The Interplay between S-Glutathionylation and Phosphorylation of Cardiac Troponin I and Myosin Binding Protein C in End-Stage Human Failing Hearts

Budde, Heidi; Hassoun, Roua; Tangos, Melina; Zhazykbayeva, Saltanat; Herwig, Melissa; Varatnitskaya, Marharyta; Sieme, Marcel; Delalat, Simin; Sultana, Innas; Kolijn, Detmar; Gömöri, Kamilla; Jarkas, Muhammad; Lódi, Mária; Jaquet, Kornélia; Kov́acs, Árṕad; Mannherz, Hans Georg; Sequeira, Vasco; Mügge, Andreas; Leichert, Lars I.; Sossalla, Samuel; Hamdani, Nazha

doi:10.3390/antiox10071134

Cited by 16 publications

(27 citation statements)

References 74 publications

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“…Hence, the net effect of myofilament sensitization/desensitization is defined by synergistic balance between different kinases/phosphatases. 9,14 In the current study, and in line with previous work reporting the reduction in PKA-dependent phosphorylation of cTnI in end stage human failing hearts, 19,43,44 we found PKA-/PKG-dependent hypophosphorylation of cTnI at Ser 23/24 in 8-month VO compared with 8-month Ctrl group. It is well established that in HF and due to the internalization of β-adrenergic receptors, the receptor density and activity are reduced leading to decreased PKA-dependent phosphorylation of cTnI at Ser 23/24.…”

Section: Altered Phosphorylation Status Of Sarcomeric Proteins and My...supporting

confidence: 92%

“…[16][17][18] Previous research by us and others has demonstrated the role of oxidative stress and inflammation in altering various signalling pathways crucial for cardiomyocyte function among which are the kinases pathways. 4,19 Reactive oxygen species (ROS) might directly oxidize kinases or their targets leading to changes in their activity/binding affinity, respectively. 19 For example, oxidation of the regulatory CaMKII domain at Met 281/282 induces a Ca 2+ /CaM-independent activation.…”

Section: Introductionmentioning

confidence: 99%

“…4,19 Reactive oxygen species (ROS) might directly oxidize kinases or their targets leading to changes in their activity/binding affinity, respectively. 19 For example, oxidation of the regulatory CaMKII domain at Met 281/282 induces a Ca 2+ /CaM-independent activation. 20,21 Through the regulation of Ca 2+ homeostasis and sarco/endoplasmic reticulum Ca 2+ -ATPase (SERCA) function, CaMKIIδ is involved in cardiac remodelling and hypertrophic responses to mechanical overload.…”

Section: Introductionmentioning

confidence: 99%

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Ca2+/calmodulin‐dependent protein kinase II and protein kinase G oxidation contributes to impaired sarcomeric proteins in hypertrophy model

et al. 2022

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Aims Volume overload (VO) induced hypertrophy is one of the hallmarks to the development of heart diseases. Understanding the compensatory mechanisms involved in this process might help preventing the disease progression. Methods and resultsTherefore, the present study used 2 months old Wistar rats, which underwent an aortocaval fistula to develop VO-induced hypertrophy. The animals were subdivided into four different groups, two sham operated animals served as age-matched controls and two groups with aortocaval fistula. Echocardiography was performed prior termination after 4and 8-month. Functional and molecular changes of several sarcomeric proteins and their signalling pathways involved in the regulation and modulation of cardiomyocyte function were investigated. ResultsThe model was characterized with preserved ejection fraction in all groups and with elevated heart/body weight ratio, left/right ventricular and atrial weight at 4-and 8-month, which indicates VO-induced hypertrophy. In addition, 8-months groups showed increased left ventricular internal diameter during diastole, RV internal diameter, stroke volume and velocity-time index compared with their age-matched controls. These changes were accompanied by increased Ca 2+ sensitivity and titin-based cardiomyocyte stiffness in 8-month VO rats compared with other groups. The altered cardiomyocyte mechanics was associated with phosphorylation deficit of sarcomeric proteins cardiac troponin I, myosin binding protein C and titin, also accompanied with impaired signalling pathways involved in phosphorylation of these sarcomeric proteins in 8-month VO rats compared with age-matched control group. Impaired protein phosphorylation status and dysregulated signalling pathways were associated with significant alterations in the oxidative status of both kinases CaMKII and PKG explaining by this the elevated Ca 2+ sensitivity and titin-based cardiomyocyte stiffness and perhaps the development of hypertrophy. Conclusions Our findings showed VO-induced cardiomyocyte dysfunction via deranged phosphorylation of myofilament proteins and signalling pathways due to increased oxidative state of CaMKII and PKG and this might contribute to the development of hypertrophy.

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Section: Altered Phosphorylation Status Of Sarcomeric Proteins and My...supporting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Ca2+/calmodulin‐dependent protein kinase II and protein kinase G oxidation contributes to impaired sarcomeric proteins in hypertrophy model

et al. 2022

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“…Accordingly, oxidized troponin I does not bind to troponin T, and the altered S-glutathionylation (an intracellular process directly regulated by the local redox status of the microenvironment) of cMyBP-C induces an impairment of cellular relaxation, with unaltered cellular Ca 2+ dynamics. The reduction in cMyBP-C S-glutathionylation improves diastolic dysfunction, suggesting a strong link between S-glutathionylation and diastolic dysfunction [ 102 ].…”

Section: The Proteins For Muscle Contraction: From Physiological To Pathological Conditionsmentioning

confidence: 99%

The Oxidative Balance Orchestrates the Main Keystones of the Functional Activity of Cardiomyocytes

Bevere

Morabito

Guarnieri

2022

Oxidative Medicine and Cellular Longevity

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This review is aimed at providing an overview of the key hallmarks of cardiomyocytes in physiological and pathological conditions. The main feature of cardiac tissue is the force generation through contraction. This process requires a conspicuous energy demand and therefore an active metabolism. The cardiac tissue is rich of mitochondria, the powerhouses in cells. These organelles, producing ATP, are also the main sources of ROS whose altered handling can cause their accumulation and therefore triggers detrimental effects on mitochondria themselves and other cell components thus leading to apoptosis and cardiac diseases. This review highlights the metabolic aspects of cardiomyocytes and wanders through the main systems of these cells: (a) the unique structural organization (such as different protein complexes represented by contractile, regulatory, and structural proteins); (b) the homeostasis of intracellular Ca2+ that represents a crucial ion for cardiac functions and E-C coupling; and (c) the balance of Zn2+, an ion with a crucial impact on the cardiovascular system. Although each system seems to be independent and finely controlled, the contractile proteins, intracellular Ca2+ homeostasis, and intracellular Zn2+ signals are strongly linked to each other by the intracellular ROS management in a fascinating way to form a “functional tetrad” which ensures the proper functioning of the myocardium. Nevertheless, if ROS balance is not properly handled, one or more of these components could be altered resulting in deleterious effects leading to an unbalance of this “tetrad” and promoting cardiovascular diseases. In conclusion, this “functional tetrad” is proposed as a complex network that communicates continuously in the cardiomyocytes and can drive the switch from physiological to pathological conditions in the heart.

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“… 19 More broadly, cMyBPC has been shown to be differentially phosphorylated in animal models of myocardial stunning and models of age-related cardiac dysfunction. 20 , 21 Furthermore, cardiac hypertrophy and heart failure have been associated with reduced overall cMyBPC phosphorylation levels, 22 − 26 and decreased cMyBPC phosphorylation is correlated with dysfunction in ischemia. 27 , 28 …”

Section: Introductionmentioning

confidence: 99%

Identification of Phosphorylation and Other Post-Translational Modifications in the Central C4C5 Domains of Murine Cardiac Myosin Binding Protein C

et al. 2022

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Cardiac myosin binding protein C (cMyBPC) is a critical multidomain protein that modulates myosin cross bridge behavior and cardiac contractility. cMyBPC is principally regulated by phosphorylation of the residues within the M-domain of its N-terminus. However, not much is known about the phosphorylation or other post-translational modification (PTM) landscape of the central C4C5 domains. In this study, the presence of phosphorylation outside the M-domain was confirmed in vivo using mouse models expressing cMyBPC with nonphosphorylatable serine (S) to alanine substitutions. Purified recombinant mouse C4C5 domain constructs were incubated with 13 different kinases, and samples from the 6 strongest kinases were chosen for mass spectrometry analysis. A total of 26 unique phosphorylated peptides were found, representing 13 different phosphorylation sites including 10 novel sites. Parallel reaction monitoring and subsequent mutagenesis experiments revealed that the S690 site (UniProtKB O70468) was the predominant target of PKA and PKG1. We also report 6 acetylation and 7 ubiquitination sites not previously described in the literature. These PTMs demonstrate the possibility of additional layers of regulation and potential importance of the central domains of cMyBPC in cardiac health and disease. Data are available via ProteomeXchange with identifier PXD031262.

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The Interplay between S-Glutathionylation and Phosphorylation of Cardiac Troponin I and Myosin Binding Protein C in End-Stage Human Failing Hearts

Cited by 16 publications

References 74 publications

Ca2+/calmodulin‐dependent protein kinase II and protein kinase G oxidation contributes to impaired sarcomeric proteins in hypertrophy model

Ca2+/calmodulin‐dependent protein kinase II and protein kinase G oxidation contributes to impaired sarcomeric proteins in hypertrophy model

The Oxidative Balance Orchestrates the Main Keystones of the Functional Activity of Cardiomyocytes

Identification of Phosphorylation and Other Post-Translational Modifications in the Central C4C5 Domains of Murine Cardiac Myosin Binding Protein C

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