P Tison scite author profile

The effect of various small and middle molecular substances on blood platelet glycolysis was studied in vitro. Creatinine inhibited glucose utilization only at a concentration of 30 mg/dl; no effect of urea was found. o-Hydroxyphenolic acid and guanidinosuccinic acid, which were supposed to interfere with platelet function, inhibited glucose utilization at concentrations found in plasma of patients with chronic renal failure (CRF). Inhibitor of glucose utilization (IGU) peptide of middle molecular weight was found to inhibit glucose utilization without affecting glycogenolysis or lactate production. No additive or potentiating eífects were found when interaction of different substances was tested. The only exception was a potentiation of IGU action on platelet glucose utilization by creatinine at a concentration of 15 mg/dl. Impaired glucose metabolism caused by ‘uremic toxins’ may contribute to the pathogenesis of bleeding in CRF by affecting platelet function.

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Effects of Dihydropyridines and Their Combination With Aspirin on Blood Pressure and Circadian Platelet Activity in Patients With Essential Hypertension

Tison

Ulicna

et al. 1994

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Blood Pressure, 5-OH Indoleacetic Acid, and Vanilmandelic Acid Excretion and Blood Platelet Aggregation in Hypertensive Patients Treated with Ketanserin

Dzúrik¹,

Fetkovska²,

Brimichová³

et al. 1985

Journal of Cardiovascular Pharmacology

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Treatment of Hypertension With Calcium Antagonists and Aspirin Effects on 24-H Platelet Activity

Fetkovska

Oravcová

et al. 1993

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P Tison

Antioxidant systems in polymorphonuclear leucocytes of Type 2 diabetes mellitus

Uremic ‘Toxins’ and Blood Platelet Carbohydrate Metabolism

Effects of Dihydropyridines and Their Combination With Aspirin on Blood Pressure and Circadian Platelet Activity in Patients With Essential Hypertension

Blood Pressure, 5-OH Indoleacetic Acid, and Vanilmandelic Acid Excretion and Blood Platelet Aggregation in Hypertensive Patients Treated with Ketanserin

Treatment of Hypertension With Calcium Antagonists and Aspirin Effects on 24-H Platelet Activity

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