Publications by authors named "S Nadtochiy"
Article Synopsis
- - The study investigates how the absence of cyclophilin D (CypD) affects mitochondrial function during heart development by comparing wildtype and CypD knockout mice from embryonic day 9.5 to adulthood.
- - Findings reveal that CypD deletion modifies the timing of mitochondrial activity transitions and keeps the mitochondrial permeability transition pore (mPTP) closed throughout development, impacting energy production and metabolic processes.
- - The results imply that adjusting CypD levels could influence heart cell growth and function, potentially serving as a strategy to enhance ATP production and overall cardiac performance in developing hearts.
Ischemic tissues accumulate succinate, which is rapidly oxidized upon reperfusion, driving a burst of mitochondrial reactive oxygen species (ROS) generation that triggers cell death. In isolated mitochondria with succinate as the sole metabolic substrate under non-phosphorylating conditions, 90 % of ROS generation is from reverse electron transfer (RET) at the Q site of respiratory complex I (Cx-I). Together, these observations suggest Cx-I RET is the source of pathologic ROS in reperfusion injury.
View Article and Find Full Text PDFBackground: The effect of the anticoagulant, dabigatran, and its antagonist, idarucizumab, on coagulation remains poorly quantified. There are few pharmacokinetic-pharmacodynamic data available to determine dabigatran dose in humans or animals undergoing cardiopulmonary bypass.
Methods: Five sheep were given intravenous dabigatran 4 mg/kg.
Introduction: Bivalirudin is recommended as an alternative to heparin in cardiac surgery with cardiopulmonary bypass. Although it has been used in infants and children for this indication, there is a paucity of data on the pharmacologic effects of bivalirudin in neonates. Given the immaturity of the hemostatic system in neonates, we hypothesized that coagulation responses to bivalirudin in this population would be different than in adults.
View Article and Find Full Text PDFIschemic tissues accumulate succinate, which is rapidly oxidized upon reperfusion, driving a burst of mitochondrial reactive oxygen species (ROS) generation that triggers cell death. In isolated mitochondria with succinate as the sole metabolic substrate under non-phosphorylating conditions, 90% of ROS generation is from reverse electron transfer (RET) at the Q site of respiratory complex I (Cx-I). Together, these observations suggest Cx-I RET is the source of pathologic ROS in reperfusion injury.
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