Division of Chemistry, Department of Medical Sciences, Faculty of Medicine, University of Miyazaki, 5200 Kihara, Kiyotake, Miyazaki, 889-1692, Japan.
Commun Biol. 2024 Jan 29;7(1):137. doi: 10.1038/s42003-024-05828-z.
In nucleotide expansion disorders, RNA foci are reportedly associated with neurodegenerative disease pathogeneses. Characteristically, these RNAs exhibit long poly-RNA repeats, such as 47 × CAG, 47 × CUG, or 29 × GGGGCC, usually becoming abnormal pathological aggregations above a critical number of nucleotide repeats. However, it remains unclear whether short, predominantly cellular RNA molecules can cause phase transitions to induce RNA foci. Herein, we demonstrated that short RNAs even with only two repeats can aggregate into a solid-like state via special RNA G-quadruplex structures. In human cells, these solid RNA foci could not dissolve even when using agents that disrupt RNA gelation. The aggregation of shorter RNAs can be clearly observed in vivo. Furthermore, we found that RNA foci induce colocalization of the RNA-binding protein Sam68, a protein commonly found in patients with fragile X-associated tremor/ataxia syndrome, suppressing cell clonogenicity and eventually causing cell death. Our results suggest that short RNA gelation promoted by specific RNA structures contribute to the neurological diseases, which disturb functional cellular processes.
在核苷酸扩展疾病中,据报道 RNA 焦点与神经退行性疾病的发病机制有关。这些 RNA 通常表现为长的多 RNA 重复序列,例如 47×CAG、47×CUG 或 29×GGGGCC,通常在核苷酸重复数超过临界值时成为异常病理性聚集。然而,目前尚不清楚短的、主要是细胞内的 RNA 分子是否可以引起相变诱导 RNA 焦点。在此,我们证明了即使只有两个重复的短 RNA 也可以通过特殊的 RNA G-四链体结构聚集到固态。在人类细胞中,即使使用破坏 RNA 胶凝的试剂,这些固态 RNA 焦点也不会溶解。在体内可以清楚地观察到较短 RNA 的聚集。此外,我们发现 RNA 焦点诱导 RNA 结合蛋白 Sam68 的共定位,Sam68 是脆性 X 相关震颤/共济失调综合征患者中常见的一种蛋白,抑制细胞集落形成能力,最终导致细胞死亡。我们的结果表明,特定 RNA 结构促进的短 RNA 凝胶化可能导致神经疾病,扰乱了正常的细胞功能过程。
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