrhythmias (TdP). In isolated normal canine ventricular cardiomyocytes, istaroxime (0.3-10 μM) evoked no afterdepolarizations and significantly shortened action potential duration (APD) at 3 and 10 μM. Istaroxime at 3 μg/kg/min significantly increased left ventricular (LV) contractility (dP/dt+) and relaxation (dP/dt-) respectively by 81 and 94% in anesthetized control dogs (n = 6) and by 61 and 49% in anesthetized CAVB dogs (n = 7) sensitive to dofetilide-induced TdP. While istaroxime induced no ventricular arrhythmias in control conditions, only single ectopic beats occurred in 2/7 CAVB dogs, which were preceded by increase of short-term variability of repolarization (STV) and T wave alternans in LV unipolar electrograms. Istaroxime pre-treatment (3 μg/kg/min for 60 min) did not alleviate dofetilide-induced increase in repolarization and STV, and mildly reduced incidence of TdP from 6/6 to 4/6 CAVB dogs. In six CAVB dogs with dofetilide-induced TdP, administration of istaroxime (90 μg/kg/5 min) suppressed arrhythmic episodes in two animals. Taken together, inotropic and lusitropic properties of istaroxime in CAVB dogs were devoid of significant proarrhythmic effects in sensitive CAVB dogs, and istaroxime provides a moderate antiarrhythmic efficacy in prevention and suppression of dofetilide-induced TdP., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published
2018
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48. Class III antiarrhythmic drugs amiodarone and dronedarone impair K IR 2.1 backward trafficking.

Author

Ji Y, Takanari H, Qile M, Nalos L, Houtman MJC, Romunde FL, Heukers R, van Bergen En Henegouwen PMP, Vos MA, and van der Heyden MAG

Subjects
Animals, Anti-Arrhythmia Agents pharmacology, COS Cells, Cell Line, Tumor, Cells, Cultured, Chlorocebus aethiops, Dronedarone, HEK293 Cells, Humans, Ion Channel Gating genetics, Ion Channel Gating physiology, Mice, Myocytes, Cardiac cytology, Myocytes, Cardiac drug effects, Myocytes, Cardiac physiology, Potassium Channels, Inwardly Rectifying genetics, Rabbits, Amiodarone analogs & derivatives, Amiodarone pharmacology, Ion Channel Gating drug effects, Potassium Channels, Inwardly Rectifying physiology
Abstract

Drug-induced ion channel trafficking disturbance can cause cardiac arrhythmias. The subcellular level at which drugs interfere in trafficking pathways is largely unknown. K IR 2.1 inward rectifier channels, largely responsible for the cardiac inward rectifier current (I K 1 ), are degraded in lysosomes. Amiodarone and dronedarone are class III antiarrhythmics. Chronic use of amiodarone, and to a lesser extent dronedarone, causes serious adverse effects to several organs and tissue types, including the heart. Both drugs have been described to interfere in the late-endosome/lysosome system. Here we defined the potential interference in K IR 2.1 backward trafficking by amiodarone and dronedarone. Both drugs inhibited I K 1 in isolated rabbit ventricular cardiomyocytes at supraclinical doses only. In HK-KWGF cells, both drugs dose- and time-dependently increased K IR 2.1 expression (2.0 ± 0.2-fold with amiodarone: 10 μM, 24 hrs; 2.3 ± 0.3-fold with dronedarone: 5 μM, 24 hrs) and late-endosomal/lysosomal K IR 2.1 accumulation. Increased K IR 2.1 expression level was also observed in the presence of Na v 1.5 co-expression. Augmented K IR 2.1 protein levels and intracellular accumulation were also observed in COS-7, END-2, MES-1 and EPI-7 cells. Both drugs had no effect on K v 11.1 ion channel protein expression levels. Finally, amiodarone (73.3 ± 10.3% P < 0.05 at -120 mV, 5 μM) enhanced I KIR 2.1 upon 24-hrs treatment, whereas dronedarone tended to increase I KIR 2.1 and it did not reach significance (43.8 ± 5.5%, P = 0.26 at -120 mV; 2 μM). We conclude that chronic amiodarone, and potentially also dronedarone, treatment can result in enhanced I K 1 by inhibiting K IR 2.1 degradation., (© 2017 The Authors. Journal of Cellular and Molecular Medicine published by John Wiley & Sons Ltd and Foundation for Cellular and Molecular Medicine.)

Published
2017
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49. Calcium release near L-type calcium channels promotes beat-to-beat variability in ventricular myocytes from the chronic AV block dog.

Author

Antoons G, Johnson DM, Dries E, Santiago DJ, Ozdemir S, Lenaerts I, Beekman JD, Houtman MJ, Sipido KR, and Vos MA

Subjects
Action Potentials drug effects, Animals, Caffeine pharmacology, Calcium Signaling drug effects, Chronic Disease, Dogs, Myocytes, Cardiac drug effects, Patch-Clamp Techniques, Sarcoplasmic Reticulum drug effects, Sodium-Calcium Exchanger antagonists & inhibitors, Sodium-Calcium Exchanger metabolism, Atrioventricular Block metabolism, Atrioventricular Block physiopathology, Calcium metabolism, Calcium Channels, L-Type metabolism, Heart Rate drug effects, Myocytes, Cardiac metabolism
Abstract

Beat-to-beat variability of ventricular repolarization (BVR) has been proposed as a strong predictor of Torsades de Pointes (TdP). BVR is also observed at the myocyte level, and a number of studies have shown the importance of calcium handling in influencing this parameter. The chronic AV block (CAVB) dog is a model of TdP arrhythmia in cardiac hypertrophy, and myocytes from these animals show extensive remodeling, including of Ca(2+) handling. This remodeling process also leads to increased BVR. We aimed to determine the role that (local) Ca(2+) handling plays in BVR. In isolated LV myocytes an exponential relationship was observed between BVR magnitude and action potential duration (APD) at baseline. Inhibition of Ca(2+) release from sarcoplasmic reticulum (SR) with thapsigargin resulted in a reduction of [Ca(2+)]i, and of both BVR and APD. Increasing ICaL in the presence of thapsigargin restored APD but BVR remained low. In contrast, increasing ICaL with preserved Ca(2+) release increased both APD and BVR. Inhibition of Ca(2+) release with caffeine, as with thapsigargin, reduced BVR despite maintained APD. Simultaneous inhibition of Na(+)/Ca(2+) exchange and ICaL decreased APD and BVR to similar degrees, whilst increasing diastolic Ca(2+). Buffering of Ca(2+) transients with BAPTA reduced BVR for a given APD to a greater extent than buffering with EGTA, suggesting subsarcolemmal Ca(2+) transients modulated BVR to a larger extent than the cytosolic Ca(2+) transient. In conclusion, BVR in hypertrophied dog myocytes, at any APD, is strongly dependent on SR Ca(2+) release, which may act through modulation of the l-type Ca(2+) current in a subsarcolemmal microdomain., (Copyright © 2015 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published
2015
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50. Insights in KIR2.1 channel structure and function by an evolutionary approach; cloning and functional characterization of the first reptilian inward rectifier channel KIR2.1, derived from the California kingsnake (Lampropeltis getula californiae).

Author

Houtman MJ, Korte SM, Ji Y, Kok B, Vos MA, Stary-Weinzinger A, and van der Heyden MA

Subjects
Amino Acid Sequence, Animals, Base Sequence, Cloning, Molecular, Humans, Molecular Sequence Data, Potassium Channels, Inwardly Rectifying chemistry, Species Specificity, Structure-Activity Relationship, Birds genetics, Colubridae genetics, Evolution, Molecular, Fishes genetics, Ion Channel Gating genetics, Potassium Channels, Inwardly Rectifying physiology
Abstract

Potassium inward rectifier KIR2.1 channels contribute to the stable resting membrane potential in a variety of muscle and neuronal cell-types. Mutations in the KIR2.1 gene KCNJ2 have been associated with human disease, such as cardiac arrhythmias and periodic paralysis. Crystal structure and homology modelling of KIR2.1 channels combined with functional current measurements provided valuable insights in mechanisms underlying channel function. KIR2.1 channels have been cloned and analyzed from all main vertebrate phyla, except reptilians. To address this lacuna, we set out to clone reptilian KIR2.1 channels. Using a degenerated primer set we cloned the KCNJ2 coding regions from muscle tissue of turtle, snake, bear, quail and bream, and compared their deduced amino acid sequences with those of KIR2.1 sequences from 26 different animal species obtained from Genbank. Furthermore, expression constructs were prepared for functional electrophysiological studies of ectopically expressed KIR2.1 ion channels. In general, KCNJ2 gene evolution followed normal phylogenetic patterns, however turtle KIR2.1 ion channel sequence is more homologues to avians than to snake. Alignment of all 31 KIR2.1 sequences showed that all disease causing KIR2.1 mutations, except V93I, V123G and N318S, are fully conserved. Homology models were built to provide structural insights into species specific amino acid substitutions. Snake KIR2.1 channels became expressed at the plasmamembrane and produced typical barium sensitive (IC50 ∼6μM) inward rectifier currents., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published
2014
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