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心房心肌细胞单层中转子的局部光遗传学靶向

Localized Optogenetic Targeting of Rotors in Atrial Cardiomyocyte Monolayers.

作者信息

Feola Iolanda, Volkers Linda, Majumder Rupamanjari, Teplenin Alexander, Schalij Martin J, Panfilov Alexander V, de Vries Antoine A F, Pijnappels Daniël A

机构信息

From the Laboratory of Experimental Cardiology, Department of Cardiology, Heart Lung Center Leiden, Leiden University Medical Center, The Netherlands (I.F., L.V., R.M., A.T., M.J.S., A.V.P., A.A.F.d.V., D.A.P.); and Department of Physics and Astronomy, Ghent University, Belgium (A.V.P.).

出版信息

Circ Arrhythm Electrophysiol. 2017 Nov;10(11). doi: 10.1161/CIRCEP.117.005591.

Abstract

BACKGROUND

Recently, a new ablation strategy for atrial fibrillation has emerged, which involves the identification of rotors (ie, local drivers) followed by the localized targeting of their core region by ablation. However, this concept has been subject to debate because the mode of arrhythmia termination remains poorly understood, as dedicated models and research tools are lacking. We took a unique optogenetic approach to induce and locally target a rotor in atrial monolayers.

METHODS AND RESULTS

Neonatal rat atrial cardiomyocyte monolayers expressing a depolarizing light-gated ion channel (Ca-translocating channelrhodopsin) were subjected to patterned illumination to induce single, stable, and centralized rotors by optical S1-S2 cross-field stimulation. Next, the core region of these rotors was specifically and precisely targeted by light to induce local conduction blocks of circular or linear shapes. Conduction blocks crossing the core region, but not reaching any unexcitable boundary, did not lead to termination. Instead, electric waves started to propagate along the circumference of block, thereby maintaining reentrant activity, although of lower frequency. If, however, core-spanning lines of block reached at least 1 unexcitable boundary, reentrant activity was consistently terminated by wave collision. Lines of block away from the core region resulted merely in rotor destabilization (ie, drifting).

CONCLUSIONS

Localized optogenetic targeting of rotors in atrial monolayers could lead to both stabilization and destabilization of reentrant activity. For termination, however, a line of block is required reaching from the core region to at least 1 unexcitable boundary. These findings may improve our understanding of the mechanisms involved in rotor-guided ablation.

摘要

背景

最近,一种用于心房颤动的新消融策略出现了,该策略涉及识别转子(即局部驱动因素),然后通过消融对其核心区域进行局部靶向。然而,这一概念一直存在争议,因为心律失常终止的模式仍知之甚少,缺乏专门的模型和研究工具。我们采用了一种独特的光遗传学方法,在心房单层中诱导并局部靶向一个转子。

方法与结果

对表达去极化光门控离子通道(钙转运通道视紫红质)的新生大鼠心房心肌细胞单层进行图案化光照,通过光学S1-S2交叉场刺激诱导单个、稳定且集中的转子。接下来,通过光对这些转子的核心区域进行特异性和精确靶向,以诱导圆形或线性的局部传导阻滞。穿过核心区域但未到达任何不可兴奋边界的传导阻滞不会导致终止。相反,电波开始沿着阻滞的圆周传播,从而维持折返活动,尽管频率较低。然而,如果跨越核心区域的阻滞线至少到达1个不可兴奋边界,折返活动会因波碰撞而持续终止。远离核心区域的阻滞线仅导致转子不稳定(即漂移)。

结论

在心房单层中对转子进行局部光遗传学靶向可导致折返活动的稳定和不稳定。然而,为了实现终止,需要一条从核心区域延伸至至少1个不可兴奋边界的阻滞线。这些发现可能会增进我们对转子引导消融所涉及机制的理解。

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