TY - JOUR
T1 - Mitochondrial resuscitation with exogenous cytochrome c in the septic heart
AU - Piel, David A.
AU - Gruber, Peter J.
AU - Weinheimer, Carla J.
AU - Courtois, Michael R.
AU - Robertson, Charles M.
AU - Coopersmith, Craig M.
AU - Deutschman, Clifford S.
AU - Levy, Richard J.
PY - 2007/9
Y1 - 2007/9
N2 - OBJECTIVE: Mitochondrial dysfunction may play a role in the pathogenesis of sepsis-induced organ dysfunction. Respiratory-chain deficiencies that occur in sepsis, however, have never been shown to cause organ failure or to be reversible. Cytochrome oxidase uses electrons donated by its substrate, cytochrome c, to reduce oxygen to H2O. In the septic heart, cytochrome oxidase is competitively inhibited. We hypothesized that cytochrome oxidase inhibition coupled with reduced substrate availability is a reversible cause of sepsis-associated myocardial depression. DESIGN: Prospective observational study aimed to overcome myocardial cytochrome oxidase inhibition with excess cytochrome c and improve cardiac function. SETTING: University hospital-based laboratory. SUBJECTS: Seventy-five C57Bl6 male mice. INTERVENTIONS: Mice underwent cecal ligation and double puncture, sham operation, or no operation. Exogenous cytochrome c or an equal volume of saline was intravenously injected at the 24-hr time point. All animals were evaluated 30 mins after injection. MEASUREMENTS AND MAIN RESULTS: Exogenous cytochrome c readily repleted cardiac mitochondria with supranormal levels of substrate (>1.6 times baseline), restored heme c content, and increased cytochrome oxidase kinetic activity. This increased left ventricular pressure and increased pressure development during isovolumic contraction (dP/dtmax) and relaxation (dP/dtmin) by >45% compared with saline injection. CONCLUSION: Impaired oxidative phosphorylation is a cause of sepsis-associated myocardial depression, and mitochondrial resuscitation with exogenous cytochrome c overcomes cytochrome oxidase inhibition and improves cardiac function.
AB - OBJECTIVE: Mitochondrial dysfunction may play a role in the pathogenesis of sepsis-induced organ dysfunction. Respiratory-chain deficiencies that occur in sepsis, however, have never been shown to cause organ failure or to be reversible. Cytochrome oxidase uses electrons donated by its substrate, cytochrome c, to reduce oxygen to H2O. In the septic heart, cytochrome oxidase is competitively inhibited. We hypothesized that cytochrome oxidase inhibition coupled with reduced substrate availability is a reversible cause of sepsis-associated myocardial depression. DESIGN: Prospective observational study aimed to overcome myocardial cytochrome oxidase inhibition with excess cytochrome c and improve cardiac function. SETTING: University hospital-based laboratory. SUBJECTS: Seventy-five C57Bl6 male mice. INTERVENTIONS: Mice underwent cecal ligation and double puncture, sham operation, or no operation. Exogenous cytochrome c or an equal volume of saline was intravenously injected at the 24-hr time point. All animals were evaluated 30 mins after injection. MEASUREMENTS AND MAIN RESULTS: Exogenous cytochrome c readily repleted cardiac mitochondria with supranormal levels of substrate (>1.6 times baseline), restored heme c content, and increased cytochrome oxidase kinetic activity. This increased left ventricular pressure and increased pressure development during isovolumic contraction (dP/dtmax) and relaxation (dP/dtmin) by >45% compared with saline injection. CONCLUSION: Impaired oxidative phosphorylation is a cause of sepsis-associated myocardial depression, and mitochondrial resuscitation with exogenous cytochrome c overcomes cytochrome oxidase inhibition and improves cardiac function.
KW - Cytochrome c
KW - Cytochrome oxidase
KW - Heart
KW - Mitochondria
KW - Oxidative phosphorylation
KW - Sepsis
UR - http://www.scopus.com/inward/record.url?scp=34548219032&partnerID=8YFLogxK
U2 - 10.1097/01.CCM.0000278914.85340.FE
DO - 10.1097/01.CCM.0000278914.85340.FE
M3 - Article
C2 - 17855825
AN - SCOPUS:34548219032
SN - 0090-3493
VL - 35
SP - 2120
EP - 2127
JO - Critical care medicine
JF - Critical care medicine
IS - 9
ER -