Depolarization‐induced differentiation of PC12 cells is mediated by phospholipase D2 through the transcription factor CREB pathway

Banno, Yoshiko; Nemoto, Satoshi; Murakami, Masashi; Kimura, Masashi; Ueno, Yoshihito; Ohguchi, Ken-ichi; Hara, Akira; Okano, Yukio; Kitade, Yukio; Onozuka, Minoru; Murate, Takashi; Nozawa, Yoshinori

doi:10.1111/j.1471-4159.2007.05085.x

Cited by 30 publications

(22 citation statements)

References 61 publications

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“…Important functions of CaMKII include the control of neurotransmitter release and the mediation of stimulus-induced gene expression (Moreno-Delgado et al 2009;Shen et al 2010). CaMKIIδ, by the very nature of its core function as a kinase, is a multifunctional signaling protein that regulates numerous physiological processes including cellular differentiation (Donai et al 2000;Ju et al 2004;Banno et al 2008;Han et al 2011;Mouton-Liger et al 2011), ion channel function (Wagner et al 2011), arrhythmogenesis during atrial fibrillation (Tobimatsu and Fujisawa 1989;Qin et al 2011), modulating inflammatory and proliferative responses (Currie et al 2011), vascular smooth muscle proliferation (House et al 2007;House and Singer 2008;Li et al 2011), heart failure (Zhang et al 2004;Maier 2005;Rokita et al 2011), and pathological processes such as apoptosis induced by ischemia/reperfusion injury in cardiomyoctyes (Ma et al 2009;Wang et al 2010). Knowledge of the participation of CaMKIIδ in cell physiology and apoptotic pathways in central nervous system is limited.…”

Section: Introductionmentioning

confidence: 99%

Increased Expression of Calcium/Calmodulin-Dependent Protein Kinase Type II Subunit Delta after Rat Traumatic Brain Injury

Zhang

Shan

et al. 2011

J Mol Neurosci

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Many cellular responses to Ca(2+) signals are mediated by Ca(2+)/calmodulin-dependent enzymes, among which is the Ca(2+)/calmodulin-dependent protein kinase II (CaMKII). CaMKII was originally described in rat brain tissue. In rat brain, four different subunits of the kinase have been identified: α, β, γ, and δ. This study aims to investigate changes of CaMKIIδ after traumatic brain injury and its possible role. Rat traumatic brain injury (TBI) model was established by controlled cortical injury system. In the present study, we mainly investigated the expression and cellular localization of CaMKIIδ after traumatic brain injury. Western blot analysis revealed that CaMKIIδ was present in normal rat brain cortex. It gradually increased, reached a peak at the third day after TBI, and then decreased. Importantly, more CaMKIIδ was colocalized with neuron. In addition, Western blot detection showed that the third day postinjury was also the apoptosis peak indicated by the elevated expression of caspase-3.Importantly, immunohistochemistry analysis revealed that injury-induced expression of CaMKIIδ was colabeled by caspase-3 (apoptosis cells marker). Moreover, pretreatment with the CaMKII inhibitor (KN62) reduced the injury-induced activation of caspase-3. Noticeably, the CaMKII inhibitor KN-62 could reduce TBI-induced cell injury assessed with lesion volume and attenuate behavioral outcome evaluated by motor test. These data suggested that CaMKIIδ may be implicated in the apoptosis of neuron and the recovery of neurological outcomes. However, the inherent mechanisms remained unknown. Further studies are needed to confirm the exact role of CaMKIIδ after brain injury.

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Section: Introductionmentioning

confidence: 99%

Increased Expression of Calcium/Calmodulin-Dependent Protein Kinase Type II Subunit Delta after Rat Traumatic Brain Injury

Zhang

Shan

et al. 2011

J Mol Neurosci

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“…In contrast, PLD2 has a constitutively high activity in the presence of PI4,5P 2 and is insensitive to PLD1 activators (28,32). PLD2 has been implicated in various cellular events, such as antiapoptosis (38), endocytic recycling (39), endocytosis (40), differentiation of PC12 cells (41), actin-based membrane dynamics (42), and L1-dependent neurite outgrowth (43). Conclusions about some of these PLD functions are based on observations from experiments using primary alcohols, such as ethanol (EtOH) and 1-butanol.…”

mentioning

confidence: 99%

Molecular Mechanisms of N-Formyl-Methionyl-Leucyl-Phenylalanine-Induced Superoxide Generation and Degranulation in Mouse Neutrophils: Phospholipase D Is Dispensable

Sato

Hongu

Sakamoto

et al. 2013

Molecular and Cellular Biology

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Phospholipase D (PLD), which produces the lipid messenger phosphatidic acid (PA), has been implicated in superoxide generation and degranulation in neutrophils. The basis for this conclusion is the observation that primary alcohols, which interfere with PLD-catalyzed PA production, inhibit these neutrophil functions. However, off-target effects of primary alcohols cannot be totally excluded. Here, we generated PLD ؊/؊ mice in order to reevaluate the involvement of PLD in and investigate the molecular mechanisms of these neutrophil functions. Surprisingly, N-formyl-methionyl-leucyl-phenylalanine (fMLP) induced these functions in PLD ؊/؊ neutrophils, and these functions were suppressed by ethanol. These results indicate that PLD is dispensable for these neutrophil functions and that ethanol nonspecifically inhibits them, warning against the use of primary alcohols as specific inhibitors of PLD-mediated PA formation. The calcium ionophore ionomycin and the membrane-permeative compound 1-oleoyl-2-acetyl-sn-glycerol (OADG) synergistically induced superoxide generation. On the other hand, ionomycin alone induced degranulation, which was further augmented by OADG. These results demonstrate that conventional protein kinase C (cPKC) is crucial for superoxide generation, and a Ca 2؉ -dependent signaling pathway(s) and cPKC are involved in degranulation in mouse neutrophils.

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“…Another study demon-strated that depolarizationinduced calcium entry promotes NE differentiation of PC12 cells. This NE differentiation characterized by neurite formation, GAP-43 and synapsin I overexpression, requires the activation of phospholipase D2 -ErK-CREB pathway and Src phosphorylation by CaMKinase II [99]. Such a pathway is similar to the one demonstrated in hippocampal neurons, where NCAM (neural cell adhesion molecules) induced neurite formation is dependent on the T-type calcium channel [100].…”

Section: Putative Signalling Mechanisms Involved In T-type Calcium Chmentioning

confidence: 65%

Expression and Role of T-type Calcium Channels during Neuroendocrine Differentiation

Warnier¹,

Gackière²,

Roudbaraki³

et al. 2017

J Cell Signal

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Neuroendocrine cells release their secretion into the extracellular environment through calcium-dependent signalling pathways. These cells share common morphological and molecular features such as the expression of specific biomarkers, neurite outgrowth and dense core secretory granules. In order to elucidate the signalling pathways leading from undifferentiated to differentiated neuroendocrine cells, the role of voltage-dependent calcium channels, central actors in the excitation-secretion coupling, has been comprehensively investigated. T-type calcium channels appear to belong to the most important ion channel family involved in the neuroendocrine differentiation process. They could also participate in the development of neuroendocrine tumours.

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Depolarization‐induced differentiation of PC12 cells is mediated by phospholipase D2 through the transcription factor CREB pathway

Cited by 30 publications

References 61 publications

Increased Expression of Calcium/Calmodulin-Dependent Protein Kinase Type II Subunit Delta after Rat Traumatic Brain Injury

Increased Expression of Calcium/Calmodulin-Dependent Protein Kinase Type II Subunit Delta after Rat Traumatic Brain Injury

Molecular Mechanisms of N-Formyl-Methionyl-Leucyl-Phenylalanine-Induced Superoxide Generation and Degranulation in Mouse Neutrophils: Phospholipase D Is Dispensable

Expression and Role of T-type Calcium Channels during Neuroendocrine Differentiation

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