BIOENERGETICS AND CONTROL OF OXYGEN-CONSUMPTION IN THE IN-SITU RAT-HEART

Authors
HEADRICK JP DOBSON GP WILLIAMS JP MCKIRDY JC JORDAN L WILLIS RJ
Citation
Jp. Headrick et al., BIOENERGETICS AND CONTROL OF OXYGEN-CONSUMPTION IN THE IN-SITU RAT-HEART, The American journal of physiology, 267(3), 1994, pp. 80001074-80001084
Citations number
42
Categorie Soggetti
Physiology
Journal title
The American journal of physiologyACNP
ISSN journal
00029513
Volume
267
Issue
3
Year of publication
1994
Part
2
Pages
80001074 - 80001084
Database
ISI
SICI code
0002-9513(1994)267:3<80001074:BACOOI>2.0.ZU;2-4
Abstract
Control of respiration by products of ATP hydrolysis was examined in t he in situ rat heart using a purpose-built nuclear magnetic resonance (NMR) coil. The in situ ratio of phosphocreatine to ATP concentrations ([PCr]/[ATP]) was 2.30 +/- 0.05, free Mg2+ concentration ([Mg2+]) was 0.57 mM, and cytosolic pH was 7.35 +/- 0.03 (n = 7). Basal inorganic phosphate concentration ([P-i]) was below NMR detection but was estima ted to be 0.83 mM. The [ATP]/[ADP] [P-i] ratio, free ADP concentration ([ADP]), and free energy of ATP hydrolyses (Delta G(ATP)) were calcul ated to be 700,000 +/- 78,000 M(-1), 18 +/- 3 mu M, and -63.93 +/- 0.3 3 kJ/mol in situ, respectively (n = 7). In contrast, in the Langendorf f perfused rat heart [ATP]/[ADP] [P-i] was only 76,140 +/- 12,830 M(-1 ), [ADP] was 65 +/- 9 mu M, and Delta G(ATP) was -59.92 +/- 0.48 kJ/mo l (n = 7), all indicative of a lower energy state in vitro. Epinephrin e infusion in situ (0.9 mu g . min(-1) . kg(-1)) increased the rate-pr essure product 2.05-fold. During stimulation [ATP] was stable at 97 +/ - 3% signal intensity, [PCr] declined by 25%, and [P-i] increased to 1 .83 mM. Cytosolic pH was 7.27 +/- 0.01 and [Mg2+] was 0.64 +/- 0.05 mM . [PCr]/[ATP] declined to 1.83 +/- 0.13, and [ATP]/[ADP] [P-i] fell to 108,000 +/- 15,000 M(-1). Delta G(ATP) only fell marginally to -59.56 +/- 0.49 kJ/mol. Free [ADP] increased threefold to 55 +/- 10 mu M. In fusion of 2.8 +/- 0.5 mu g . min(-1) . kg(-1) epinephrine increased th e rate-pressure product 2.7-fold, further reduced [ATP]/[ADP] [P-i] (5 % of basal), and elevated [ADP] more than fourfold without changing [A TP]. We conclude that the in situ heart is highly energetic compared w ith isolated perfused hearts and operates at a different metabolic ''s et-point.'' Because free [ADP] and [P-i] in situ approximate apparent Michaelis constants for mitochondrial respiration in vitro and increas e with increased cardiac work, we conclude that each fulfills the crit eria for the kinetic control of O-2 consumption in the in situ rat myo cardium.