TY - JOUR
T1 - Schistosoma mansoni
T2 - Inhibition of glucosephosphate isomerase and glycolysis by sugar phosphates
AU - Shapiro, Theresa A.
AU - Talalay, Paul
N1 - Funding Information:
These studies were supported by National Institutes of Health Research Grants GM 16492 and AI 18349, Training Grant GM 1183, and United States Agency for International Development Contract D.P.E.-5921-G-00-1009-00. The helpful advice of our colleague Professor Ernest Bueding is acknowledged with gratitude. Miss Marguerite Renaud provided expert technical assistance. Theresa A. Shapiro is a Fellow of the Stetler Research Fund for Women Physicians.
Copyright:
Copyright 2014 Elsevier B.V., All rights reserved.
PY - 1982/10
Y1 - 1982/10
N2 - Glucosephosphate isomerase (EC 5.3.1.9) of Schistosoma mansoni is inhibited competitively by a number of tetrose, pentose, and hexose phosphates with inhibitor constant (Ki) values in the range of 0.5 to 400 μM. The most potent inhibitor is 5-phospho-d-arabinonate which resembles the cis-enediolate transition state intermediate of the reaction. These analogs were also found to be effective inhibitors of the production of lactate from glucose by suitably supplemented worm homogenates. The rank order of potency of inhibition of glycolysis was inversely related to the magnitudes of the Ki values for glucosephosphate isomerase. These Ki values were similar to those previously reported for mammalian glucosephosphate isomerase, suggesting similarities in the steric and electronic characteristics of the active sites of these isofunctional enzymes. This conclusion was further supported by the observed pH dependence of the inhibition by 5-phospho-d-arabinonate. Although glucosephosphate isomerase is not a rate-limiting enzyme of glycolysis, in the conventional sense, its selective inhibition could be of chemotherapeutic importance, in part because of the accumulation in glycolyzing systems of glucose 6-phosphate which is a potent feedback inhibitor of hexokinase.
AB - Glucosephosphate isomerase (EC 5.3.1.9) of Schistosoma mansoni is inhibited competitively by a number of tetrose, pentose, and hexose phosphates with inhibitor constant (Ki) values in the range of 0.5 to 400 μM. The most potent inhibitor is 5-phospho-d-arabinonate which resembles the cis-enediolate transition state intermediate of the reaction. These analogs were also found to be effective inhibitors of the production of lactate from glucose by suitably supplemented worm homogenates. The rank order of potency of inhibition of glycolysis was inversely related to the magnitudes of the Ki values for glucosephosphate isomerase. These Ki values were similar to those previously reported for mammalian glucosephosphate isomerase, suggesting similarities in the steric and electronic characteristics of the active sites of these isofunctional enzymes. This conclusion was further supported by the observed pH dependence of the inhibition by 5-phospho-d-arabinonate. Although glucosephosphate isomerase is not a rate-limiting enzyme of glycolysis, in the conventional sense, its selective inhibition could be of chemotherapeutic importance, in part because of the accumulation in glycolyzing systems of glucose 6-phosphate which is a potent feedback inhibitor of hexokinase.
KW - 2-deoxy-d-glucose 6-phosphate
KW - 5-phospho-d-arabinonate
KW - 6-phosphogluconate
KW - Glucosamine 6-phosphate
KW - Glucosephosphate isomerase (EC 5.3.1.9)
KW - Glycolysis
KW - Inhibition, competitive
KW - Schistosoma mansoni, adult
KW - Trematode, parasitic
KW - d-arabinose 5-phosphate
KW - d-erythrose 4-phosphate
KW - d-sorbitol 6-phosphate
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U2 - 10.1016/0014-4894(82)90127-8
DO - 10.1016/0014-4894(82)90127-8
M3 - Article
C2 - 7128716
AN - SCOPUS:0020361163
SN - 0014-4894
VL - 54
SP - 196
EP - 201
JO - Experimental Parasitology
JF - Experimental Parasitology
IS - 2
ER -