par Malmendier, Claude 
;Delcroix, Claude ;Berman, Mones
Référence The Journal of clinical investigation, 54, 2, page (461-476)
Publication Publié, 1974
;Delcroix, Claude ;Berman, MonesRéférence The Journal of clinical investigation, 54, 2, page (461-476)
Publication Publié, 1974
Article révisé par les pairs
| Résumé : | Palmitate, glucose, and glycerol oxidation to CO2 were investigated in the fasted state in 10 normal subjects and 9 patients (6 hyperlipoproteinemias, 1 xanthomatosis, and 2 glycogenosis) after intravenous injection of [1 14C]palmitate, [1 14C]glucose, or [1 14C]glycerol in tracer amounts. The specific activities and concentrations of plasma palmitate, glycerol, or glucose and expired CO2 were measured at various intervals after the injection for a period of 24 hr. All studies were analyzed in terms of a multicompartment model describing the structure for each of the subsystems, the transfer of carbon label between subsystems, and the oxidation to CO2. A bicarbonate subsystem was also included in the model to account for its role in shaping the CO2 curves. All the CO2 activity following a palmitate injection could be accounted for by a direct oxidative pathway from plasma FFA with the addition of a 20 min delay compartment. The same also applied to glucose, except that the delay compartment had a mean time of about 150 min. Only about a third of the injected glycerol was directly oxidized to CO2 from plasma; the delay time was about 4 min. Most of the remainder was converted to glucose. In normals about 45% of the FFA is oxidized to CO2 directly. This constitutes about 30% of the total CO2 output. In hyperlipemia the CO2 output is nearly unchanged and the contribution from FFA is nearly the same. There is a considerable increase (factor of 2), however, in FFA mobilization, most of which is probably diverted to triglyceride synthesis. The glucose and glycerol subsystems are roughly the same in normals and hyperlipemics. About 50% of glucose is oxidized by the direct pathways which accounts for about 35% of the CO2 output. Glycerol accounts for only 1.5% of the CO2 produced. Major changes occurred in the glycerol and glucose subsystems in glycogenesis. The changes are consistent with the known deficiency in glucose 6 phosphatase in this disorder. There is a considerable reduction (factor of 2 or more) in the release of glucose to plasma (gluconeogenesis) and in the conversion of glycerol to glucose. Despite the integration of the kinetics of the glucose, glycerol, and FFA subsystems over a 24 hr period, 36% of the CO2 production was still unaccounted for in normals and 50% in hyperlipemics. Thus, some of the carbon must wind up in very slowly turning over pools which supply CO2 through subsystems not covered in these studies (triglycerides, glycogen, amino acids, etc.). |
