Regulation of Adenylyl Cyclase, ERK1/2, and CREB by G<sub>z</sub> Following Acute and Chronic Activation of the δ‐Opioid Receptor

Tso, Prudence H.; Yung, Lisa Y.; Wong, Yung Hou

doi:10.1046/j.1471-4159.2000.0741685.x

Cited by 39 publications

(44 citation statements)

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“…Failure of PKA inhibitors to modify acute morphine analgesia also supports the notion that cAMP effectors are minimally involved in the acute analgesic responses to opioids (Bernstein and Welch, 1999), as does the observation that phosphodiesterase inhibitors do not modify analgesia caused by intracerebroventricular or intrathecal administration of DPDPE (Suh et al, 1995). On the other hand, cAMP signaling has been consistently implicated in cellular adaptations that result from sustained DOPr stimulation and may contribute to analgesic tolerance (Tso et al, 2000;Varga, 2003;Zhang et al, 2006). These adaptations generally involve an increase in AC catalytic activity, although the mechanisms contributing to such an increase vary according to the type of AC involved (Avidor-Reiss et al, 1997;Varga, 2003).…”

mentioning

confidence: 56%

“…In immortalized cell lines expressing either endogenous or recombinant DOPr, Gai2 has been frequently associated with cAMP inhibition, although additional subtypes are also involved in this response (Table 4). For example, DOPrs expressed in Chinese hamster ovary (CHO), COS cells (George et al, 2000;Fan et al, 2005), and HEK293 cells (Tsu et al, 1997;Tso et al, 2000) activate Gaz and modulate AC activity in a PTXinsensitive manner. In COS and CHO cells, AC inhibition by DOPr agonists was only evident when these receptors were coexpressed with MOPrs (George et al, 2000); however, in HEK cells, DOPrs expressed by themselves were able to both inhibit (Tsu et al, 1997;Ho and Wong, 2000;Tso et al, 2000) or stimulate cAMP production via Gaz (Tsu et al, 1997;Ho et al, 2001).…”

Section: A D-opioid Receptors and Adenylate Cyclase Signalingmentioning

confidence: 99%

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Molecular Pharmacology ofδ-Opioid Receptors

et al. 2016

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confidence: 56%

Section: A D-opioid Receptors and Adenylate Cyclase Signalingmentioning

confidence: 99%

Molecular Pharmacology ofδ-Opioid Receptors

et al. 2016

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“…It has been previously demonstrated that ␦-or -ORs expressed in HEK293 cells or Rat-1 fibroblasts stimulate ERK1/2 activity via PTX-sensitive or -insensitive G protein signaling mechanisms (Burt et al, 1996;Tso et al, 2000;Belcheva et al, 2002). To examine whether the ␦-i3L peptide can be also used as potential inhibitor of this type of GPCR signaling, ERK activation was measured in response to ␦-and -opioid agonist stimulation in serum-starved HEK293 cells expressing these receptors.…”

Section: Downloaded Frommentioning

confidence: 99%

Expression of the Third Intracellular Loop of the δ-Opioid Receptor Inhibits Signaling by Opioid Receptors and Other G Protein-Coupled Receptors

Morou

Georgoussi²

2005

J Pharmacol Exp Ther

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To explore the feasibility of developing inhibitors of signaling by opioid receptors and other G protein-coupled receptors (GPCRs) that use the same G protein pool, we investigated the capacity of a minigene encoding the third intracellular loop of the ␦-opioid receptor (␦-i3L) to act as competitive antagonist of the receptor-G protein interface interaction. In ␦-i3L-expressing cells, the peptide blocked high-affinity agonist binding to both the ␦-and the -opioid (␦-OR and -OR) and attenuated opioid and ␣ 2 -adrenergic receptor (␣2AR)-dependent [35 S]guanosine-5Ј-O-(3-thio)triphosphate binding. Furthermore, ␦-i3L expression resulted in inhibition of ␦-, -OR-, and ␣2AR-receptormediated cAMP accumulation, whereas the cAMP response produced by activation of the ␤ 2 -adrenergic receptor was unaffected, suggesting that the inhibitory effects of ␦-i3L expression were selective for G i /G o proteins. Moreover, although ␦-i3L expression also attenuated drastically phospholipase C accumulation and Ca 2ϩ release following -and ␦-OR stimulation, it failed to inhibit carbachol-mediated stimulation of inositol phosphate accumulation in M1-muscarinic receptor-expressing human embryonic kidney 293 cells. Finally, we also examined the effects of ␦-i3L expression on the regulation of the extracellular signal-regulated kinase (ERK) mitogen-activated protein kinase pathway. Our results demonstrate that, although ERK activation by -and ␦-ORs is attenuated by the presence of ␦-i3L, ERK activation mediated by ␣2AR remained unaffected. Collectively, our data demonstrate that the ␦-i3L can be used as potent inhibitor of G protein signaling for various GPCRs that use a common pool of G proteins.

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“…Cells were assayed for ERK and JNK activities as previously described [36,37]. Briefly, cells were challenged with chemokines and the cell contents were extracted, separated by SDS-PAGE, and transferred to nitrocellulose membrane before incubation with antisera against phospho-ERK1/2 or phospho-JNK and detection using the ECL kit.…”

Section: Western Blotting Analysis and Mapk Assaysmentioning

confidence: 99%

Differential chemokine activation of CC chemokine receptor 1‐regulated pathways: ligand selective activation of Gα ₁₄‐coupled pathways

et al. 2004

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Chemokines regulate the chemotaxis, development, and differentiation of many cell types enabling the regulation of routine immunosurveillance and immunological adaptation. CC chemokine receptor 1 (CCR1) is the target of 11 chemokines. This promiscuity of receptorligand interactions and the potential for functional redundancy has led us to investigate the selective activation of CCR1-coupled pathways by known CCR1 agonists. Chemokines leukotactin-1, macrophage inflammatory protein (MIP)-1 § , monocyte chemotactic peptide (MCP)-3, RANTES, and MIP-1ˇall inhibited adenylyl cyclase activity in cells transiently transfected with CCR1. In contrast, only MIP-1ˇwas unable to signal via G 14 -, G 16 -or chimeric 16z44-coupled pathways. In a stable cell line expressing CCR1 and G § 14 , all of these five chemokines along with hemofiltrate CC chemokine (HCC)-1 and myeloid progenitor inhibitory factor (MPIF)-1 were able to stimulate G i/o -coupled pathways, but MIP-1ˇ, HCC-1 and MPIF-1 were unable to activate G 14 -mediated stimulation of phospholipase C g activity. In addition, MIP-1ˇwas unable to promote the phosphorylation of extracellular signalregulated kinase and c-Jun N-terminal kinase. This suggests that different chemokines are able to selectively activate CCR1-coupled pathways, probably because of different intrinsic ligand efficacies. CCR1 and G § 14 or G § 16 are co-expressed in several cell types and we hypothesize that selective activation of chemokine receptors provides a mechanism by which chemokines are able to fine-tune intracellular signaling pathways.

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Regulation of Adenylyl Cyclase, ERK1/2, and CREB by G_z Following Acute and Chronic Activation of the δ‐Opioid Receptor

Cited by 39 publications

References 40 publications

Molecular Pharmacology ofδ-Opioid Receptors

Molecular Pharmacology ofδ-Opioid Receptors

Expression of the Third Intracellular Loop of the δ-Opioid Receptor Inhibits Signaling by Opioid Receptors and Other G Protein-Coupled Receptors

Differential chemokine activation of CC chemokine receptor 1‐regulated pathways: ligand selective activation of Gα ₁₄‐coupled pathways

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Regulation of Adenylyl Cyclase, ERK1/2, and CREB by Gz Following Acute and Chronic Activation of the δ‐Opioid Receptor

Cited by 39 publications

References 40 publications

Molecular Pharmacology ofδ-Opioid Receptors

Molecular Pharmacology ofδ-Opioid Receptors

Expression of the Third Intracellular Loop of the δ-Opioid Receptor Inhibits Signaling by Opioid Receptors and Other G Protein-Coupled Receptors

Differential chemokine activation of CC chemokine receptor 1‐regulated pathways: ligand selective activation of Gα 14‐coupled pathways

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Product

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About

Regulation of Adenylyl Cyclase, ERK1/2, and CREB by G_z Following Acute and Chronic Activation of the δ‐Opioid Receptor

Differential chemokine activation of CC chemokine receptor 1‐regulated pathways: ligand selective activation of Gα ₁₄‐coupled pathways