Inhibition of cyclic GMP‐dependent protein kinase‐mediated effects by (Rp)‐8‐bromo‐PET‐cyclic GMPS

Butt, Elke; Pöhler, D; Genieser, Hans‐Gottfried; Huggins, John P.; Bucher, Bernard

doi:10.1111/j.1476-5381.1995.tb15112.x

Cited by 103 publications

(92 citation statements)

References 28 publications

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“…8). These results are consistent with a previous study showing that Rp-PET can inhibit cGMPactivated cGKI in intact cells under certain conditions (24). Considering the 46-fold higher lipophilicity (14) and the 4-fold higher concentration of Rp-PET versus 8-Br-cGMP used in our experiment, it appears that the inhibitory potential of Rp-PET in intact cells is quite moderate and that it must be present in large excess to inhibit the effect of a strong agonist such as 8-Br-cGMP.…”

Section: Resultssupporting

confidence: 83%

“…3B, lower panel), respectively. These K i values were similar to K i values reported previously for the inhibition of the cGKI isozymes by Rp-PET in vitro (24). Interestingly, inhibition of cGMP-activated cGKI␣ by Rp-PET was less complete than inhibition of cGKI␤ (Fig.…”

Section: Resultssupporting

confidence: 75%

“…For instance, the cGMP analogue 8-Br-PET-cGMP (PET) is a cGKI agonist (23), whereas Rp-8-Br-PET-cGMPS (Rp-PET) (see Fig. 1B) competitively inhibits activation of purified cGKI by cGMP (24). Rp-PET is currently considered one of the most permeable, selective, and potent cGKI inhibitors available for intact cell studies (14,19).…”

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confidence: 99%

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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

Nestorov

Beck

et al. 2009

Journal of Biological Chemistry

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cGMP is a cyclic-nucleotide second messenger with multiple targets and functions. Small-molecule modulators of cGMP generators and effectors are important biochemical tools as well as established and prospective drugs for the treatment of human diseases, such as erectile dysfunction, pulmonary hypertension, and various cardiovascular disorders (1-3). cGMP is generated by nitric oxide-or natriuretic peptide-stimulated guanylyl cyclases and can bind to and modulate the activity of at least three classes of cGMP effector proteins: cyclic nucleotide-hydrolyzing phosphodiesterases (PDEs), 2 cyclic nucleotide-gated cation channels, and cGMP-dependent protein kinases (cGKs, also known as protein kinase G or PKG) (4).Based on pharmacological and genetic studies, the cGK type I (cGKI) is considered the major mediator of cGMP signaling in many tissues including the cardiovascular system (5-8). The mammalian cGKI is a cytosolic Ser/Thr protein kinase comprising an N-terminal regulatory domain with two cGMPbinding sites and a C-terminal catalytic domain. It exists in two isoforms termed cGKI␣ and cGKI␤. The isozymes have identical cGMP-binding sites and catalytic domains but differ in their N-terminal ϳ100 amino acids, which contribute to homodimerization, sensitivity to cGMP activation, and interaction with anchoring and substrate proteins. Recent in vivo studies with transgenic mice demonstrated that both isoforms can induce smooth muscle relaxation and vasodilation (9), but the respective molecular mechanisms behind these effects are controversial (6, 10). Similarly, opposing effects of cGMP/cGKI signaling have been reported on the growth and phenotype of vascular smooth muscle cells (VSMCs) (11,12). The inconsistency of the results concerning the function of cGKI might in part be related to unexpected effects of the pharmacological cGKI activators and inhibitors that are commonly used to distinguish between cGKI-dependent and cGKI-independent signaling. For instance, cGMP analogues can bind to multiple * This work was supported by grants from the Deutsche Forschungsgemeinschaft. The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. Section 1734 solely to indicate this fact. 2 The abbreviations used are: PDE, phosphodiesterase; cGKI, cGMP-dependent protein kinase type I; PET, 8-Br-PET-cGMP; Rp-PET, Rp-8-Br-PETcGMPS; 8-Br-PET-cGMP, ␤-phenyl-1,N 2 -etheno-8-bromoguanosine-3Ј,5Ј-cyclic monophosphate; Rp-8-pCPT-cGMPS, 8-(4-chlorophenylthio)-guanosine-3Ј, 5Ј-cyclic monophosphorothioate, Rp-isomer; Rp-8-Br-PET-cGMPS, ␤-phenyl-1,N 2 -etheno-8-bromoguanosine-3Ј,5Ј-cyclic monophosphorothioate, Rp-isomer; VASP, vasodilator-stimulated phosphoprotein; VSMC, vascular smooth muscle cell; MTS, 3-(4,5-dimethylthiazol-2-yl)-5-(3-carboxymethoxyphenyl)-2-(4-sulfophenyl)-2H-tetrazolium, inner salt; CFP, cyan fluorescent protein; YFP, yellow fluorescent protein; ESI-MS, electrospray ionization-mass spectrometry; ...

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Section: Resultssupporting

confidence: 83%

Section: Resultssupporting

confidence: 75%

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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

Nestorov

Beck

et al. 2009

Journal of Biological Chemistry

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“…Finally our observation that R p -cGMPS analogs, with some degree of specificity, can inhibit cGK II-controlled functions in intact tissues, as well as cGK I action described earlier (36,37), indicates that these compounds are more generally applicable as tools to demonstrate the involvement of cGK I or II in specific physiological processes. For example, in a separate study of the mechanism of action of heat-stable enterotoxin (STa) in rat intestinal epithelium, R p -8-pCPT-cGMPS appeared also able to inhibit the STa-induced Cl Ϫ secretion (15).…”

Section: Discussionmentioning

confidence: 99%

Endogenous Type II cGMP-dependent Protein Kinase Exists as a Dimer in Membranes and Can Be Functionally Distinguished from the Type I Isoforms

Vaandrager¹,

Edixhoven²,

Bot³

et al. 1997

Journal of Biological Chemistry

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In mammalian tissues two types of cGMP-dependent protein kinase (cGK) have been identified. In contrast to the dimeric cGK I, cGK II purified from pig intestine was shown previously to behave as a monomer. However, recombinant rat cGK II was found to have hydrodynamic parameters indicative of a homodimer. Chemical cross-linking studies showed that pig cGK II in intestinal membranes has a dimeric structure as well. However, after purification, cGK II was found to be partly proteolyzed into C-terminal monomeric fragments. Phosphorylation studies in rat intestinal brush borders revealed that the potency of cGMP analogs to stimulate or inhibit native cGK II in vitro (i.e. 8-(4-chlorophenylthio)-cGMP > cGMP > ␤-phenyl-1,N 2 -etheno-8-bromocGMP > ␤-phenyl-1,N 2 -etheno-cGMP and R p -8-(4-chlorophenylthio)-cGMPs > R p -␤-phenyl-1,N 2 -etheno-8-bromocGMPs, respectively) correlated well with their potency to stimulate or inhibit cGK II-mediated Cl ؊ secretion across intestinal epithelium but differed strikingly from their potency to affect cGK I activity. These data show that the N terminus of cGK II is involved in dimerization and that endogenous cGK II displays a distinct activation/inhibition profile with respect to cGMP analogs, which permits a pharmacological dissection between cGK II-and cGK I-mediated physiological processes.

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“…This is consistent with the current study in that we effectively inhibited pulmonary vasodilatory responses to 8-BrcGMP in lungs from both control and CH rats with mechanistically distinct inhibitors of PKG-1. Rp-8-Br-PET-cGMPS is the most potent and selective PKG inhibitor amongst the (Rp)-phosphorothioate cGMP analogs and antagonizes signaling by binding to PKG 1␣ or -␤ and prohibiting the conformational change of the enzyme required for its activation (5). In contrast, KT-5823, one of several K-252b derivatives that mediate inhibition by competing with ATP, is highly selective for PKG.…”

Section: Discussionmentioning

confidence: 99%

Pulmonary PKG-1 is upregulated following chronic hypoxia

Jernigan

Walker

Resta

2003

American Journal of Physiology-Lung Cellular and Molecular Phys

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. Pulmonary PKG-1 is upregulated following chronic hypoxia. Am J Physiol Lung Cell Mol Physiol 285: L634-L642, 2003. First published May 23, 2003 10.1152/ ajplung.00328.2002.-Recent studies from our laboratory indicate that pulmonary vasodilatory responses to exogenous nitric oxide (NO) are attenuated following chronic hypoxia (CH) and that this NO-dependent vasodilation is mediated by cGMP. Similarly, we have demonstrated that CH attenuates vasodilatory responses to the cGMP analog 8-bromoguanosine 3',5'-cyclic monophosphate (8-BrcGMP). We hypothesized that attenuated pulmonary vasodilation to 8-BrcGMP following CH is mediated by decreased protein kinase G-1 (PKG-1) expression/activity. Therefore, we examined vasodilatory responses to 8-BrcGMP (1 M) in isolated, saline-perfused lungs from control and CH (4 wk at barometric pressure of 380 mmHg) rats in the presence of the competitive PKG inhibitor Rp-␤-phenyl-1, N2-etheno-8-bromoguanosine 3',5'-cyclic monophosphorothionate (30 M) or the highly specific PKG inhibitor KT-5823 (10 M). PKG-1 expression and activity were determined in whole lung homogenates from each group, and vascular PKG-1 levels were assessed by quantitative immunohistochemistry. PKG inhibition with either Rp-8-Br-PET-cGMPS or KT-5823 diminished vasodilatory responses to 8-BrcGMP in lungs from both control and CH rats, thus indicating a role for PKG in mediating reactivity to 8-BrcGMP in each group. However, in contrast to our hypothesis, PKG-1 levels were approximately twofold greater in lungs from CH rats vs. controls, and furthermore, this upregulation was localized to the vasculature. This correlates with an increase in PKG activity following CH. We conclude that PKG-1 is involved in 8-BrcGMPmediated vasodilation; however, attenuated pulmonary vasodilation following CH is not associated with decreased expression/activity of PKG-1. isolated rat lung; nitric oxide; pulmonary hypertension; 8-bromoguanosine 3',5'-cyclic monophosphate; KT-5823; Rp-␤-phenyl-1, N2-etheno-8-bromoguanosine 3',5'-cyclic monophosphorothioate CHRONIC EXPOSURE TO HYPOXIA has been shown to augment pulmonary vasodilatory responses to endothelium-derived nitric oxide (EDNO)-dependent vasodilators (18, 26, 28, 32-34, 36, 37). EDNO is synthesized in the vasculature by endothelial nitric oxide synthase (eNOS), and several studies have demonstrated that chronic hypoxia (CH) is associated with increased pulmonary eNOS levels, gene expression, and activity (18,21,26,33,34,39,46). Consistent with elevated eNOS levels, nitric oxide (NO) synthesis appears to be greater in lungs isolated from CH rats compared with controls (18,26,44). In contrast to enhanced reactivity to our laboratory (19,34) and others (35) have demonstrated impaired responsiveness to exogenous NO following CH. However, the mechanism(s) responsible for this diminished reactivity is not fully understood.NO leads to pulmonary vascular smooth muscle (VSM) relaxation by stimulating soluble guanylyl cyclase (sGC) (7). The subsequent elevation in cGMP activates prot...

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Inhibition of cyclic GMP‐dependent protein kinase‐mediated effects by (Rp)‐8‐bromo‐PET‐cyclic GMPS

Cited by 103 publications

References 28 publications

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

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

Endogenous Type II cGMP-dependent Protein Kinase Exists as a Dimer in Membranes and Can Be Functionally Distinguished from the Type I Isoforms

Pulmonary PKG-1 is upregulated following chronic hypoxia

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