Asakawa Kazuhide, Handa Hiroshi, Kawakami Koichi
National Institute of Genetics.
Tokyo Medical University.
Nihon Yakurigaku Zasshi. 2023;158(1):16-20. doi: 10.1254/fpj.22085.
TAR DNA-binding protein 43 (TDP-43) is an evolutionarily conserved RNA/DNA-binding protein that is nuclear-enriched in healthy cells, but deposited in the cytoplasm as aggregates in affected neurons in certain neurodegenerative diseases, including amyotrophic lateral sclerosis (ALS). We have previously developed an optogenetic TDP-43 variant (opTDP-43h) whose oligomerization status can be modulated via the CRY2olig tag, which self-assembles upon absorption of blue light. Illumination of zebrafish spinal motor neurons expressing opTDP-43h with a blue light triggers its cytoplasmic mislocalization, eventually leading to cytoplasmic deposition of opTDP-43h aggregates. Intriguingly, a light illumination-dependent transient opTDP-43 mislocalization can halt motor axon outgrowth, even in the absence of cytoplasmic deposition of opTDP-43 aggregates. These observations point toward an oligomerization-dependent, but aggregation-independent, cytotoxic effect of TDP-43 that might contribute to pathogenesis of ALS. In the present review, we would like to overview the zebrafish ALS model based on the optogenetic TDP-43, and then discuss about the potential mechanisms of TDP-43 cytotoxicity that trigger and/or promote motor neuron degeneration in ALS.
TAR DNA结合蛋白43(TDP - 43)是一种在进化上保守的RNA/DNA结合蛋白,在健康细胞中主要富集于细胞核,但在某些神经退行性疾病(包括肌萎缩侧索硬化症,即ALS)的受影响神经元中,会以聚集体的形式沉积在细胞质中。我们之前开发了一种光遗传学TDP - 43变体(opTDP - 43h),其寡聚化状态可通过CRY2olig标签进行调控,该标签在吸收蓝光后会自组装。用蓝光照射表达opTDP - 43h的斑马鱼脊髓运动神经元会触发其在细胞质中的错误定位,最终导致opTDP - 43h聚集体在细胞质中沉积。有趣的是,即使在没有opTDP - 43聚集体在细胞质中沉积的情况下,光照射依赖的短暂opTDP - 43错误定位也会阻止运动轴突生长。这些观察结果表明TDP - 43存在一种依赖寡聚化但不依赖聚集的细胞毒性作用,这可能有助于ALS的发病机制。在本综述中,我们将概述基于光遗传学TDP - 43的斑马鱼ALS模型,然后讨论触发和/或促进ALS中运动神经元变性的TDP - 43细胞毒性的潜在机制。
