The Commonly Used cGMP-dependent Protein Kinase Type I (cGKI) Inhibitor Rp-8-Br-PET-cGMPS Can Activate cGKI in Vitro and in Intact Cells

Valtcheva, Nadejda; Nestorov, Peter; Beck, Alexander; Russwurm, Michael; Hillenbrand, Matthias; Weinmeister, Pascal; Feil, Robert

doi:10.1074/jbc.m806161200

Cited by 37 publications

(37 citation statements)

References 41 publications

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“…This suggests that PKG signaling in the amygdala is required for LTM formation. Consistent results have been obtained with pharmacological inhibition in the amygdala, although there is concern about the specificity of PKG blockers (Valtcheva et al 2009). Post-training injection of the most specific PKG inhibitor into the lateral amygdala impairs cued fear LTM (Ota et al 2008).…”

Section: Pkgsupporting

confidence: 57%

The roles of protein kinases in learning and memory

2013

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In the adult mammalian brain, more than 250 protein kinases are expressed, but only a few of these kinases are currently known to enable learning and memory. Based on this information it appears that learning and memory-related kinases either impact on synaptic transmission by altering ion channel properties or ion channel density, or regulate gene expression and protein synthesis causing structural changes at existing synapses as well as synaptogenesis. Here, we review the roles of these kinases in short-term memory formation, memory consolidation, memory storage, retrieval, reconsolidation, and extinction. Specifically, we discuss the roles of calcium/calmodulin-dependent kinase II (CaMKII

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Section: Pkgsupporting

confidence: 57%

The roles of protein kinases in learning and memory

2013

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“…Antibodies used were rabbit anti-cGKI common (DH) (1∶5000), a pan-specific (nonphospho-specific) antiserum detecting both cGKIα and cGKIβ [26], rabbit anti-VASP (1∶1000, Cell Signaling, 9A2, 3132), rabbit anti-GAPDH (1∶5000, Cell Signaling, 14C10, 2118), and rabbit anti-Akt (1∶1000; Cell Signaling, 9272). The polyclonal rabbit antisera against phospho-cGKI species that were generated and characterized in this study were AffPS3 (1∶100), PS6 (1∶2000), and PS7 (1∶2000).…”

Section: Methodsmentioning

confidence: 99%

Catalytic Activity of cGMP-Dependent Protein Kinase Type I in Intact Cells Is Independent of N-Terminal Autophosphorylation

2014

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Although cGMP-dependent protein kinase type I (cGKI) is an important mediator of cGMP signaling and upcoming drug target, its in vivo-biochemistry is not well understood. Many studies showed that purified cGKI autophosphorylates multiple sites at its N-terminus. Autophosphorylation might be involved in kinase activation, but it is unclear whether this happens also in intact cells. To study cGKI autophosphorylation in vitro and in vivo, we have generated phospho-specific antisera against major in vitro-autophosphorylation sites of the cGKI isoforms, cGKIα and cGKIβ. These antisera detected specifically and with high sensitivity phospho-cGKIα (Thr58), phospho-cGKIα (Thr84), or phospho-cGKIβ (Thr56/Ser63/Ser79). Using these antisera, we show that ATP-induced autophosphorylation of cGKI in purified preparations and cell extracts did neither require nor induce an enzyme conformation capable of substrate heterophosphorylation; it was even inhibited by pre-incubation with cGMP. Interestingly, phospho-cGKI species were not detectable in intact murine cells and tissues, both under basal conditions and after induction of cGKI catalytic activity. We conclude that N-terminal phosphorylation, although readily induced in vitro, is not required for the catalytic activity of cGKIα and cGKIβ in vivo. These results will also inform screening strategies to identify novel cGKI modulators.

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“…Some cN analogs (e.g., 1,N 2 -phenyletheno-cGMP) are more potent PKGI activators than cGMP, and others, (e.g., 8-bromo-␤-phenyl-1,N 2 -ethenoguanosine-3Ј,5Ј-cyclic monophosphorothioate, Rp-isomer) bind to the allosteric site but only partially activate catalysis; the latter compound is commonly used as a PKGI inhibitor because it blocks access of the more effective activator, cGMP, to the binding sites (Sekhar et al, 1992;Butt et al, 1994b;Taylor et al, 2004;Poppe et al, 2008;Valtcheva et al, 2009). Cyclic nucleotide analogs have proved to be highly useful tools in investigating biological effects mediated by PKAs, EPACs, or PKGs; the analogs freely traverse the cell membrane to directly act on the target proteins, thereby circumventing involvement of proteins that generate the signaling molecule, factors involved in delivery of the signal to the target cell, specific membrane receptors, or the adenylyl or guanylyl cyclases that produce the cNs (Beebe et al, 1988a,b;Francis et al, 1988;Christensen et al, 2003;Dao et al, 2006;Poppe et al, 2008).…”

Section: B Cgmp-dependent Protein Kinase Imentioning

confidence: 99%