Department of Physiology, Wayne State University School of Medicine, Detroit, MI 48201, USA.
Am J Physiol Regul Integr Comp Physiol. 2013 Feb 15;304(4):R286-95. doi: 10.1152/ajpregu.00517.2012. Epub 2013 Jan 9.
Multiple systems and regulatory strategies interact to control cardiac homeostasis. In fact, regulated systems, feedback controls, and redundant control mechanisms dominate in whole animals. Accordingly, molecular and cellular tools and techniques must be utilized in complex models with multiple systems and regulatory strategies to fully appreciate the physiological context. Currently, these techniques are mainly performed under conditions remote from the normal in vivo condition; thus, the extrapolation of molecular changes to the in vivo situation and the facilitation of translational aspect of the findings are limited. A major obstacle has been the reliance on preparations that do not mimic the clinical or physiological situation. This is particularly true regarding measurements of cardiac function in mice. To address these concerns, we used a permanently implanted Doppler ultrasonic flow probe on the ascending aorta and coronary artery occluder for repeated measurements of ascending aortic blood flow (cardiac output) in conscious mice, at rest and during exercise, before and during coronary artery occlusion/reperfusion and infarction. The conscious mouse model permits detailed monitoring of within-animal changes in cardiac function during myocardial ischemia, reperfusion, and infarction in an intact, complex model free of the confounding influences of anesthetics, surgical trauma, and restraint stress. Results from this study suggest that previous protocols may have overestimated resting baseline values and underestimated cardiac output reserve. Using these procedures in currently available spontaneous or engineered mouse mutants has the potential to be of major importance for advancing the concepts and methods that drive cardiovascular research.
多个系统和调节策略相互作用以控制心脏的稳态。事实上,在整体动物中,受调节的系统、反馈控制和冗余的控制机制占据主导地位。因此,在具有多个系统和调节策略的复杂模型中,必须利用分子和细胞工具及技术,才能充分了解生理背景。目前,这些技术主要在远离正常体内条件的情况下进行;因此,分子变化向体内情况的推断以及研究结果转化的促进受到限制。一个主要障碍是依赖于不能模拟临床或生理情况的制剂。这在测量小鼠心脏功能方面尤其如此。为了解决这些问题,我们在升主动脉和冠状动脉结扎器上使用了永久性植入的多普勒超声流量探头,以便在清醒的小鼠休息和运动时、在冠状动脉闭塞/再灌注和梗塞之前和期间,对升主动脉血流(心输出量)进行重复测量。清醒的小鼠模型允许在完整的、复杂的模型中,在没有麻醉、手术创伤和约束应激等混杂影响的情况下,对心肌缺血、再灌注和梗塞期间心脏功能的个体内变化进行详细监测。本研究的结果表明,以前的方案可能高估了静息基础值,低估了心输出量储备。在目前可用的自发或工程化的小鼠突变体中使用这些程序,对于推进推动心血管研究的概念和方法具有重要意义。