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Select G-Protein-Coupled Receptors Modulate Agonist-Induced Signaling via a ROCK, LIMK, and Î²-Arrestin 1 Pathway

Author: Bentolila LaurentÂ A.
Cahill Catherine
Conner David
DeFea Kathryn
Evans Christopher
Fultz Elissa
Minasyan Ani
Mittal Nitish
Pal Katsuri
Pradhan Amynah
Roberts Kristofer
Walwyn Wendy
Publication venue: eScholarship, University of California
Publication date: 01/11/2013
Field of study

eScholarship - University of California

Select G-Protein-Coupled Receptors Modulate Agonist-Induced Signaling via a ROCK, LIMK, and β-Arrestin 1 Pathway

Author: Amynah Pradhan
Ani Minasyan
Catherine Cahill
Christopher Evans
David Conner
Elissa Fultz
Kathryn DeFea
Katsuri Pal
Kristofer Roberts
Laurent A. Bentolila
Nitish Mittal
Wendy Walwyn
Publication venue: 'Elsevier BV'
Publication date: 01/11/2013
Field of study

G-protein-coupled receptors (GPCRs) are typically present in a basal, inactive state but, when bound to an agonist, activate downstream signaling cascades. In studying arrestin regulation of opioid receptors in dorsal root ganglia (DRG) neurons, we find that agonists of delta opioid receptors (δORs) activate cofilin through Rho-associated coiled-coil-containing protein kinase (ROCK), LIM domain kinase (LIMK), and β-arrestin 1 (β-arr1) to regulate actin polymerization. This controls receptor function, as assessed by agonist-induced inhibition of voltage-dependent Ca2+ channels in DRGs. Agonists of opioid-receptor-like receptors (ORL1) similarly influence the function of this receptor through ROCK, LIMK, and β-arr1. Functional evidence of this cascade was demonstrated in vivo, where the behavioral effects of δOR or ORL1 agonists were enhanced in the absence of β-arr1 or prevented by inhibiting ROCK. This pathway allows δOR and ORL1 agonists to rapidly regulate receptor function

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PubMed Central

eScholarship - University of California

Select G-Protein-Coupled Receptors Modulate Agonist-Induced Signaling via a ROCK, LIMK, and Î²-Arrestin 1 Pathway

Author: Bentolila LaurentÂ A.
Cahill Catherine
Conner David
DeFea Kathryn
Evans Christopher
Fultz Elissa
Minasyan Ani
Mittal Nitish
Pal Katsuri
Pradhan Amynah
Roberts Kristofer
Walwyn Wendy
Publication venue: eScholarship, University of California
Publication date: 01/11/2013
Field of study

G-protein coupled receptors (GPCRs) are typically present in a basal, inactive state, but when bound to agonist they activate downstream signaling cascades. In studying arrestin regulation of opioid receptors in dorsal root ganglia (DRG) neurons, we find that agonists of delta opioid receptors (δORs) activate cofilin through Rho-associated coiled-coiled containing protein kinase (ROCK), LIM domain kinase (LIMK) and β- arrestin 1 (β-arr1), to regulate actin polymerization. This controls receptor function, as assessed by agonist-induced inhibition of voltage-dependent Ca2+ channels in DRGs. Agonists of opioid-receptor like receptors (ORL1) similarly influence the function of this receptor through ROCK, LIMK and β-arr1. Functional evidence of this cascade was demonstrated in vivo where the behavioral effects of δOR or ORL1 agonists were enhanced in the absence of β-arr1 or prevented by inhibiting ROCK. This pathway allows δOR and ORL1 agonists to rapidly regulate receptor function

Crossref

Directory of Open Access Journals

PubMed Central

eScholarship - University of California