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阴离子通道视蛋白在抑制性心脏光遗传学中的应用。

Anion channelrhodopsins for inhibitory cardiac optogenetics.

机构信息

Center for Membrane Biology, Department of Biochemistry &Molecular Biology, University of Texas Health Science Center at Houston - McGovern Medical School, Houston, Texas, USA.

Department of Integrative Biology &Pharmacology, University of Texas Health Science Center at Houston - McGovern Medical School, Houston, Texas, USA.

出版信息

Sci Rep. 2016 Sep 15;6:33530. doi: 10.1038/srep33530.

Abstract

Optical control of the heart muscle is a promising strategy for cardiology because it is more specific than traditional electrical stimulation, and allows a higher temporal resolution than pharmacological interventions. Anion channelrhodopsins (ACRs) from cryptophyte algae expressed in cultured neonatal rat ventricular cardiomyocytes produced inhibitory currents at less than one-thousandth of the light intensity required by previously available optogenetic tools, such as the proton pump archaerhodopsin-3 (Arch). Because of their greater photocurrents, ACRs permitted complete inhibition of cardiomyocyte electrical activity under conditions in which Arch was inefficient. Most importantly, ACR expression allowed precisely controlled shortening of the action potential duration by switching on the light during its repolarization phase, which was not possible with previously used optogenetic tools. Optical shortening of cardiac action potentials may benefit pathophysiology research and the development of optogenetic treatments for cardiac disorders such as the long QT syndrome.

摘要

光学控制心肌是心脏病学中很有前途的策略,因为它比传统的电刺激更具特异性,并且比药理学干预具有更高的时间分辨率。在培养的新生大鼠心室心肌细胞中表达的隐藻蓝细菌来源的阴离子通道视紫红质(ACR)产生的抑制电流,所需的光强不到以前可用的光遗传学工具(如质子泵视紫红质-3(Arch))的千分之一。由于它们具有更大的光电流,因此在 Arch 效率低下的情况下,ACR 允许完全抑制心肌细胞的电活动。最重要的是,通过在复极化阶段打开光来表达 ACR,允许精确控制动作电位持续时间的缩短,这是以前使用的光遗传学工具所不可能的。心脏动作电位的光学缩短可能有益于病理生理学研究和开发用于心脏疾病(如长 QT 综合征)的光遗传学治疗方法。

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