Regulated Nucleocytoplasmic Transport of Protein Kinase D in Response to G Protein-coupled Receptor Activation

Rey, Osvaldo; Sinnett‐Smith, James; Zhukova, Elena; Rozengurt, Enrique

doi:10.1074/jbc.m109395200

Cited by 83 publications

(101 citation statements)

References 76 publications

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“…Furthermore, deletion of the C1a, the C1b, or the PH subdomain, respectively, leads to the constitutive activation of PKD1, suggesting that these subdomains have a negative/inhibitory impact on its catalytic activity . The PH domain also has been shown to mediate nuclear export, whereas the C1b domain regulates nuclear import of PKD1 (Rey et al, 2001). At present little is known about whether the various PKD isoforms are regulated and act in a similar manner or exhibit distinct regulatory and functional properties.…”

Section: Introductionmentioning

confidence: 99%

Role of the Regulatory Domain of Protein Kinase D2 in Phorbol Ester Binding, Catalytic Activity, and Nucleocytoplasmic Shuttling

Auer

Blume

Sturany

et al. 2005

MBoC

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Protein kinase D2 (PKD2) belongs to the PKD family of serine/threonine kinases that is activated by phorbol esters and G protein-coupled receptors (GPCRs). Its C-terminal regulatory domain comprises two cysteine-rich domains (C1a/C1b) followed by a pleckstrin homology (PH) domain. Here, we examined the role of the regulatory domain in PKD2 phorbol ester binding, catalytic activity, and subcellular localization: The PH domain is a negative regulator of kinase activity. C1a/C1b, in particular C1b, is required for phorbol ester binding and gastrin-stimulated PKD2 activation, but it has no inhibitory effect on the catalytic activity. Gastrin triggers nuclear accumulation of PKD2 in living AGS-B cancer cells. C1a/C1b, not the PH domain, plays a complex role in the regulation of nucleocytoplasmic shuttling: We identified a nuclear localization sequence in the linker region between C1a and C1b and a nuclear export signal in the C1a domain. In conclusion, our results define the critical components of the PKD2 regulatory domain controlling phorbol ester binding, catalytic activity, and nucleocytoplasmic shuttling and reveal marked differences to the regulatory properties of this domain in PKD1. These findings could explain functional differences between PKD isoforms and point to a functional role of PKD2 in the nucleus upon activation by GPCRs.

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Section: Introductionmentioning

confidence: 99%

Role of the Regulatory Domain of Protein Kinase D2 in Phorbol Ester Binding, Catalytic Activity, and Nucleocytoplasmic Shuttling

Auer

Blume

Sturany

et al. 2005

MBoC

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Section: The Pkd Family Belongs To the Camk Groupmentioning

confidence: 99%

“…For example, G-proteincoupled receptors or receptor tyrosine kinases that activate PLC and PKCε or PKCη cause the phosphorylation of PKD at Ser744 and Ser748 in the activation loop [16][17][18][19] . Second, Gβγ subunits directly activate PKD1 [20][21][22] . The precise mechanism of this activation in vivo needs to be defi ned.…”

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confidence: 99%

“…As no interactions have been found between the PH domain of PKD1 and phosphorylated inositol lipids, which are important ligands responsible for membrane localization, this domain is not required for plasma membrane translocation [31,32] or Golgi localization [33][34][35][36][37][38][39] like other PH-domain-containing AGC kinases, such as PKB and the GRKs. However, the PH domain is required for the nuclear export of PKD1 [22,40] .The different lipid-binding specificity of the zinc-fingers C1A and C1B results in their different roles in targeting PKD1 to different destinations [29,33,[41][42][43] . Plasma membrane translocation of PKD1 is dependent on the C1B domain, while its Golgi localization requires the C1A domain and the phosphorylation of loop serines.…”

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confidence: 99%

“…Plasma membrane translocation of PKD1 is dependent on the C1B domain, while its Golgi localization requires the C1A domain and the phosphorylation of loop serines. After activation by G-protein-coupled receptors, PKD1 can shuttle between nucleus and cytosol, requiring the C1B domain for import and the PH domain for export from the nucleus [22] . …”

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confidence: 99%

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Protein kinase D: a new player among the signaling proteins that regulate functions in the nervous system

Wang

2014

Neurosci. Bull.

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Protein kinase D (PKD) is an evolutionarily-conserved family of protein kinases. It has structural, regulatory, and enzymatic properties quite different from the PKC family. Many stimuli induce PKD signaling, including G-protein-coupled receptor agonists and growth factors. PKD1 is the most studied member of the family. It functions during cell proliferation, differentiation, secretion, cardiac hypertrophy, immune regulation, angiogenesis, and cancer. Previously, we found that PKD1 is also critically involved in pain modulation. Since then, a series of studies performed in our lab and by other groups have shown that PKDs also participate in other processes in the nervous system including neuronal polarity establishment, neuroprotection, and learning. Here, we discuss the connections between PKD structure, enzyme function, and localization, and summarize the recent fi ndings on the roles of PKD-mediated signaling in the nervous system. Keywords: PKD; neuronal polarity; pain modulation; neuroprotection; learning IntroductionMembers of the protein kinase D (PKD) family are diacylglycerol (DAG) and protein kinase C (PKC) effectors.They are activated by the actions of hormones, growth factors, neurotransmitters, and other stimuli through phospholipase C (PLC) [1] . Three widely-expressed mammalian homologs are PKD1 (mouse PKD, human PKCμ) [2,3] , PKD2 [3] , and PKD3 [4] (also named PKC), but the levels of individual PKDs vary in different tissues.Recent fi ndings have revealed that PKDs participate in the regulation of Golgi function through modulating the fi ssion of vesicles from the trans-Golgi network (TGN) [5,6] . Other recent reports have shown that PKDs function during cell proliferation and apoptosis, carcinogenesis, and intracellular trafficking. Here, we describe the connections between PKD structure, enzymatic function, and localization, and then summarize recent fi ndings on the roles of PKD in the nervous system. The PKD Family Belongs to the CaMK GroupThe PKD family comprises PKD1, PKD2, and PKD3. PKD was initially described as an atypical isoform of the PKC family [7] , which is a member of the protein kinase A, G, and C (AGC) serine/threonine kinase subfamily [8,9] . However, later studies revealed that PKD has mixed features of different subclasses of the PKC family, so it does not belong to any one of them. For example, its pleckstrin-homology (PH) domain is closely related to the PKB and G-proteincoupled receptor kinase (GRK) families and is not found in any PKC enzyme, while the cysteine-rich domains are more reminiscent of classical and novel PKCs. The structure and function of the catalytic domain of PKD are quite different from those of the AGC/PKC family members [2][3][4]10] . Indeed, PKD has now been classified as a new family within the (Fig. 1). The elaborate constitution of PKD1 is intricately linked to its catalytic functions, regulation, and intracellular localization (Table 1). PKD1 can be activated through different pathways.First, some stimuli activate PLC, which induces PKD phosp...

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Protein kinase D isoforms are expressed in rat and mouse primary sensory neurons and are activated by agonists of protease‐activated receptor 2

Amadesi

Grant

Cottrell

et al. 2009

J of Comparative Neurology

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Serine proteases generated during injury and inflammation cleave protease-activated receptor 2 (PAR 2 ) on primary sensory neurons to induce neurogenic inflammation and hyperalgesia. Hyperalgesia requires sensitization of transient receptor potential vanilloid (TRPV) ion channels by mechanisms involving phospholipase C and protein kinase C (PKC). The protein kinase D (PKD) serine/threonine kinases are activated by diacylglycerol and PKCs, and can phosphorylate TRPV1. Thus, PKDs may participate in novel signal transduction pathways triggered by serine proteases during inflammation and pain. However, it is not known whether PAR 2 activates PKD, and the expression of PKD isoforms by nociceptive neurons is poorly characterized. Using HEK293 cells transfected with PKDs, we found that PAR 2 stimulation promoted plasma membrane translocation and phosphorylation of PKD1, PKD2 and PKD3, indicating activation. This effect was partially dependent on PKCε. Using immunofluorescence and confocal microscopy, with antibodies against PKD1/PKD2, PKD3 and neuronal markers, we found that PKDs were expressed in rat and mouse dorsal root ganglia (DRG) neurons, including nociceptive neurons that expressed TRPV1, PAR 2 and neuropeptides. PAR 2 agonist induced phosphorylation of PKD in cultured DRG neurons, indicating PKD activation. Intraplantar injection of PAR 2 agonist also caused phosphorylation of PKD in neurons of lumbar DRG, confirming activation in vivo. Thus, PKD1, PKD2 and PKD3 are expressed in primary sensory neurons that mediate neurogenic inflammation and pain transmission, and PAR 2 agonists activate PKDs in HEK293 cells and DRG neurons in culture and in intact animals. PKD may be a novel component of a signal transduction pathway for protease-induced activation of nociceptive neurons and an important new target for anti-inflammatory and analgesic therapies.

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Regulated Nucleocytoplasmic Transport of Protein Kinase D in Response to G Protein-coupled Receptor Activation

Cited by 83 publications

References 76 publications

Role of the Regulatory Domain of Protein Kinase D2 in Phorbol Ester Binding, Catalytic Activity, and Nucleocytoplasmic Shuttling

Role of the Regulatory Domain of Protein Kinase D2 in Phorbol Ester Binding, Catalytic Activity, and Nucleocytoplasmic Shuttling

Protein kinase D: a new player among the signaling proteins that regulate functions in the nervous system

Protein kinase D isoforms are expressed in rat and mouse primary sensory neurons and are activated by agonists of protease‐activated receptor 2

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