SK channel enhancers attenuate Ca2+-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR

Tae Yun Kim; Radmila Terentyeva; Karim H.F. Roder; Weiyan Li; Man Liu; Ian Greener; Shanna Hamilton; Iuliia Polina; Kevin R. Murphy; Richard T. Clements; Samuel C. Dudley; Gideon Koren; Bum Rak Choi; Dmitry Terentyev

doi:10.1093/cvr/cvx005

SK channel enhancers attenuate Ca²⁺-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR

Tae Yun Kim
, Radmila Terentyeva
, Karim H.F. Roder
, Weiyan Li
, Man Liu
, Ian Greener
, Shanna Hamilton
, Iuliia Polina
, Kevin R. Murphy
, Richard T. Clements
, Samuel C. Dudley
, Gideon Koren
, Bum Rak Choi
, Dmitry Terentyev

نتاج البحث: نشر في مجلة › مقالة › مراجعة النظراء

62 اقتباسات (Scopus)

ملخص

Aims: Plasmamembrane small conductance Ca2+-activated K+ (SK) channels were implicated in ventricular arrhythmias in infarcted and failing hearts. Recently, SK channels were detected in the inner mitochondria membrane (IMM) (mSK), and their activation protected from acute ischaemia-reperfusion injury by reducing intracellular levels of reactive oxygen species (ROS). We hypothesized that mSK play an important role in regulating mitochondrial function in chronic cardiac diseases. We investigated the role of mSK channels in Ca2+-dependent ventricular arrhythmia using rat model of cardiac hypertrophy induced by banding of the ascending aorta thoracic aortic banding (TAB). Methods and results: Dual Ca2+ and membrane potential optical mapping of whole hearts derived from TAB rats revealed that membrane-permeable SK enhancer NS309 (2 μM) improved aberrant Ca2+ homeostasis and abolished VT/VF induced by β-adrenergic stimulation. Using whole cell patch-clamp and confocal Ca2+ imaging of cardiomyocytes derived from TAB hearts (TCMs) we found that membrane-permeable SK enhancers NS309 and CyPPA (10 μM) attenuated frequency of spontaneous Ca2+ waves and delayed afterdepolarizations. Furthermore, mSK inhibition enhanced (UCL-1684, 1 μM); while activation reduced mitochondrial ROS production in TCMs measured with MitoSOX. Protein oxidation assays demonstrated that increased oxidation of ryanodine receptors (RyRs) in TCMs was reversed by SK enhancers. Experiments in permeabilized TCMs showed that SK enhancers restored SR Ca2+ content, suggestive of substantial improvement in RyR function. Conclusion: These data suggest that enhancement of mSK channels in hypertrophic rat hearts protects from Ca2+-dependent arrhythmia and suggest that the protection is mediated via decreased mitochondrial ROS and subsequent decreased oxidation of reactive cysteines in RyR, which ultimately leads to stabilization of RyR-mediated Ca2+ release.

اللغة الأصلية	الإنجليزيّة
الصفحات (من إلى)	343-353
عدد الصفحات	11
دورية	Cardiovascular Research
مستوى الصوت	113
رقم الإصدار	3
المعرِّفات الرقمية للأشياء	https://doi.org/10.1093/cvr/cvx005
حالة النشر	نُشِر - 1 مارس 2017
منشور خارجيًا	نعم

الوصول إلى المستند

10.1093/cvr/cvx005

الملفات والروابط الأخرى

Link to publication in Scopus

قم بذكر هذا

Kim, T. Y., Terentyeva, R., Roder, K. H. F., Li, W., Liu, M., Greener, I., Hamilton, S., Polina, I., Murphy, K. R., Clements, R. T., Dudley, S. C., Koren, G., Choi, B. R., & Terentyev, D. (2017). SK channel enhancers attenuate Ca²⁺-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR. Cardiovascular Research, 113(3), 343-353. https://doi.org/10.1093/cvr/cvx005

@article{1d3f1aaf2dab4a00a23a53dd5a0b81fc,

title = "SK channel enhancers attenuate Ca2+-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR",

abstract = "Aims: Plasmamembrane small conductance Ca2+-activated K+ (SK) channels were implicated in ventricular arrhythmias in infarcted and failing hearts. Recently, SK channels were detected in the inner mitochondria membrane (IMM) (mSK), and their activation protected from acute ischaemia-reperfusion injury by reducing intracellular levels of reactive oxygen species (ROS). We hypothesized that mSK play an important role in regulating mitochondrial function in chronic cardiac diseases. We investigated the role of mSK channels in Ca2+-dependent ventricular arrhythmia using rat model of cardiac hypertrophy induced by banding of the ascending aorta thoracic aortic banding (TAB). Methods and results: Dual Ca2+ and membrane potential optical mapping of whole hearts derived from TAB rats revealed that membrane-permeable SK enhancer NS309 (2 μM) improved aberrant Ca2+ homeostasis and abolished VT/VF induced by β-adrenergic stimulation. Using whole cell patch-clamp and confocal Ca2+ imaging of cardiomyocytes derived from TAB hearts (TCMs) we found that membrane-permeable SK enhancers NS309 and CyPPA (10 μM) attenuated frequency of spontaneous Ca2+ waves and delayed afterdepolarizations. Furthermore, mSK inhibition enhanced (UCL-1684, 1 μM); while activation reduced mitochondrial ROS production in TCMs measured with MitoSOX. Protein oxidation assays demonstrated that increased oxidation of ryanodine receptors (RyRs) in TCMs was reversed by SK enhancers. Experiments in permeabilized TCMs showed that SK enhancers restored SR Ca2+ content, suggestive of substantial improvement in RyR function. Conclusion: These data suggest that enhancement of mSK channels in hypertrophic rat hearts protects from Ca2+-dependent arrhythmia and suggest that the protection is mediated via decreased mitochondrial ROS and subsequent decreased oxidation of reactive cysteines in RyR, which ultimately leads to stabilization of RyR-mediated Ca2+ release.",

keywords = "Cardiac hypertrophy, Reactive oxygen species, Ryanodine receptor, Small conductance Ca-activated Kchannels, Ventricular arrhythmia",

author = "Kim, \{Tae Yun\} and Radmila Terentyeva and Roder, \{Karim H.F.\} and Weiyan Li and Man Liu and Ian Greener and Shanna Hamilton and Iuliia Polina and Murphy, \{Kevin R.\} and Clements, \{Richard T.\} and Dudley, \{Samuel C.\} and Gideon Koren and Choi, \{Bum Rak\} and Dmitry Terentyev",

year = "2017",

month = mar,

day = "1",

doi = "10.1093/cvr/cvx005",

language = "אנגלית",

volume = "113",

pages = "343--353",

journal = "Cardiovascular Research",

issn = "0008-6363",

publisher = "Oxford University Press",

number = "3",

}

Kim, TY, Terentyeva, R, Roder, KHF, Li, W, Liu, M, Greener, I, Hamilton, S, Polina, I, Murphy, KR, Clements, RT, Dudley, SC, Koren, G, Choi, BR & Terentyev, D 2017, 'SK channel enhancers attenuate Ca²⁺-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR', Cardiovascular Research, المجلد 113, رقم 3, الصفحات 343-353. https://doi.org/10.1093/cvr/cvx005

SK channel enhancers attenuate Ca²⁺-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR. / Kim, Tae Yun; Terentyeva, Radmila; Roder, Karim H.F. وآخرون.
في: Cardiovascular Research, المجلد 113, رقم 3, 01.03.2017, صفحة 343-353.

نتاج البحث: نشر في مجلة › مقالة › مراجعة النظراء

TY - JOUR

T1 - SK channel enhancers attenuate Ca2+-dependent arrhythmia in hypertrophic hearts by regulating mito-ROS-dependent oxidation and activity of RyR

AU - Kim, Tae Yun

AU - Terentyeva, Radmila

AU - Roder, Karim H.F.

AU - Li, Weiyan

AU - Liu, Man

AU - Greener, Ian

AU - Hamilton, Shanna

AU - Polina, Iuliia

AU - Murphy, Kevin R.

AU - Clements, Richard T.

AU - Dudley, Samuel C.

AU - Koren, Gideon

AU - Choi, Bum Rak

AU - Terentyev, Dmitry

PY - 2017/3/1

Y1 - 2017/3/1

N2 - Aims: Plasmamembrane small conductance Ca2+-activated K+ (SK) channels were implicated in ventricular arrhythmias in infarcted and failing hearts. Recently, SK channels were detected in the inner mitochondria membrane (IMM) (mSK), and their activation protected from acute ischaemia-reperfusion injury by reducing intracellular levels of reactive oxygen species (ROS). We hypothesized that mSK play an important role in regulating mitochondrial function in chronic cardiac diseases. We investigated the role of mSK channels in Ca2+-dependent ventricular arrhythmia using rat model of cardiac hypertrophy induced by banding of the ascending aorta thoracic aortic banding (TAB). Methods and results: Dual Ca2+ and membrane potential optical mapping of whole hearts derived from TAB rats revealed that membrane-permeable SK enhancer NS309 (2 μM) improved aberrant Ca2+ homeostasis and abolished VT/VF induced by β-adrenergic stimulation. Using whole cell patch-clamp and confocal Ca2+ imaging of cardiomyocytes derived from TAB hearts (TCMs) we found that membrane-permeable SK enhancers NS309 and CyPPA (10 μM) attenuated frequency of spontaneous Ca2+ waves and delayed afterdepolarizations. Furthermore, mSK inhibition enhanced (UCL-1684, 1 μM); while activation reduced mitochondrial ROS production in TCMs measured with MitoSOX. Protein oxidation assays demonstrated that increased oxidation of ryanodine receptors (RyRs) in TCMs was reversed by SK enhancers. Experiments in permeabilized TCMs showed that SK enhancers restored SR Ca2+ content, suggestive of substantial improvement in RyR function. Conclusion: These data suggest that enhancement of mSK channels in hypertrophic rat hearts protects from Ca2+-dependent arrhythmia and suggest that the protection is mediated via decreased mitochondrial ROS and subsequent decreased oxidation of reactive cysteines in RyR, which ultimately leads to stabilization of RyR-mediated Ca2+ release.

AB - Aims: Plasmamembrane small conductance Ca2+-activated K+ (SK) channels were implicated in ventricular arrhythmias in infarcted and failing hearts. Recently, SK channels were detected in the inner mitochondria membrane (IMM) (mSK), and their activation protected from acute ischaemia-reperfusion injury by reducing intracellular levels of reactive oxygen species (ROS). We hypothesized that mSK play an important role in regulating mitochondrial function in chronic cardiac diseases. We investigated the role of mSK channels in Ca2+-dependent ventricular arrhythmia using rat model of cardiac hypertrophy induced by banding of the ascending aorta thoracic aortic banding (TAB). Methods and results: Dual Ca2+ and membrane potential optical mapping of whole hearts derived from TAB rats revealed that membrane-permeable SK enhancer NS309 (2 μM) improved aberrant Ca2+ homeostasis and abolished VT/VF induced by β-adrenergic stimulation. Using whole cell patch-clamp and confocal Ca2+ imaging of cardiomyocytes derived from TAB hearts (TCMs) we found that membrane-permeable SK enhancers NS309 and CyPPA (10 μM) attenuated frequency of spontaneous Ca2+ waves and delayed afterdepolarizations. Furthermore, mSK inhibition enhanced (UCL-1684, 1 μM); while activation reduced mitochondrial ROS production in TCMs measured with MitoSOX. Protein oxidation assays demonstrated that increased oxidation of ryanodine receptors (RyRs) in TCMs was reversed by SK enhancers. Experiments in permeabilized TCMs showed that SK enhancers restored SR Ca2+ content, suggestive of substantial improvement in RyR function. Conclusion: These data suggest that enhancement of mSK channels in hypertrophic rat hearts protects from Ca2+-dependent arrhythmia and suggest that the protection is mediated via decreased mitochondrial ROS and subsequent decreased oxidation of reactive cysteines in RyR, which ultimately leads to stabilization of RyR-mediated Ca2+ release.

KW - Cardiac hypertrophy

KW - Reactive oxygen species

KW - Ryanodine receptor

KW - Small conductance Ca-activated Kchannels

KW - Ventricular arrhythmia

UR - https://www.scopus.com/pages/publications/85026314465

U2 - 10.1093/cvr/cvx005

DO - 10.1093/cvr/cvx005

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C2 - 28096168

AN - SCOPUS:85026314465

SN - 0008-6363

VL - 113

SP - 343

EP - 353

JO - Cardiovascular Research

JF - Cardiovascular Research

IS - 3