TY  - JOUR
AU  - Ljubojević-Holzer, Senka
AU  - Herren, Anthony W.
AU  - Đalinac, Nataša
AU  - Voglhuber, Julia
AU  - Morotti, Stefano
AU  - Holzer, Michael
AU  - Wood, Brent M.
AU  - Abdellatif, Mahmoud
AU  - Matzer, Ingrid
AU  - Sacherer, Michael
AU  - Radulović, Snježana
AU  - Wallner, Markus
AU  - Ivanov, Milan
AU  - Wagner, Stefan
AU  - Sossalla, Samuel
AU  - von Lewinski, Dirk
AU  - Pieske, Burkert
AU  - Brown, Joan Heller
AU  - Sedej, Simon
AU  - Bossuyt, Julie
AU  - Bers, Donald M.
PY  - 2020
UR  - http://rimi.imi.bg.ac.rs/handle/123456789/991
AB  - Rationale: CaMKII (Ca2+-Calmodulin dependent protein kinase) delta C activation is implicated in pathological progression of heart failure (HF) and CaMKII delta C transgenic mice rapidly develop HF and arrhythmias. However, little is known about early spatio-temporal Ca(2+)handling and CaMKII activation in hypertrophy and HF. Objective: To measure time- and location-dependent activation of CaMKII delta C signaling in adult ventricular cardiomyocytes, during transaortic constriction (TAC) and in CaMKII delta C transgenic mice. Methods and Results: We used human tissue from nonfailing and HF hearts, 4 mouse lines: wild-type, KO (CaMKII delta-knockout), CaMKII delta C transgenic in wild-type (TG), or KO background, and wild-type mice exposed to TAC. Confocal imaging and biochemistry revealed disproportional CaMKII delta C activation and accumulation in nuclear and perinuclear versus cytosolic regions at 5 days post-TAC. This CaMKII delta activation caused a compensatory increase in sarcoplasmic reticulum Ca(2+)content, Ca(2+)transient amplitude, and [Ca2+] decline rates, with reduced phospholamban expression, all of which were most prominent near and in the nucleus. These early adaptive effects in TAC were entirely mimicked in young CaMKII delta TG mice (6-8 weeks) where no overt cardiac dysfunction was present. The (peri)nuclear CaMKII accumulation also correlated with enhanced HDAC4 (histone deacetylase) nuclear export, creating a microdomain for transcriptional regulation. At longer times both TAC and TG mice progressed to overt HF (at 45 days and 11-13 weeks, respectively), during which time the compensatory Ca(2+)transient effects reversed, but further increases in nuclear and time-averaged [Ca2+] and CaMKII activation occurred. CaMKII delta TG mice lacking delta B exhibited more severe HF, eccentric myocyte growth, and nuclear changes. Patient HF samples also showed greatly increased CaMKII delta expression, especially for CaMKII delta C in nuclear fractions. Conclusions: We conclude that in early TAC perinuclear CaMKII delta C activation promotes adaptive increases in myocyte Ca(2+)transients and nuclear transcriptional responses but that chronic progression of this nuclear Ca2+-CaMKII delta C axis contributes to eccentric hypertrophy and HF.
PB  - Lippincott Williams & Wilkins, Philadelphia
T2  - Circulation Research
T1  - CaMKII delta C Drives Early Adaptive Ca(2+)Change and Late Eccentric Cardiac Hypertrophy
EP  - 1178
IS  - 9
SP  - 1159
VL  - 127
DO  - 10.1161/CIRCRESAHA.120.316947
ER  - 

@article{
author = "Ljubojević-Holzer, Senka and Herren, Anthony W. and Đalinac, Nataša and Voglhuber, Julia and Morotti, Stefano and Holzer, Michael and Wood, Brent M. and Abdellatif, Mahmoud and Matzer, Ingrid and Sacherer, Michael and Radulović, Snježana and Wallner, Markus and Ivanov, Milan and Wagner, Stefan and Sossalla, Samuel and von Lewinski, Dirk and Pieske, Burkert and Brown, Joan Heller and Sedej, Simon and Bossuyt, Julie and Bers, Donald M.",
year = "2020",
abstract = "Rationale: CaMKII (Ca2+-Calmodulin dependent protein kinase) delta C activation is implicated in pathological progression of heart failure (HF) and CaMKII delta C transgenic mice rapidly develop HF and arrhythmias. However, little is known about early spatio-temporal Ca(2+)handling and CaMKII activation in hypertrophy and HF. Objective: To measure time- and location-dependent activation of CaMKII delta C signaling in adult ventricular cardiomyocytes, during transaortic constriction (TAC) and in CaMKII delta C transgenic mice. Methods and Results: We used human tissue from nonfailing and HF hearts, 4 mouse lines: wild-type, KO (CaMKII delta-knockout), CaMKII delta C transgenic in wild-type (TG), or KO background, and wild-type mice exposed to TAC. Confocal imaging and biochemistry revealed disproportional CaMKII delta C activation and accumulation in nuclear and perinuclear versus cytosolic regions at 5 days post-TAC. This CaMKII delta activation caused a compensatory increase in sarcoplasmic reticulum Ca(2+)content, Ca(2+)transient amplitude, and [Ca2+] decline rates, with reduced phospholamban expression, all of which were most prominent near and in the nucleus. These early adaptive effects in TAC were entirely mimicked in young CaMKII delta TG mice (6-8 weeks) where no overt cardiac dysfunction was present. The (peri)nuclear CaMKII accumulation also correlated with enhanced HDAC4 (histone deacetylase) nuclear export, creating a microdomain for transcriptional regulation. At longer times both TAC and TG mice progressed to overt HF (at 45 days and 11-13 weeks, respectively), during which time the compensatory Ca(2+)transient effects reversed, but further increases in nuclear and time-averaged [Ca2+] and CaMKII activation occurred. CaMKII delta TG mice lacking delta B exhibited more severe HF, eccentric myocyte growth, and nuclear changes. Patient HF samples also showed greatly increased CaMKII delta expression, especially for CaMKII delta C in nuclear fractions. Conclusions: We conclude that in early TAC perinuclear CaMKII delta C activation promotes adaptive increases in myocyte Ca(2+)transients and nuclear transcriptional responses but that chronic progression of this nuclear Ca2+-CaMKII delta C axis contributes to eccentric hypertrophy and HF.",
publisher = "Lippincott Williams & Wilkins, Philadelphia",
journal = "Circulation Research",
title = "CaMKII delta C Drives Early Adaptive Ca(2+)Change and Late Eccentric Cardiac Hypertrophy",
pages = "1178-1159",
number = "9",
volume = "127",
doi = "10.1161/CIRCRESAHA.120.316947"
}

Ljubojević-Holzer, S., Herren, A. W., Đalinac, N., Voglhuber, J., Morotti, S., Holzer, M., Wood, B. M., Abdellatif, M., Matzer, I., Sacherer, M., Radulović, S., Wallner, M., Ivanov, M., Wagner, S., Sossalla, S., von Lewinski, D., Pieske, B., Brown, J. H., Sedej, S., Bossuyt, J.,& Bers, D. M.. (2020). CaMKII delta C Drives Early Adaptive Ca(2+)Change and Late Eccentric Cardiac Hypertrophy. in Circulation Research
Lippincott Williams & Wilkins, Philadelphia., 127(9), 1159-1178.
https://doi.org/10.1161/CIRCRESAHA.120.316947

Ljubojević-Holzer S, Herren AW, Đalinac N, Voglhuber J, Morotti S, Holzer M, Wood BM, Abdellatif M, Matzer I, Sacherer M, Radulović S, Wallner M, Ivanov M, Wagner S, Sossalla S, von Lewinski D, Pieske B, Brown JH, Sedej S, Bossuyt J, Bers DM. CaMKII delta C Drives Early Adaptive Ca(2+)Change and Late Eccentric Cardiac Hypertrophy. in Circulation Research. 2020;127(9):1159-1178.
doi:10.1161/CIRCRESAHA.120.316947 .

Ljubojević-Holzer, Senka, Herren, Anthony W., Đalinac, Nataša, Voglhuber, Julia, Morotti, Stefano, Holzer, Michael, Wood, Brent M., Abdellatif, Mahmoud, Matzer, Ingrid, Sacherer, Michael, Radulović, Snježana, Wallner, Markus, Ivanov, Milan, Wagner, Stefan, Sossalla, Samuel, von Lewinski, Dirk, Pieske, Burkert, Brown, Joan Heller, Sedej, Simon, Bossuyt, Julie, Bers, Donald M., "CaMKII delta C Drives Early Adaptive Ca(2+)Change and Late Eccentric Cardiac Hypertrophy" in Circulation Research, 127, no. 9 (2020):1159-1178,
https://doi.org/10.1161/CIRCRESAHA.120.316947 . .