The switching role of β-adrenergic receptor signalling in cell survival or death decision of cardiomyocytes

Shin, Sung-Young; Kim, Tae-Yong; Lee, Ho Sung; Kang, Jun Hyuk; Lee, Ji Young; Cho, Kwang Hyun; Kim, Do Han

doi:10.1038/ncomms6777

Cited by 60 publications

(55 citation statements)

References 65 publications

(88 reference statements)

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“…Temporal dynamics of phosphorylation events upon GPCR activation are highly complex (31)(32)(33); therefore, we performed time course experiments and demonstrated the phosphorylation of ERK within the first 15 min after AngII stimulation (14). Thus, we chose this time point for our proteomic study.…”

Section: Angii Leads To Quantitative Changes In the Phosphoproteome Omentioning

confidence: 99%

Angiotensin II regulates phosphorylation of actin‐associated proteins in human podocytes

et al. 2017

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Within the kidney, angiotensin II (AngII) targets different cell types in the vasculature, tubuli, and glomeruli. An important part of the renal filtration barrier is composed of podocytes with their actin-rich foot processes. In this study, we used stable isotope labeling with amino acids in cell culture coupled to mass spectrometry to characterize relative changes in the phosphoproteome of human podocytes in response to short-term treatment with AngII. In 4 replicates, we identified a total of 17,956 peptides that were traceable to 2081 distinct proteins. Bioinformatic analyses revealed that among the increasingly phosphorylated peptides are predominantly peptides that are related to actin filaments, cytoskeleton, lamellipodia, mammalian target of rapamycin, and MAPK signaling. Among others, this screening approach highlighted the increased phosphorylation of actin-bundling protein, L-plastin (LCP1). AngII-dependent phosphorylation of LCP1 in cultured podocytes was mediated by the kinases ERK, p90 ribosomal S6 kinase, PKA, or PKC. LCP1 phosphorylation increased filopodia formation. In addition, treatment with AngII led to LCP1 redistribution to the cell margins, membrane ruffling, and formation of lamellipodia. Our data highlight the importance of AngII-triggered actin cytoskeleton-associated signal transduction in

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Section: Angii Leads To Quantitative Changes In the Phosphoproteome Omentioning

confidence: 99%

Angiotensin II regulates phosphorylation of actin‐associated proteins in human podocytes

et al. 2017

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“…c-Src/ERK has been demonstrated to activate a survival signal through up regulation of the anti-apoptotic/survival protein, Bcl2 [27]. Western blot examination of Bcl2 revealed a single polypeptidẽ 26 kDa which was barely detectable in Wt myocardium, but was induced~100 fold by E2F6 expression (p-value: 0.00001) (Fig.…”

Section: E2f6 Activates C-src/erk and Bcl2 In E2f6-tg Myocardiummentioning

confidence: 93%

Interplay between the E2F pathway and β-adrenergic signaling in the pathological hypertrophic response of myocardium

Major¹,

Salih²,

Tuana³

2015

Journal of Molecular and Cellular Cardiology

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“…These investigators combined experimental measurements with simulations to uncover mechanisms by which high and sustained doses of the β-adrenergic receptor agonist isoproterenol could increase myocyte susceptibility to apoptosis (Shin et al, 2014). This study is an important example of how simulations often generate novel experimentally-testable predictions, and the work can potentially be extended to examine TKI-induced toxicity.…”

Section: Initial Efforts To Use Qsp Approaches To Understand Tki-indumentioning

confidence: 99%

“…For instance, cell death via apoptosis, which may be important in the development of toxicity caused by some TKIs, has been described mathematically by many previous models (Schleich and Lavrik, 2013;Shin et al, 2014). Once these are tuned to reflect apoptotic signaling in cardiac myocytes, the models can be integrated with the experimental gene expression data to generate novel predictions.…”

Section: Future Directionsmentioning

confidence: 99%

“…Another notable recent effort is a study by Shin et al (2014). These investigators combined experimental measurements with simulations to uncover mechanisms by which high and sustained doses of the β-adrenergic receptor agonist isoproterenol could increase myocyte susceptibility to apoptosis (Shin et al, 2014).…”

Section: Initial Efforts To Use Qsp Approaches To Understand Tki-indumentioning

confidence: 99%

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Mechanistic Systems Modeling to Improve Understanding and Prediction of Cardiotoxicity Caused by Targeted Cancer Therapeutics

Shim

2018

Biophysical Journal

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Tyrosine kinase inhibitors (TKIs) are highly potent cancer therapeutics that have been linked with serious cardiotoxicity, including left ventricular dysfunction, heart failure, and QT prolongation. TKI-induced cardiotoxicity is thought to result from interference with tyrosine kinase activity in cardiomyocytes, where these signaling pathways help to control critical processes such as survival signaling, energy homeostasis, and excitation-contraction coupling. However, mechanistic understanding is limited at present due to the complexities of tyrosine kinase signaling, and the wide range of targets inhibited by TKIs. Here, we review the use of TKIs in cancer and the cardiotoxicities that have been reported, discuss potential mechanisms underlying cardiotoxicity, and describe recent progress in achieving a more systematic understanding of cardiotoxicity via the use of mechanistic models. In particular, we argue that future advances are likely to be enabled by studies that combine large-scale experimental measurements with Quantitative Systems Pharmacology (QSP) models describing biological mechanisms and dynamics. As such approaches have proven extremely valuable for understanding and predicting other drug toxicities, it is likely that QSP modeling can be successfully applied to cardiotoxicity induced by TKIs. We conclude by discussing a potential strategy for integrating genome-wide expression measurements with models, illustrate initial advances in applying this approach to cardiotoxicity, and describe challenges that must be overcome to truly develop a mechanistic and systematic understanding of cardiotoxicity caused by TKIs.

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The switching role of β-adrenergic receptor signalling in cell survival or death decision of cardiomyocytes

Cited by 60 publications

References 65 publications

Angiotensin II regulates phosphorylation of actin‐associated proteins in human podocytes

Angiotensin II regulates phosphorylation of actin‐associated proteins in human podocytes

Interplay between the E2F pathway and β-adrenergic signaling in the pathological hypertrophic response of myocardium

Mechanistic Systems Modeling to Improve Understanding and Prediction of Cardiotoxicity Caused by Targeted Cancer Therapeutics

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