(R(P))-CAMPS INHIBITS THE CAMP-DEPENDENT PROTEIN-KINASE BY BLOCKING THE CAMP-INDUCED CONFORMATIONAL TRANSITION

(R(P))-cAMPS is known to inhibit competitively the cAMP-induced activa tion of cAMP-dependent protein kinase (PKA). The molecular nature of t his inhibition, however, is unknown. By monitoring the intrinsic trypt ophan fluorescence of recombinant type I regulatory submit of PKA unde r unfolding conditions, a free energy value (Delta G(D)(H2O)) of 8.23 +/- 0.22 kcal/mol was calculated, The cAMP-free form of the regulatory subunit was less stable with Delta G(D)(H2O) = 6.04 +/- 0.05 kcal/mol . Native stability was recovered by treatment of the cAMP-free protein with either cAMP or (S-P)-cAMPS but not with (R(P))-cAMPS. Thus, (R(P ))-cAMPS binding to the regulatory subunit keeps the protein in a lock ed conformation, unable to release the catalytic subunit. This finding was further supported by demonstrating that holoenzyme formation was greatly accelerated only when bound cAMP was replaced with (R(P))-cAMP S but not with cAMP or (S-P)-cAMPS.