Biphasic effect of SIN-1 is reliant upon cardiomyocyte contractile state

Kohr, Mark J.; Wang, Honglan; Wheeler, Debra G.; Murugesan, V.; Zweíer, Jay L.; Ziolo, Mark T.

doi:10.1016/j.freeradbiomed.2008.03.019

Cited by 20 publications

(29 citation statements)

References 41 publications

(79 reference statements)

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“…These data are consistent with our previous study that showed that low levels of exogenous peroxynitrite (produced from SIN-1) increased basal Ca 2ϩ transient and shortening amplitude in murine myocytes. Interestingly, similar to NOS1 inhibition, the contractile effects of SIN-1 were absent in PLB Ϫ/Ϫ myocytes (22). However, it still remains to be determined whether NO itself or other reactive nitrogen species are also part of the NOS1 signaling pathway.…”

Section: Discussionmentioning

confidence: 91%

Neuronal nitric oxide synthase signaling within cardiac myocytes targets phospholamban

Wang

Kohr

Traynham

et al. 2008

American Journal of Physiology-Cell Physiology

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Studies have shown that neuronal nitric oxide synthase (nNOS, NOS1) knockout mice (NOS1-/-) have increased or decreased contractility, but consistently have found a slowed rate of intracellular Ca2+ ([Ca2+]i) decline and relengthening. Contraction and [Ca2+]i decline are determined by many factors, one of which is phospholamban (PLB). The purpose of this study is to determine the involvement of PLB in the NOS1-mediated effects. Force-frequency experiments were performed in trabeculae isolated from NOS1-/- and wild-type (WT) mice. We also simultaneously measured Ca2+ transients (Fluo-4) and cell shortening (edge detection) in myocytes isolated from WT, NOS1-/-, and PLB-/- mice. NOS1-/- trabeculae had a blunted force-frequency response and prolonged relaxation. We observed similar effects in myocytes with NOS1 knockout or specific NOS1 inhibition with S-methyl-l-thiocitrulline (SMLT) in WT myocytes (i.e., decreased Ca2+ transient and cell shortening amplitudes and prolonged decline of [Ca2+]i). Alternatively, NOS1 inhibition with SMLT in PLB-/- myocytes had no effect. Acute inhibition of NOS1 with SMLT in WT myocytes also decreased basal PLB serine16 phosphorylation. Furthermore, there was a decreased SR Ca2+ load with NOS1 knockout or inhibition, which is consistent with the negative contractile effects. Perfusion with FeTPPS (peroxynitrite decomposition catalyst) mimicked the effects of NOS1 knockout or inhibition. beta-Adrenergic stimulation restored the slowed [Ca2+]i decline in NOS1-/- myocytes, but a blunted contraction remained, suggesting additional protein target(s). In summary, NOS1 inhibition or knockout leads to decreased contraction and slowed [Ca2+]i decline, and this effect is absent in PLB-/- myocytes. Thus NOS1 signaling modulates PLB serine16 phosphorylation, in part, via peroxynitrite.

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Section: Discussionmentioning

confidence: 91%

Neuronal nitric oxide synthase signaling within cardiac myocytes targets phospholamban

Wang

Kohr

Traynham

et al. 2008

American Journal of Physiology-Cell Physiology

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“…Indeed, it was reported that 10 µmol/L SIN-1 would correspond to 3 nmol/L of peroxynitrite and thus represent physiological rather than pathological conditions [48]. Furthermore, the differences in the total (175% increase at 15 min) and protein-specific (significant increase at 30 min) carbonylation suggested that compared to proteins, lipids might be the primary targets of ROS/RNS.…”

Section: Resultsmentioning

confidence: 99%

“…In the presence of carbon dioxide (CO 2 ) peroxynitrite anion forms nitroso-peroxocarbonate (ONOOCO 2 - ), which in turn decomposes to • NO 2 , CO 3 - and NO 3 - [47]. We and others have previously demonstrated the complex nitroxidative effect of SIN-1 treatment in cell culture models [46], [48], [49], [50]. Here, free radical production in SIN-1-treated (10 µmol/L) CM was monitored by DCFDA assay (Fig.…”

Section: Resultsmentioning

confidence: 99%

Cross-talk between lipid and protein carbonylation in a dynamic cardiomyocyte model of mild nitroxidative stress

et al. 2017

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Reactive oxygen and nitrogen species (ROS/RNS) play an important role in the regulation of cardiac function. Increase in ROS/RNS concentration results in lipid and protein oxidation and is often associated with onset and/or progression of many cardiovascular disorders. However, interplay between lipid and protein modifications has not been simultaneously studied in detail so far. Biomolecule carbonylation is one of the most common biomarkers of oxidative stress. Using a dynamic model of nitroxidative stress we demonstrated rapid changes in biomolecule carbonylation in rat cardiomyocytes. Levels of carbonylated species increased as early as 15 min upon treatment with the peroxynitrite donor, 3-morpholinosydnonimine (SIN-1), and decreased to values close to control after 16 h. Total (lipids+proteins) vs. protein-specific carbonylation showed different dynamics, with a significant increase in protein-bound carbonyls at later time points. Treatment with SIN-1 in combination with inhibitors of proteasomal and autophagy/lysosomal degradation pathways allowed confirmation of a significant role of the proteasome in the degradation of carbonylated proteins, whereas lipid carbonylation increased in the presence of autophagy/lysosomal inhibitors. Electrophilic aldehydes and ketones formed by lipid peroxidation were identified and relatively quantified using LC-MS/MS. Molecular identity of reactive species was used for data-driven analysis of their protein targets. Combination of different enrichment strategies with LC-MS/MS analysis allowed identification of more than 167 unique proteins with 332 sites modified by electrophilic lipid peroxidation products. Gene ontology analysis of modified proteins demonstrated enrichment of several functional categories including proteins involved in cytoskeleton, extracellular matrix, ion channels and their regulation. Using calcium mobilization assays, the effect of nitroxidative stress on the activity of several ion channels was further confirmed.

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“…But, similar to ROS, may also modulate the activity of various kinases and phosphatases to change the protein phosphorylation status. We have previously shown that a peroxynitrite donor (SIN-1) in a low dose was able to increase PLB Serine16 phosphorylation via activation of PKA (96,97). Surprisingly, the peroxynitrite-mediated increase in PKA activity occurred in the absence of cAMP, and most likely occurs via Snitrosylation (28).…”

Section: Nitroso-redox Imbalance In Hf 2049mentioning

confidence: 92%

Abnormal Ca²⁺Cycling in Failing Ventricular Myocytes: Role of NOS1-Mediated Nitroso-Redox Balance

Ziolo

Houser

2014

Antioxidants & Redox Signaling

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Significance: Heart failure (HF) results from poor heart function and is the leading cause of death in Western society. Abnormalities of Ca 2+ handling at the level of the ventricular myocyte are largely responsible for much of the poor heart function. Recent Advances: Although studies have unraveled numerous mechanisms for the abnormal Ca 2+ handling, investigations over the past decade have indicated that much of the contractile dysfunction and adverse remodeling that occurs in HF involves oxidative stress. Critical Issues: Regrettably, antioxidant therapy has been an immense disappointment in clinical trials. Thus, redox signaling is being reassessed to elucidate why antioxidants failed to treat HF. Future Directions: A recently identified aspect of redox signaling (specifically the superoxide anion radical) is its interaction with nitric oxide, known as the nitroso-redox balance. There is a large nitroso-redox imbalance with HF, and we suggest that correcting this imbalance may be able to restore myocyte contraction and improve heart function.

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Biphasic effect of SIN-1 is reliant upon cardiomyocyte contractile state

Cited by 20 publications

References 41 publications

Neuronal nitric oxide synthase signaling within cardiac myocytes targets phospholamban

Neuronal nitric oxide synthase signaling within cardiac myocytes targets phospholamban

Cross-talk between lipid and protein carbonylation in a dynamic cardiomyocyte model of mild nitroxidative stress

Abnormal Ca²⁺Cycling in Failing Ventricular Myocytes: Role of NOS1-Mediated Nitroso-Redox Balance

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Biphasic effect of SIN-1 is reliant upon cardiomyocyte contractile state

Cited by 20 publications

References 41 publications

Neuronal nitric oxide synthase signaling within cardiac myocytes targets phospholamban

Neuronal nitric oxide synthase signaling within cardiac myocytes targets phospholamban

Cross-talk between lipid and protein carbonylation in a dynamic cardiomyocyte model of mild nitroxidative stress

Abnormal Ca2+Cycling in Failing Ventricular Myocytes: Role of NOS1-Mediated Nitroso-Redox Balance

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Abnormal Ca²⁺Cycling in Failing Ventricular Myocytes: Role of NOS1-Mediated Nitroso-Redox Balance