Philip Nickson scite author profile

The endoplasmic reticulum (ER) is a multifunctional organelle responsible for the synthesis and folding of proteins as well as calcium storage and signaling. Perturbations of ER function cause ER stress leading to the unfolded protein response (UPR), which includes inhibition of protein synthesis, protein refolding and clearance of misfolded proteins. The UPR aims at restoring cellular homeostasis, however, prolonged ER stress can trigger apoptosis. ER stress-induced apoptosis has been implicated in the pathogenesis of various diseases such as brain ischemia/reperfusion, neurodegeneration, diabetes and, most recently, myocardial infarction and heart failure. Initial events leading to UPR and apoptosis in the heart include protein oxidation and disturbed calcium handling upon ischemia/reperfusion, and forced protein synthesis during cardiac hypertrophy. While XBP-1 and ATF6-mediated induction of ER chaperones seems to protect the heart from ischemia/reperfusion injury, the PERK/ATF4/CHOP branch of the UPR might transmit proapoptotic signals. The precise mechanism of ER stress-induced cardiomyocyte apoptosis remains elusive, however, recent data suggest that the mitochondrial apoptotic machinery is recruited through the upregulation of Puma, a proapoptotic member of the Bcl-2 family. Importantly, suppression of Puma activity prevented both ER stress and ischemia/reperfusion-induced cardiomyocyte loss, highlighting the ER stress pathways as potential therapeutic targets in cardiovascular diseases.

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Targeted deletion of Puma attenuates cardiomyocyte death and improves cardiac function during ischemia-reperfusion

Tóth

Jeffers

Nickson

et al. 2006

American Journal of Physiology-Heart and Circulatory Physiology

122

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The p53-upregulated modulator of apoptosis (Puma), a BH3-only member of the Bcl-2 protein family, is required for p53-dependent and -independent forms of apoptosis and has been implicated in the pathomechanism of several diseases, including cancer, acquired immunodeficiency syndrome, and ischemic brain disease. The role of Puma in cardiomyocyte death, however, has not been analyzed. On the basis of the ability of Puma to integrate diverse cell death stimuli, we hypothesized that Puma might be critical for cardiomyocyte death upon ischemia-reperfusion (I/R) of the heart. Here we show that hypoxia-reoxygenation of isolated cardiomyocytes led to an increase in Puma mRNA and protein levels. Moreover, if Puma was delivered by an adenoviral construct, cardiomyocytes died by apoptosis. Under ATP-depleted conditions, however, Puma overexpression primarily induced necrosis, suggesting that Puma is involved in the development of both types of cell death. Consistent with these findings, targeted deletion of Puma in a mouse model attenuated both apoptosis and necrosis. When the Langendorff ex vivo I/R model was used, infarcts were approximately 50% smaller in Puma(-/-) than in wild-type mice. As a result, after I/R, cardiac function was significantly better preserved in Puma(-/-) mice than in their wild-type littermates. Our study thus establishes Puma as an essential mediator of cardiomyocyte death upon I/R injury and offers a novel therapeutic target to limit cell loss in ischemic heart disease.

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PUMA is critical for neonatal cardiomyocyte apoptosis induced by endoplasmic reticulum stress

Nickson

Tóth

Erhardt

2007

Cardiovascular Research

116

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Differential Regulation of Cardiomyocyte Survival and Hypertrophy by MDM2, an E3 Ubiquitin Ligase

Tóth

Nickson

Qin

et al. 2006

Journal of Biological Chemistry

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MDM2 is an E3 ubiquitin ligase that regulates the proteasomal degradation and activity of proteins involved in cell growth and apoptosis, including the tumor suppressors p53 and retinoblastoma and the transcription factor E2F1. Although the effect of several MDM2 targets on cardiomyocyte survival and hypertrophy has already been investigated, the role of MDM2 in these processes has not yet been established. We have, therefore, analyzed the effect of overexpression as well as inhibition of MDM2 on cardiac ischemia/ reperfusion injury and hypertrophy. Here we show that isolated cardiac myocytes overexpressing MDM2 acquired resistance to hypoxia/reoxygenation-induced cell death. Conversely, inactivation of MDM2 by a peptide inhibitor resulted in elevated p53 levels and promoted hypoxia/reoxygenation-induced apoptosis. Consistent with this, decreased expression of MDM2 in a genetic mouse model was accompanied by reduced functional recovery of the left ventricles determined with the Langendorff ex vivo model of ischemia/ reperfusion. In contrast to cell survival, cell hypertrophy induced by the ␣-agonists phenylephrine or endothelin-1 was inhibited by MDM2 overexpression. Collectively, our studies indicate that MDM2 promotes survival and attenuates hypertrophy of cardiac myocytes. This differential regulation of cell growth and cell survival is unique, because most other survival factors are prohypertrophic. MDM2, therefore, might be a potential therapeutic target to down-regulate both cell death and pathologic hypertrophy during remodeling upon cardiac infarction. In addition, our data also suggest that cancer treatments with MDM2 inhibitors to reactivate p53 may have adverse cardiac side effects by promoting cardiomyocyte death.The murine double minute 2 (mdm2) 2 gene was originally discovered as one of three genes that was overexpressed in spontaneously transformed mouse BALB/c fibroblasts (1, 2). Overexpression of the mdm2 gene product was shown to lead to transformation, which requires the binding of MDM2 to the tumor suppressor p53 (3). Through this protein-protein interaction, MDM2 inhibits the transcriptional activity of p53 (4). In addition, MDM2 also promotes the ubiquitination and proteasomal degradation of p53 by functioning as an E3 ubiquitin ligase (5, 6). p53 exerts its tumor suppressor effect by transcriptionally activating many target genes, including p21 and PUMA/Noxa, thereby promoting growth arrest both at G 1 and G 2 phases of the cell cycle and programmed cell death (apoptosis), respectively (7). Another transcriptional target of p53 is MDM2 itself, providing an autoregulatory negative feedback loop with a significant role in regulating cell cycle progression and apoptosis (7,8).The importance of the MDM2/p53 interaction has been convincingly demonstrated by in vivo studies. Mice lacking mdm2 are embryonic lethal and die before implantation as early as the blastocyst stage (9). This phenotype is completely rescued by concomitant deletion of p53 (10, 11), suggesting that the embryo lethality was ...

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Philip Nickson

Endoplasmic Reticulum Stress as a Novel Therapeutic Target in Heart Diseases

Targeted deletion of Puma attenuates cardiomyocyte death and improves cardiac function during ischemia-reperfusion

PUMA is critical for neonatal cardiomyocyte apoptosis induced by endoplasmic reticulum stress

Differential Regulation of Cardiomyocyte Survival and Hypertrophy by MDM2, an E3 Ubiquitin Ligase

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