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Abstract
Yeast beta-(1 goes to 3)glucan synthetase is stimulated by ATP or GTP. The structural requirements for the activation were investigated by testing several phosphorylated compounds. The simplest substance with stimulatory ability was inorganic pyrophosphate. Addition of a nucleoside, as in GDP, decreased the concentration required for half-maximal stimulation; a third phosphate group, as in GTP, further enhanced the stimulatory capacity. On the other hand, esterification of the terminal phosphate of GTP with a nucleoside or a methyl group led to a total loss of activating ability: dinucleoside triphosphates and the gamma-phosphate methyl ester of GTP acted as competitive antagonists of the activators. alpha,beta- and beta,gamma-imino and -methylene derivatives of both ATP and GTP stimulated the enzymatic activity, suggesting that activation can occur without covalent transfer either of the terminal phosphate or pyrophosphate, or of the nucleotidyl residue. The stimulatory effect of the beta,gamma-imino derivatives of ATP and GTP was not additive. The inhibition constants obtained with gamma-phosphate esters of GTP were the same for either one of the two imino analogs. It is concluded that adenosine and guanosine derivatives bind to the same domain of the enzyme. It is also postulated that activators may interact with the enzyme or with a regulatory protein at two locations, a binding site for the nucleoside moiety and a "functional" site for the pyrophosphate residue.
Highlights
Yeast 8-(1-+ 3)glucan synthetase is stimulated by preparation as well as by the different conditionsrequired for ATP or GTP
The structural requirements for the acti- optimal effect of guanosine and adenosine nucleotides (3).For vation were investigated by testing several phospho- these reasons, we could not ascertain whether both types of rylated compounds
Esterification of the terminal phosphate of GTP with a nucleoside or a methyl group led to a total loss of activating ability: dinucleoside triphosphates and the y-phosphatemethyl availability of nucleotide analogs which are resistant to phosphatase action and whose stimulatory activity is less sensitive to environmental conditions has provided a new approach to this problem
Summary
Yeast 8-(1-+ 3)glucan synthetase is stimulated by preparation as well as by the different conditionsrequired for ATP or GTP. As in GDP, decreased the concentration required for half-maximal stimulation; a third phosphate group, as in GTP, further enhanced the stimulatory capacity. Esterification of the terminal phosphate of GTP with a nucleoside or a methyl group led to a total loss of activating ability: dinucleoside triphosphates and the y-phosphatemethyl availability of nucleotide analogs which are resistant to phosphatase action and whose stimulatory activity is less sensitive to environmental conditions has provided a new approach to this problem. With the use of these and other model compounds it has been possible to determine more precisely the structural requirements for activation of glucan synthetase. Ester of GTP acted as competitive antagonists of the activators. a$- and 8,y-imino and -methylene deriva-
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