Your search keyword '"Kurose, Hitoshi"' showing total 8 results

1. Increased ubiquitination and the crosstalk of G protein signaling in cardiac myocytes: involvement of Ric-8 B in Gs suppression by Gq signal.

Author

Jenie, Riris I, Nishimura, Motoki, Fujino, Mika, Nakaya, Michio, Mizuno, Norikazu, Tago, Kenji, Kurose, Hitoshi, and Itoh, Hiroshi

Subjects

UBIQUITINATION, G proteins, CELLULAR signal transduction, HEART cells, GENE expression, UBIQUITIN

Abstract

Hyperactivation of Gq signaling causes cardiac hypertrophy, and β-adrenergic receptor-mediated Gs signaling is attenuated in hypertrophic cardiomyocytes. Here, we found the increase in a global ubiquitination in hypertrophic mouse heart. The activation of Gq signaling resulted in the ubiquitination of Gαs in neonatal rat cardiomyocytes, reduced Gαs expression, and suppressed cAMP response to β-adrenergic receptor stimulation. Ectopic expression of Gαq induced a similar suppression, which is due to the degradation of Gαs by a ubiquitin-proteasome pathway. Co-expression of Ric-8B, a positive regulator of Gαs, effectively canceled the Gαq-induced ubiquitination of Gαs and recovered the cAMP accumulation. In vitro, Gαq competes for the binding of Gαs to Ric-8B. These data show a new role of Ric-8B in the crosstalk of two distinct G protein signaling pathways, which are possibly involved in a part of mechanisms of chronic heart failure. [ABSTRACT FROM AUTHOR]

Published

2013

2. Heterologous down-regulation of angiotensin type 1 receptors by purinergic P2Y2 receptor stimulation through S-nitrosylation of NF-KB.

Author

Nishida, Motohiro, Ogushi, Mariko, Suda, Reiko, Toyotaka, Miyuki, Saikia, Shota, Kitajima, Naoyuki, Nakaya, Michio, Kim, Kyeong-Man, Ide, Tomomi, Sato, Yoji, Inoue, Kazuhide, and Kurose, Hitoshi

Subjects

ANGIOTENSIN I, PHYSIOLOGICAL effects of nitric oxide, ADENOSINE triphosphate, FIBROBLASTS, LABORATORY rats, CYTOSOL, HEART cells, PHYSIOLOGY

Abstract

Cross-talk between G protein-coupled receptor (GPCR) signaling pathways serves to fine tune cellular responsiveness by neurohumoral factors. Accumulating evidence has implicated nitric oxide (NO)-based signaling downstream of GPCRs, but the molecular details are unknown. Here, we show that adenosine triphosphate (ATP) decreases angiotensin type 1 receptor (AT1R) density through NO-mediated S-nitrosylation of nuclear factor KB (NF-κB) in rat cardiac fibroblasts. Stimulation of purinergic P2Y2 receptor by ATP increased expression of inducible NO synthase (iNOS) through activation of nuclear factor of activated T cells, NFATc1 and NFATc3. The ATP-induced iNOS interacted with p65 subunit of NF-κB in the cytosol through flavin-binding domain, which was indispensable for the locally generated NO-mediated S-nitrosylation of p65 at Cys38. β-Arrestins anchored the formation of p65/ lκBα/β-arrestins/iNOS quaternary complex. The S-nitrosylated p65 resulted in decreases in NF-κB transcriptional activity and ATκR density. In pressure-overloaded mouse hearts, ATP released from cardiomyocytes led to decrease in AT1R density through iNOS-mediated S-nitrosylation of p65. These results show a unique regulatory mechanism of heterologous regulation of GPCRs in which cysteine modification of transcriptional factor rather than protein phosphorylation plays essential roles. [ABSTRACT FROM AUTHOR]

Published

2011

3. The prokineticin receptor-1 (GPR73) promotes cardiomyocyte survival and angiogenesis.

Author

Urayama, Kyoji, Guilini, Célia, Messaddeq, Nadia, Kai Hu, Steenman, Marja, Kurose, Hitoshi, Ert, Georg, and Nebigil, Canan G.

Subjects

VASCULAR endothelial growth factors, HEART cells, MYOCARDIAL infarction treatment, OXIDATIVE stress, GENETIC transformation, NEOVASCULARIZATION

Abstract

Prokineticins are potent angiogenic factors that bind to two G protein-coupled receptors to initiate their biological effects. We hypothesize that prokineticin receptor-1 (PKR1/GPR73) signaling may contribute to cardiomyocyte survival or repair in myocardial infarction. Since we showed that prokineticin-2 and PKR1 are expressed in adult mouse heart and cardiac cells, we investigated the role of prokineticin-2 on capillary endothelial cell and cardiomyocyte function. In cultured cardiac endothelial cells, prokineticin-2 or overexpression of PKR1 induces vessel-like formation without increasing VEGF levels. In cardiomyocytes and H9c2 cells, prokineticin-2 or overexpressing PKR1 activates Akt to protect cardiomyocytes against oxidative stress. The survival and angiogenesis promoting effects of prokineticin-2 in cardiac cells were completely reversed by siRNA-PKR1, indicating PKR1 involvement. We thus, further investigated whether intramyocardial gene transfer of DNA encoding PKR1 may rescue the myocardium against myocardial infarction in mouse model. Transient PKR1 gene transfer after coronary ligation reduces mortality and preserves left ventricular function by promoting neovascularization and protecting cardiomyocytes without altering VEGF levels. In human end-stage failing heart samples, reduced PKR1 and prokineticin-2 transcripts and protein levels implicate a more important role for prokineticin-2/PKR1 signaling in heart. Our results suggest that PKR1 may represent a novel therapeutic target to limit myocardial injury following ischemic events. [ABSTRACT FROM AUTHOR]

Published

2007

4. TRPC3 and TRPC6 are essential for angiotensin II-induced cardiac hypertrophy.

Author

Onohara, Naoya, Nishida, Motohiro, Inoue, Ryuji, Kobayashi, Hiroyuki, Sumimoto, Hideki, Sato, Yoji, Mori, Yasuo, Nagao, Taku, and Kurose, Hitoshi

Subjects

ANGIOTENSINS, HEART failure, CARDIAC hypertrophy, HEART cells, T cells, PHOSPHOLIPASES

Abstract

Angiotensin (Ang) II participates in the pathogenesis of heart failure through induction of cardiac hypertrophy. Ang II-induced hypertrophic growth of cardiomyocytes is mediated by nuclear factor of activated T cells (NFAT), a Ca2+-responsive transcriptional factor. It is believed that phospholipase C (PLC)-mediated production of inositol-1,4,5-trisphosphate (IP3) is responsible for Ca2+ increase that is necessary for NFAT activation. However, we demonstrate that PLC-mediated production of diacylglycerol (DAG) but not IP3 is essential for Ang II-induced NFAT activation in rat cardiac myocytes. NFAT activation and hypertrophic responses by Ang II stimulation required the enhanced frequency of Ca2+ oscillation triggered by membrane depolarization through activation of DAG-sensitive TRPC channels, which leads to activation of L-type Ca2+ channel. Patch clamp recordings from single myocytes revealed that Ang II activated DAG-sensitive TRPC-like currents. Among DAG-activating TRPC channels (TRPC3, TRPC6, and TRPC7), the activities of TRPC3 and TRPC6 channels correlated with Ang II-induced NFAT activation and hypertrophic responses. These data suggest that DAG-induced Ca2+ signaling pathway through TRPC3 and TRPC6 is essential for Ang II-induced NFAT activation and cardiac hypertrophy. [ABSTRACT FROM AUTHOR]

Published

2006

5. G alpha [sub]i and G alpha [sub]0 are target proteins of reactive oxygen species.

Author

Nishida, Motohiro, Maruyama, Yoshiko, Tanaka, Rie, Kotani, Kenji, Nagao, Taku, and Kurose, Hitoshi

Subjects

BETA adrenoceptors, GAMMA functions, HYDROGEN peroxide, HEART cells

Abstract

Presents a report on the inhibition of the Betagamma-subunit of G protein (GBetagamma) and how it attenuates hydrogen peroxide H[sub2]O[sub2]-induced ERK activation in rat neonatal cardiomyocytes. Identification of reactive oxygen species as central mediators in certain signalling events; Analysis using heterotrimeric G[sub0} and its individual subunits; Conclusion that Galpha[sub1] and Galpha[sub0] are targets of oxidative stress for activation of ERK.

Published

2000

6. TRPC3-mediated Ca2+ influx contributes to Rac1-mediated production of reactive oxygen species in MLP-deficient mouse hearts

Author

Kitajima, Naoyuki, Watanabe, Kunihiro, Morimoto, Sachio, Sato, Yoji, Kiyonaka, Shigeki, Hoshijima, Masahiko, Ikeda, Yasuhiro, Nakaya, Michio, Ide, Tomomi, Mori, Yasuo, Kurose, Hitoshi, and Nishida, Motohiro

Subjects

*TRP channels, *PHYSIOLOGICAL effects of calcium, *ACTIVE oxygen in the body, *CARDIOMYOPATHIES, *OXIDATIVE stress, *ANGIOTENSINS, *HEART cells, *CALMODULIN

Abstract

Abstract: Dilated cardiomyopathy (DCM) is a myocardial disorder that is characterized by dilation and dysfunction of the left ventricle (LV). Accumulating evidence has implicated aberrant Ca2+ signaling and oxidative stress in the progression of DCM, but the molecular details are unknown. In the present study, we report that inhibition of the transient receptor potential canonical 3 (TRPC3) channels partially prevents LV dilation and dysfunction in muscle LIM protein-deficient (MLP (−/−)) mice, a murine model of DCM. The expression level of TRPC3 and the activity of Ca2+/calmodulin-dependent kinase II (CaMKII) were increased in MLP (−/−) mouse hearts. Acitivity of Rac1, a small GTP-binding protein that participates in NADPH oxidase (Nox) activation, and the production of reactive oxygen species (ROS) were also increased in MLP (−/−) mouse hearts. Treatment with pyrazole-3, a TRPC3 selective inhibitor, strongly suppressed the increased activities of CaMKII and Rac1, as well as ROS production. In contrast, activation of TRPC3 by 1-oleoyl-2-acetyl-sn-glycerol (OAG), or by mechanical stretch, induced ROS production in rat neonatal cardiomyocytes. These results suggest that up-regulation of TRPC3 is responsible for the increase in CaMKII activity and the Nox-mediated ROS production in MLP (−/−) mouse cardiomyocytes, and that inhibition of TRPC3 is an effective therapeutic strategy to prevent the progression of DCM. [Copyright &y& Elsevier]

Published

2011

7. Phosphorylation of TRPC6 Channels at Thr69 Is Required for Anti-hypertrophic Effects of Phosphodiesterase 5 Inhibition.

Author

Nishida, Motohiro, Watanabe, Kenta, Sato, Yoji, Nakaya, Michio, Kitajima, Naoyuki, Ide, Tomomi, Inoue, Ryuji, and Kurose, Hitoshi

Subjects

*PHOSPHORYLATION, *CARDIAC hypertrophy, *MEMBRANE proteins, *CYCLIC nucleotide phosphodiesterase inhibitors, *SILDENAFIL, *HEART cells, *PROTEIN kinases

Abstract

Activation of Ca2+ signaling induced by receptor stimulation and mechanical stress plays a critical role in the development of cardiac hypertrophy. A canonical transient receptor potential protein subfamily member, TRPC6, which is activated by diacylglycerol and mechanical stretch, works as an upstream regulator of the Ca2+ signaling pathway. Although activation of protein kinase G (PKG) inhibits TRPC6 channel activity and cardiac hypertrophy, respectively, it is unclear whether PKG suppresses cardiac hypertrophy through inhibition of TRPC6. Here, we show that inhibition of cGMP-selective PDE5 (phosphodiesterase 5) suppresses endothelin-1-, diacylglycerol analog-, and mechanical stretch-induced hypertrophy through inhibition of Ca2+ influx in rat neonatal cardiomyocytes. Inhibition of PDE5 suppressed the increase in frequency of Ca2+ spikes induced by agonists or mechanical stretch. However, PDE5 inhibition did not suppress the hypertrophic responses induced by high KCI or the activation of protein kinase C, suggesting that PDE5 inhibition suppresses Ca2+ influx itself or molecule(s) upstream of Ca2+ influx. PKG activated by PDE5 inhibition phosphorylated TRPC6 proteins at Thr69 and prevented TRPC6-mediated Ca2+ influx. Substitution of Ala for Thr69 in TRPC6 abolished the anti-hypertrophic effects of PDE5 inhibition. In addition, chronic PDE5 inhibition by oral sildenafil treatment actually induced TRPC6 phosphorylation in mouse hearts. Knockdown of RGS2 (regulator of G protein signaling 2) and RGS4, both of which are activated by PKG to reduce Gαq-mediated signaling, did not affect the suppression of receptor-activated Ca2+ influx by PDE5 inhibition. These results suggest that phosphorylation and functional suppression of TRPC6 underlie prevention of pathological hypertrophy by PDE5 inhibition. [ABSTRACT FROM AUTHOR]

Published

2010

8. Gα12/13- and Reactive Oxygen Species-dependent Activation of c-Jun NH2-terminal Kinase and p38 Mitogen-activated Protein Kinase by Angiotensin Receptor Stimulation in Rat Neonatal Cardiomyocytes.

Author

Nishida, Motohiro, Tanabe, Shihori, Maruyama, Yoshiko, Mangmool, Supachoke, Urayama, Kyoji, Nagamatsu, Yuichi, Takagahara, Shuichi, Turner, Justin H., Kozasa, Tohru, Kobayashi, Hiroyuki, Sato, Yoji, Kawanishi, Toru, Inoue, Ryuji, Nagao, Taku, and Kurose, Hitoshi

Subjects

*REACTIVE oxygen species, *PROTEIN kinases, *ANGIOTENSINS, *HEART cells, *MITOGENS, *IONIZATION of gases

Abstract

In the present study, we examined signal transduction mechanism of reactive oxygen species (ROS) production and the role of ROS in angiotensin II-induced activation of mitogen-activated protein kinases (MAPKs) in rat neonatal cardiomyocytes. Among three MAPKs, c-Jun NH2-terminal kinase (JNK) and p38 MAPK required ROS production for activation, as an NADPH oxidase inhibitor, diphenyleneiodonium, inhibited the activation. The angiotensin II-induced activation of JNK and p38 MAPK was also inhibited by the expression of the Gα2/13-specific regulator of G protein signaling (RGS) domain, a specific inhibitor of Gα12/13, but not by an RGS domain specific for Gαq. Constitutively active Gα12- or Gα13-induced activation of JNK and p38 MAPK, but not extracellular signal-regulated kinase (ERK), was inhibited by diphenyleneiodonium. Angiotensin II receptor stimulation rapidly activated Gα13, which was completely inhibited by the Gα12/13-specific RGS domain. Furthermore, the Gα12/13-specific but not the Gαq-Specific RGS domain inhibited angiotensin II-induced ROS production. Dominant negative Rac inhibited angiotensin II-stimulated ROS production, JNK activation, and p38 MAPK activation but did not affect ERK activation. Rac activation was mediated by Rho and Rho kinase, because Rac activation was inhibited by C3 toxin and a Rho kinase inhibitor, Y27632. Furthermore, angiotensin II-induced Rho activation was inhibited by Gα12/13-specific RGS domain but not dominant negative Rac. An inhibitor of epidermal growth factor receptor kinase AG1478 did not affect angiotensin II-induced JNK activation cascade. These results suggest that Gα12/13-mediated ROS production through Rho and Rac is essential for JNK and p38 MAPK activation. [ABSTRACT FROM AUTHOR]

Published

2005