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J. Biol. Chem., Vol. 256, Issue 4, 1593-1597, 02, 1981
H Arad, G Rimon and A Levitzki
The guanylyl imidodiphosphate-activated state of turkey erythrocyte cyclase
can be reversed to the basal state by the simultaneous action of
beta-agonists and GTP. The rate of reversal diminishes progressively with
decreasing concentration of beta-adrenergic receptors on the membrane
surface, whereas the extent of reversal is always maximal. The rate of
reversal is found to be linearly dependent on the concentration of
beta-adrenergic receptors within the membranes. This result supports the
notion that the interaction of the enzyme unit and the beta- adrenergic
receptor is catalytic and therefore of the "collision coupling" type. The
dependence of the rate of reversal reaction on epinephrine concentration is
noncooperative with an apparent dissociation constant of KD = 3.0 X 10(-6)
M. The fraction of guanylyl imidodiphosphate-activated cyclase system which
can be reversed by GTP and a beta-agonist strongly depends on temperature
and reveals a sharp transition at 24 degrees C which is the freezing
temperature of the inner monolayer. It is suggested that the GTP regulatory
unit is inactive when the inner monolayer is frozen.
The reversal of the Gpp(NH)p-activated state of adenylate cyclase by GTP and hormone is by the "collision coupling" mechanism
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  A Levitzki From epinephrine to cyclic AMP Science, August 12, 1988; 241(4867): 800 - 806. [Abstract] [PDF]
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