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心室肌细胞逐搏按需ATP合成的演示揭示了性别特异性线粒体和胞质动力学。

Demonstration of Beat-to-Beat, On-Demand ATP Synthesis in Ventricular Myocytes Reveals Sex-Specific Mitochondrial and Cytosolic Dynamics.

作者信息

Rhana Paula, Matsumoto Collin, Santana L Fernando

出版信息

bioRxiv. 2025 Jul 10:2025.07.07.663572. doi: 10.1101/2025.07.07.663572.

Abstract

UNLABELLED

The substantial energetic demands on ventricular myocytes imposed by the transport of ions and cross-bridge cycling associated with each heartbeat are well known, yet the spatiotemporal dynamics of ATP supply and demand remain poorly understood. Here, using confocal microscopy and genetically encoded fluorescent sensors targeted to mitochondria and cytosol, we visualized beat-to-beat ATP dynamics in ventricular myocytes from adult male and female mice. These probes showed fluctuations in mitochondrial ATP levels with each contraction, revealing two distinct, spatially localized waveforms-ATP "gain" and ATP "dip"-representing transient increases or decreases in matrix ATP levels, respectively. These waveforms were tightly phase-locked to intracellular Ca transients and organized into energetic microdomains. Although female myocytes exhibited larger local mitochondrial ATP transients than their male counterparts, their total mitochondrial volume was lower. Female myocytes also exhibited tighter coupling between the sarcoplasmic reticulum and mitochondria and showed a higher concentration of mitofusin 2 and ATP synthase catalytic α-subunit per unit volume, suggesting more efficient ATP production. Cytosolic ATP transients mirrored mitochondrial waveforms and domain structure in both male and female myocytes. During faster pacing, diastolic cytosolic ATP rose more rapidly in female myocytes, whereas the accompanying beat-locked ATP transients increased in both sexes but did so proportionally more in males than in females. These findings demonstrate that ATP is synthesized on demand-beat by beat-in a modular, microdomain-specific manner. We propose that male myocytes rely on greater mitochondrial mass for energetic scaling, whereas female cells employ architectural precision to optimize ATP delivery.

KEY POINTS SUMMARY

It is known that each heartbeat requires precise ATP delivery to fuel ion transport and cross-bridge cycling, but the timing and spatial organization of ATP production in heart cells has been unclear.Using advanced imaging and genetically encoded sensors, we visualized beat-to-beat ATP fluctuations in the mitochondria and cytosol of individual male and female mouse ventricular myocytes. Mitochondrial ATP levels rose or fell with each beat in spatially confined regions, forming ATP "gain" or "dip" microdomains that were synchronized with Ca transients. At higher firing rates, beat-locked, diastolic ATP transients rose more quickly in female myocytes, but were larger in male myocytes, highlighting distinct sex-specific strategies for matching energy supply to contractile demand.Ventricular myocytes "live paycheck-to-paycheck", producing just enough ATP on demand to fuel each beat. Male and female myocytes adopt distinct strategies to meet this demand: male myocytes scale output through greater mitochondrial mass, while female myocytes achieve energetic precision via enhanced sarcoplasmic reticulum-mitochondrial coupling.

摘要

未标记

每次心跳时离子运输和横桥循环对心室肌细胞造成的巨大能量需求是众所周知的,但ATP供需的时空动态仍知之甚少。在这里,我们使用共聚焦显微镜和靶向线粒体和细胞质的基因编码荧光传感器,可视化了成年雄性和雌性小鼠心室肌细胞逐搏的ATP动态变化。这些探针显示,每次收缩时线粒体ATP水平都会波动,揭示了两种不同的、空间定位的波形——ATP“增加”和ATP“下降”,分别代表基质ATP水平的瞬时增加或减少。这些波形与细胞内钙瞬变紧密锁相,并组织成能量微区。尽管雌性心肌细胞的局部线粒体ATP瞬变比雄性心肌细胞大,但其线粒体总体积较低。雌性心肌细胞在肌浆网和线粒体之间也表现出更紧密的耦合,并且每单位体积中显示出更高浓度的线粒体融合蛋白2和ATP合酶催化α亚基,表明ATP产生更有效。在雄性和雌性心肌细胞中,细胞质ATP瞬变反映了线粒体波形和区域结构。在更快的起搏过程中,雌性心肌细胞舒张期细胞质ATP上升更快,而伴随的逐搏锁定ATP瞬变在两性中均增加,但雄性增加的比例比雌性更大。这些发现表明,ATP是按需逐搏以模块化、微区特异性方式合成的。我们提出,雄性心肌细胞依靠更大的线粒体质量进行能量调节,而雌性细胞则利用结构精度来优化ATP传递。

关键点总结

众所周知,每次心跳都需要精确的ATP供应来为离子运输和横桥循环提供能量,但心脏细胞中ATP产生的时间和空间组织尚不清楚。使用先进的成像技术和基因编码传感器,我们可视化了单个雄性和雌性小鼠心室肌细胞线粒体和细胞质中逐搏的ATP波动。线粒体ATP水平在空间受限区域随每次心跳上升或下降,形成与钙瞬变同步的ATP“增加”或“下降”微区。在更高的发放频率下,逐搏锁定的舒张期ATP瞬变在雌性心肌细胞中上升更快,但在雄性心肌细胞中更大,突出了满足能量供应与收缩需求的不同性别特异性策略。心室肌细胞“量入为出”,按需产生刚好足够的ATP来为每次心跳提供能量。雄性和雌性心肌细胞采用不同策略来满足这一需求:雄性心肌细胞通过更大的线粒体质量来扩大输出,而雌性心肌细胞则通过增强肌浆网 - 线粒体耦合来实现能量精确性。

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