Ashkenazi_1987_Science_238_672

Reference

Title : An M2 muscarinic receptor subtype coupled to both adenylyl cyclase and phosphoinositide turnover - Ashkenazi_1987_Science_238_672
Author(s) : Ashkenazi A , Winslow JW , Peralta EG , Peterson GL , Schimerlik MI , Capon DJ , Ramachandran J
Ref : Science , 238 :672 , 1987
Abstract :

To investigate whether a particular receptor subtype can be coupled to multiple effector systems, recombinant M2 muscarinic receptors were expressed in cells lacking endogenous receptor. The muscarinic agonist carbachol both inhibited adenylyl cyclase and stimulated phosphoinositide hydrolysis. The stimulation of phosphoinositide hydrolysis was significantly less efficient and more dependent on receptor levels than the inhibition of adenylyl cyclase. Both responses were mediated by guanine nucleotide binding proteins, as evidenced by their inhibition by pertussis toxin; the more efficiently coupled adenylyl cyclase response was significantly more sensitive. Thus, individual subtypes of a given receptor are capable of regulating multiple effector pathways.

PubMedSearch : Ashkenazi_1987_Science_238_672
PubMedID: 2823384

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Citations formats

Ashkenazi A, Winslow JW, Peralta EG, Peterson GL, Schimerlik MI, Capon DJ, Ramachandran J (1987)
An M2 muscarinic receptor subtype coupled to both adenylyl cyclase and phosphoinositide turnover
Science 238 :672

Ashkenazi A, Winslow JW, Peralta EG, Peterson GL, Schimerlik MI, Capon DJ, Ramachandran J (1987)
Science 238 :672