Zhang Ying, Ma Yan, Ji Yu-Ke, Jiang Yi-Fei, Li Duo, Mu Wan, Yao Mu-Di, Yao Jin, Yan Biao
The Affiliated Eye Hospital, Nanjing Medical University, Nanjing, 210000, China.
The Fourth School of Clinical Medicine, Nanjing Medical University, Nanjing, 210000, China.
Cell Commun Signal. 2025 Jan 10;23(1):18. doi: 10.1186/s12964-024-02013-x.
Ischemic retinopathies are the major causes of blindness, yet effective early-stage treatments remain limited due to an incomplete understanding of the underlying molecular mechanisms. Significant changes in gene expression often precede structural and functional alterations. Transfer RNA (tRNA)-derived small RNAs (tsRNAs) are emerging as novel gene regulators, involved in various biological processes and human diseases. In this study, tsRNA-Gln-i-0095 was identified as a novel regulator, which was significantly upregulated in retinal ischemia/reperfusion (I/R) injury. Reducing the levels of tsRNA-Gln-i-0095 suppressed reactive gliosis, lowered inflammatory cytokine levels, and protected retinal ganglion cells from I/R injury. These effects led to reduced structural and functional damage, inhibited glial activation and inflammation, and enhanced neuronal function. Mechanistically, tsRNA-Gln-i-0095 downregulated the expression of NFIA and TGFBR2 through a miRNA-like mechanism. Collectively, this study highlights the potential of targeting tsRNA-Gln-i-0095 as a novel therapeutic approach to reduce retinal I/R injury and preserve visual function.
缺血性视网膜病变是失明的主要原因,但由于对潜在分子机制的不完全理解,有效的早期治疗方法仍然有限。基因表达的显著变化通常先于结构和功能改变。转运RNA(tRNA)衍生的小RNA(tsRNAs)正成为新型基因调节剂,参与各种生物过程和人类疾病。在本研究中,tsRNA-Gln-i-0095被鉴定为一种新型调节剂,在视网膜缺血/再灌注(I/R)损伤中显著上调。降低tsRNA-Gln-i-0095的水平可抑制反应性胶质增生,降低炎性细胞因子水平,并保护视网膜神经节细胞免受I/R损伤。这些作用导致结构和功能损伤减轻,胶质细胞活化和炎症受到抑制,神经元功能增强。机制上,tsRNA-Gln-i-0095通过类似miRNA的机制下调NFIA和TGFBR2的表达。总的来说,本研究突出了以tsRNA-Gln-i-0095为靶点作为减少视网膜I/R损伤和保护视觉功能的新型治疗方法的潜力。
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