Structure-Activity Relationships of Cardiotonic Steroids for the Inhibition of Sodium- and Potassium-Dependent Adenosine Triphosphatase: III. Dissociation Rate Constants of Various Enzyme—Cardiac Glycoside Complexes Formed in the Presence of Sodium, Magnesium, and Adenosine Triphosphate

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Structure-Activity Relationships of Cardiotonic Steroids for the Inhibition of Sodium- and Potassium-Dependent Adenosine Triphosphatase

III. Dissociation Rate Constants of Various Enzyme—Cardiac Glycoside Complexes Formed in the Presence of Sodium, Magnesium, and Adenosine Triphosphate

ATSUNOBU YODA ¹ and SHIZUKO YODA ¹

¹ Department of Pharmacology, University of Wisconsin Medical School, Madison, Wisconsin 53706

The dissociation rate constants (k_d) of cardiac monoglycoside—(Na⁺+ K⁺)-ATPase complexes formed in the Na⁺-Mg²⁺-ATP system (typeI complex) were determined by enzymatic assay after dilution.The k_d value of each cardiac glycoside—enzyme complex thusformed was greater than that of the complex formed in the Mg²⁺-P_isystem (type II complex). Whereas the k_d values of type II complexeswere dependent only on the sugar moiety, the k_d values of typeI complexes were affected by both the steroid and sugar moieties.For cardiac glycoside—enzyme complexes in which the sugarmoiety was the same, the stability of type I complexes increasedin the order: digitoxigenin glycoside < strophanthidin glycoside< digoxigenin glycoside and strophanthidin glycoside <ouabagenin glycoside. If the steroid moiety was the same, thestability increased in the order: digitoxide [unknown]6-deoxyglucoside [unknown] fucoside < 6-deoxyguloside< rhamnoside. Methylation of the sugar 3'-hydroxyl groupdecreased stability. These data indicate that in type I complexesa sugarspecific site(s) on the enzyme binds the sugar moietyat the 2'- $agr$ - and 3'- $agr$ or $beta$ -hydroxyl groups by hydrogen bond(s),and at the 5'- $agr$ -methyl group by a hydrophobic bond. The activationenergy of this dissociation was approximately 30 kcal/mol withall the cardiac monoglycosides tested. The differences in k_dvalues between type I and type II complexes indicate that thetwo are distinct, possibly as a result of conformational differencesin the sugar-specific site of the (Na⁺ + K⁺)-ATPase.

Note:
ACKNOWLEDGMENT We thank Dr. Lowell E. Hokin for his interest and thoughtful help with the manuscript.

Submitted on October 24, 1973