J Mol Cell Cardiol. 2011 Nov;51(5):627-31. doi: 10.1016/j.yjmcc.2011.08.003. Epub 2011 Aug 16.
The importance of [Ca] in the mitochondrial matrix, [Ca], had been proposed by early work of Carafoli and others [1], [2] and [3]. The key suggestion in the 1970s [4] was that regulatory [Ca] played a role in controlling the rate of activation of tricarboxylic acid cycle dehydrogenases, important in the regulation of ATP production by the electron transport chain (ETC) during oxidative phosphorylation. This view is now established [5] and [6] and the key questions currently debated are to what extent do the mitochondria acquire and release Ca, and what impact do mitochondria have on the dynamic Ca signal in the cardiac ventricular myocyte [7]. Although investigations of Ca dynamics in mitochondria have been problematic, disparate and inconclusive, they have also been both provocative and exciting. A recent special issue of this journal presented contrasting perspectives on the speed, extent and mechanisms of changes in [Ca], and how these changes may influence cellular spatio-temporal [Ca] dynamics [8]. An audio discussion is also available online [9]. The uncertain nature of the signaling pathways is noted in Table 1 (see below) which shows mitochondrial proteins and processes that are of current focus and which remain contentious. Each of the “items” listed is largely unsettled, or is a “work in progress”. There may be advocates for opposing positions noted or recent discoveries that must still be tested at multiple levels by diverse laboratories. Currently, the first item, the mitochondrial sodium/calcium exchanger (NCLX) [10], appears the most solid with respect to the molecular identification and physiological function, whereas, the recently described candidates of the mitochondrial Ca uniporter (MCU) [11] and [12] still need to be verified and broadly examined by the scientific community.
[Ca]在基质中的重要性,[Ca],已被 Carafoli 等人的早期工作[1]、[2]和[3]提出。20 世纪 70 年代的关键建议是[4],调节[Ca]在控制三羧酸循环脱氢酶的激活速率方面发挥作用,这对电子传递链(ETC)在氧化磷酸化过程中产生 ATP 的调节很重要。这一观点现在已经确立[5]和[6],目前正在争论的关键问题是线粒体获取和释放 Ca 的程度,以及线粒体对心脏心室肌细胞中动态 Ca 信号的影响[7]。尽管对线粒体 Ca 动力学的研究一直存在问题,而且结果各不相同,没有定论,但这些研究也具有启发性和令人兴奋。该杂志最近的一个特刊提出了关于[Ca]变化的速度、程度和机制的对比观点,以及这些变化如何影响细胞时空[Ca]动力学[8]。在线也提供了音频讨论[9]。表 1(见下文)指出了信号通路的不确定性,表中显示了当前关注的线粒体蛋白和过程,以及仍然存在争议的线粒体蛋白和过程。列出的每一个“项目”在很大程度上都没有定论,或者仍在进行中。可能有对立观点的支持者或最近的发现需要由不同的实验室在多个层面上进行测试。目前,第一个项目,线粒体钠/钙交换器(NCLX)[10],就分子鉴定和生理功能而言,似乎是最可靠的,而最近描述的线粒体 Ca 单向转运体(MCU)[11]和[12]的候选物仍需要得到科学界的验证和广泛研究。