N-Substituted dibenzoxazepines as analgesic PGE2 antagonists

Hallinan, E. Ann; Hagen, Timothy J.; Husa, R. K.; Tsymbalov, Sofya; Rao, Sheila; Vanhoeck, Jp.; Rafferty, Michael; Stapelfeld, Awilda; Savage, Michael A.; Reichman, Melvin

doi:10.1021/jm00074a010

Cited by 74 publications

(45 citation statements)

References 4 publications

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“…Both EP1 receptor antagonists (16)(17)(18) and EP1 knockout mice exist, but have not been characterized in models of hypertension. While conventional targeting of the gene encoding EP1 in mice suggests a role for EP1 in maintaining basal blood pressure (19), interpretation of these data is complicated by the circumstance that the EP1 locus encompasses a second gene on the antiparallel strand, the serine/ threonine protein kinase N (PKN) (20).…”

Section: Introductionmentioning

confidence: 99%

Antihypertensive effects of selective prostaglandin E2 receptor subtype 1 targeting

Guan¹,

Zhang²,

Wu³

et al. 2007

J. Clin. Invest.

106

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Section: Introductionmentioning

confidence: 99%

Antihypertensive effects of selective prostaglandin E2 receptor subtype 1 targeting

Guan¹,

Zhang²,

Wu³

et al. 2007

J. Clin. Invest.

106

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“…In order to determine whether EP1 receptors are also involved, the EP1 receptor antagonist SC-51089 [32][33][34] was employed. Initially, the effect of increasing concentrations of SC-51089 on the stimulatory effect of 0.028 μM PGE 1 was examined.…”

Section: Pge 1 Stimulation Of the β1 Promoter: Signaling Through Ep1 mentioning

confidence: 99%

Involvement of EP1 and EP2 receptors in the regulation of the Na,K-ATPase by prostaglandins in MDCK cells

Matlhagela

Taub

2006

Prostaglandins & Other Lipid Mediators

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Prostaglandins are key regulators of ion transport in the kidney. In MDCK cells, which model distal tubule cells, the transcription of the Na,K-ATPase β1 subunit is regulated by PGE 1 and PGE 2 . To identify the EP receptors that mediate transcriptional regulation, transient transfection studies are conducted using the human β1 promoter/luciferase construct, pHβ1-1141 Luc. The involvement of EP1 and EP2 receptors is indicated by studies with the EP1 selective agonist 17-phenyl trinor PGE 2 , and the EP2 selective agonist butaprost (which stimulate), as well as by studies with the antagonists SC-51089 (EP1 specific) and AH 6809 (EP1 and EP2 specific). Consistent with the involvement of Gs coupled EP2 receptors, is that the PGE 1 stimulation is inhibited by the PKAI expression vector (encoding the protein kinase A (PKA) inhibitory protein), as well as by the myristolated PKA inhibitory peptide PKI. In addition to this evidence (for the involvement of EP2 receptors), evidence for the involvement of EP1 receptors in the PGE 1 mediated stimulation of Na,KATPase β subunit gene transcription includes the stimulatory effect of 17-phenyl trinor PGE 2 , as well as the inhibitory effects of SC-51089. Also consistent with the involvement of Gq coupled EP1 receptors, the PGE 1 stimulation is inhibited by the PKCI vector (encoding the PKC inhibitory domain), the PKC inhibitor Go 6976, thapsigargin, as well as the calmodulin antagonists W7 and W13.

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“…Studies which were aimed to identify key structural requirements to synthesize EP selective agonists and/or antagonists and to provide insights to the mechanism of receptor ligand selectivity revealed that sensitive positions for agonist-activity at the EP1 receptor is the hydroxyl group at the carbon 15 position and C-1 carboxylate [29]. The selective EP1 antagonists may aid in characterization of the effects mediated by this receptor subtype [30][31][32]. The reported selective EP1 receptor antagonists are the acylhydrazide derivative SC51322 (by Searle group) [31], ZD6416 (by AstraZeneca) [33,34], ONO-8713 (by Ono) [35] and thiophene derivative ((by Merck Frosst) [36].…”

Section: Introductionmentioning

confidence: 99%

“…The selective EP1 antagonists may aid in characterization of the effects mediated by this receptor subtype [30][31][32]. The reported selective EP1 receptor antagonists are the acylhydrazide derivative SC51322 (by Searle group) [31], ZD6416 (by AstraZeneca) [33,34], ONO-8713 (by Ono) [35] and thiophene derivative ((by Merck Frosst) [36]. Studies revealed that EP1 receptor plays a central role in PGE2-mediated allodynia [37,38] and inflammatory pain [39].…”

Section: Introductionmentioning

confidence: 99%

QSAR rationales for the 1,2-diarylcyclopentenes as prostaglandin EP1 receptor antagonists: Potentially useful in the treatment of inflammatory pain

Sharma¹,

Pilania²,

Singh³

2010

Eur. J. Chem.

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N-Substituted dibenzoxazepines as analgesic PGE2 antagonists

Cited by 74 publications

References 4 publications

Antihypertensive effects of selective prostaglandin E2 receptor subtype 1 targeting

Antihypertensive effects of selective prostaglandin E2 receptor subtype 1 targeting

Involvement of EP1 and EP2 receptors in the regulation of the Na,K-ATPase by prostaglandins in MDCK cells

QSAR rationales for the 1,2-diarylcyclopentenes as prostaglandin EP1 receptor antagonists: Potentially useful in the treatment of inflammatory pain

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