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利用光驱动外向质子泵视紫红质-3 引发的光触发细胞凋亡(PTA)

Phototriggered Apoptotic Cell Death (PTA) Using the Light-Driven Outward Proton Pump Rhodopsin Archaerhodopsin-3.

机构信息

Division of Pharmaceutical Sciences, Okayama University, Okayama 700-8530, Japan.

Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, Okayama University, Okayama 700-8530, Japan.

出版信息

J Am Chem Soc. 2022 Mar 9;144(9):3771-3775. doi: 10.1021/jacs.1c12608. Epub 2022 Feb 17.

Abstract

Apoptosis is a type of programmed cell death that commonly occurs in multicellular organisms including humans and that is essential to eliminate unnecessary cells to keep organisms healthy. Indeed, inappropriate apoptosis leads to various diseases such as cancer and autoimmune disease. Here, we developed an optical method to regulate apoptotic cell death by controlling the intracellular pH with outward or inward proton pump rhodopsins, Archaerhodopsin-3 (AR3) or xenorhodopsin (XeR), respectively. The alkalization-induced shrinking of human HeLa cells cultured at pH 9.0 was significantly accelerated or decelerated by light-activated AR3 or XeR, respectively, implying the contribution of intracellular alkalization to the cell death. The light-activated AR3 induced cell shrinking at a physiologically neutral pH 7.4 and biochemical analysis revealed that the intracellular alkalization caused by AR3 triggered the mitochondrial apoptotic signaling pathway, which resulted in cell death accompanied by morphological changes. Phototriggered apoptosis (PTA) was also observed for other human cell lines, SH-SY5Y and A549 cells, implying its general applicability. We then used the PTA method with the nematode as a model for living animals. Irradiation of transgenic worms expressing AR3 in chemosensing amphid sensory neurons significantly decreased their chemotaxis responses, which suggests that AR3 induced the cell death of amphid sensory neurons and the depression of chemotaxis responses. Thus, the PTA method has a high applicability both and , which suggests its potential as an optogenetic tool to selectively eliminate target cells with a high spatiotemporal resolution.

摘要

细胞凋亡是一种普遍存在于包括人类在内的多细胞生物中的程序性细胞死亡方式,对于清除不必要的细胞以保持生物体健康至关重要。事实上,不合适的细胞凋亡会导致各种疾病,如癌症和自身免疫性疾病。在这里,我们开发了一种光学方法,通过控制细胞内的 pH 值来调节细胞凋亡,分别使用向外质子泵视紫红质(Archaerhodopsin-3,AR3)或内向质子泵视紫红质(xenorhodopsin,XeR)。在 pH 值为 9.0 的条件下培养的人宫颈癌细胞(HeLa)的碱化诱导收缩分别被光激活的 AR3 或 XeR 显著加速或减速,这表明细胞内碱化对细胞死亡有贡献。光激活的 AR3 在生理中性 pH 值 7.4 下诱导细胞收缩,生化分析表明,AR3 引起的细胞内碱化触发了线粒体凋亡信号通路,导致细胞死亡,并伴有形态变化。其他人类细胞系 SH-SY5Y 和 A549 也观察到了光触发的细胞凋亡(PTA),这表明其具有普遍性。然后,我们使用 PTA 方法对作为活体动物模型的线虫进行了研究。在化学感应触角感觉神经元中表达 AR3 的转基因线虫的照射显著降低了它们的趋化反应,这表明 AR3 诱导了触角感觉神经元的细胞死亡和趋化反应的抑制。因此,PTA 方法具有高度的适用性,可用于选择性地以高时空分辨率消除靶细胞,这表明其作为光遗传学工具的潜力。

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