Qi Qianyi, Chen Bairong, Wu Jinran, Xu Jing, Bao Hongyi, Jin Kangfeng, Chen Lin, Zhu Guang, Wang Feng
Research Center of Clinical Medicine, Affiliated Hospital of Nantong University, Medical School of Nantong University, Nantong, China.
Department of Laboratory Medicine, Affiliated Hospital of Nantong University, Medical School of Nantong University, Nantong, China.
Ann Med. 2025 Dec;57(1):2531253. doi: 10.1080/07853890.2025.2531253. Epub 2025 Jul 13.
tRNA-derived small RNAs (tsRNAs), newly developed non-coding RNAs with specialized biological features, are aberrantly expressed in the majority of malignancies. However, whether tsRNAs are involved in metabolic reprogramming of colorectal cancer (CRC) remains to be elucidated.
A novel tsRNA, tsRNA-Ser-3-0072 (tsR-0072), was screened from the tsRFun database and its expression was characterized by real-time quantitative PCR (qRT-PCR). CCK8, 5-ethynyl-2'-deoxyuridine (EdU), colony formation, transwell experiments and nude mice transplantation models were performed to assess CRC cell proliferation and metastasis and . The target genes of tsR-0072 were verified using a dual luciferase reporter assay, and enzyme-linked immunosorbent assay (ELISA), Western blotting, and qRT-PCR were employed to analyse the potential mechanisms of CRC.
TsR-0072 was downregulated in CRC and was found to be associated with TNM stage, T stage, lymph node metastasis and the prognosis of CRC patients. Functional experiments revealed that tsR-0072 inhibited CRC growth and metastasis both and . Moreover, sterol O-acyltransferase 1 (SOAT1) and 25-hydroxyvitamin D-24-hydroxylase (CYP24A1) were identified as direct targets of tsR-0072. Mechanistic studies revealed that tsR-0072 arrested lipid metabolism by downregulating the expression of SOAT1, which inhibited the activity of sterol regulatory element-binding protein 1 (SREBP1), sterol regulatory element-binding protein 2 (SREBP2) and fatty acid synthase (FASN). In addition, tsR-0072 promoted vitamin D metabolism by decreasing the expression of CYP24A1, thereby increasing 1α,25-dihydroxyvitamin D (1,25(OH)D) secretion and vitamin D receptor (VDR) expression. Both lipid and vitamin D metabolic reprogramming induced by tsR-0072 resulted in inhibition of CRC progression through inactivation of the Wnt/β-catenin signalling pathway.
TsR-0072 acted as an anti-oncogene to modulate lipid and vitamin D metabolic reprogramming, thereby impeding CRC progression. Consequently, it might be a potential therapeutic target to overcome metabolic disorders in tumours. This study provided a promising transfer RNA (tRNA)-oriented strategy for the treatment of CRC treatment.
tRNA衍生的小RNA(tsRNAs)是新发现的具有特殊生物学特性的非编码RNA,在大多数恶性肿瘤中异常表达。然而,tsRNAs是否参与结直肠癌(CRC)的代谢重编程仍有待阐明。
从tsRFun数据库中筛选出一种新的tsRNA,即tsRNA-Ser-3-0072(tsR-0072),并通过实时定量PCR(qRT-PCR)对其表达进行表征。进行CCK8、5-乙炔基-2'-脱氧尿苷(EdU)、集落形成、Transwell实验和裸鼠移植模型,以评估CRC细胞的增殖和转移。使用双荧光素酶报告基因检测验证tsR-0072的靶基因,并采用酶联免疫吸附测定(ELISA)、蛋白质印迹法和qRT-PCR分析CRC的潜在机制。
tsR-0072在CRC中表达下调,且发现其与TNM分期、T分期、淋巴结转移及CRC患者的预后相关。功能实验表明,tsR-0072在体内和体外均抑制CRC的生长和转移。此外,固醇O-酰基转移酶1(SOAT1)和25-羟基维生素D-24-羟化酶(CYP24A1)被确定为tsR-0072的直接靶标。机制研究表明,tsR-0072通过下调SOAT1的表达来阻止脂质代谢,从而抑制固醇调节元件结合蛋白1(SREBP1)、固醇调节元件结合蛋白2(SREBP2)和脂肪酸合酶(FASN)的活性。此外,tsR-0072通过降低CYP24A1的表达促进维生素D代谢,从而增加1α,25-二羟基维生素D(1,25(OH)D)的分泌和维生素D受体(VDR)的表达。tsR-0072诱导的脂质和维生素D代谢重编程均通过Wnt/β-连环蛋白信号通路的失活导致CRC进展受到抑制。
tsR-0072作为一种抑癌基因,调节脂质和维生素D代谢重编程,从而阻碍CRC进展。因此,它可能是克服肿瘤代谢紊乱的潜在治疗靶点。本研究为CRC治疗提供了一种有前景的以转运RNA(tRNA)为导向的策略。
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