Antitumor and off-target effects of cholesterol-conjugated let-7a mimics in an orthotopic hepatocellular carcinoma xenograft nude mouse model.

Q4 Biochemistry, Genetics and Molecular Biology Journal of BioX Research Pub Date : 2022-12-01 DOI:10.1097/JBR.0000000000000103
Jian Guan, Mingyang Liu, Xin Li, Liangrui Zhou, Xueyu Dong, Wei Dai, Yu Xia, Tao Yang, Shaojuan Guo, Xingqi Li, Yehua Han, Yufeng Luo
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Abstract

To explore the antitumor and potential off-target effects of systemically delivered cholesterol-conjugated let-7a mimics (Chol-let-7a) and control mimics (Chol-miRCtrl) on hepatocellular carcinoma in vivo.

Methods: The antitumor effects of two intravenous dosing regimens of Chol-let-7a on heptocellular carcinoma growth were compared using an orthotopic xenograft mouse model. Off-targets were analyzed with histopathological and ultrapathological features of heparenal tissue and cells in the Chol-let-7a-, Chol-miRCtrl-, and saline-treated (blank) xenograft mice and normal control mice. Then, let-7a abundance in orthotopic tumors, corresponding paracancerous hepatic tissue, and normal liver tissue from healthy nude mice was examined by reverse transcription-polymerase chain reaction. The distribution of Chol-let-7a and Chol-miRCtrl in vivo was examined by whole-animal imaging and frozen-sections observation. The experiments were approved by the Institutional Research Board of Peking Union Medical College Hospital.

Results: Continuous treatment with Chol-let-7a resulted in tumors that were 35.86% and 40.02% the size of those in the Chol-miRCtrl and blank xenograft group (P < 0.01 and P < 0.01, respectively), while intermittent dosing with Chol-let-7a resulted in tumors that were 65.42% and 56.66% the size of those in the Chol-miRCtrl and the blank control group, respectively (P < 0.05 and P < 0.05). In addition, some histopathological and ultrapathological features were only observed after treatment with the two cholesterol-conjugated molecules, however mild with intermittent dosing Chol-let-7a treatment, such as diffuse sinusoidal dilation and edema, primarily around the centrolobular vein in heptic tissues; mild hypercellularity with dilated capillary lumens in the renal tissue; and some organelle abnormalities found in heptic and renal cells. Furthermore, whole-animal imaging showed that Chol-let-7a and Chol-miRCtrl were predominantly distributed in the liver, kidney, and bladder regions after injection, and that the concentration of Chol-let-7a and Chol-miRCtrl in the kidney and the bladder decreased much slowly in the xenograft animals, especially in the Chol-miRCtrl group. Finally, RT-PCR analysis showed that let-7a levels were significantly increased in Chol-let-7a-treated xenografts compared with Chol-miRCtrl group (P=0.003) and blank xenograft group (P=0.001); however, the level was only equivalent to 50.6% and 40.7% of that in paracancerous hepatic tissue and hepatic tissue in normal mice, respectively.

Conclusions: Chol-let-7a, administered either continuously or intermittently, showed effective antitumor efficacy. Chol-let-7a had some off-target effects, such as mild acute hepatitis-like inflammation and non-specific drug-induced kidney injury. The intermittent dosing regimen resulted in less damage than the continuous regimen, while maintaining relatively satisfactory antitumor efficacy, which could be useful for the investigation and possible clinical use of miRNA treatment regimens in the future.

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胆固醇缀合let-7a模拟物在原位肝癌异种移植裸鼠模型中的抗肿瘤和脱靶作用
探讨系统给药的胆固醇共轭let-7a模拟物(choll -let-7a)和对照模拟物(choll - mirctrl)在体内对肝癌的抗肿瘤和潜在脱靶作用。方法:采用同种异种移植小鼠肝细胞癌模型,比较两种静脉给药方案对肝癌生长的抑制作用。用组织病理学和超病理学特征分析了脱靶的胆-let-7a-、胆- mirctrl -和盐处理(空白)异种移植小鼠和正常对照小鼠的肝脏组织和细胞。然后用逆转录聚合酶链反应检测健康裸鼠原位肿瘤、相应癌旁肝组织和正常肝组织中let-7a的丰度。采用全动物成像和冷冻切片观察胆-let-7a和胆- mirctrl在体内的分布。本实验经北京协和医院机构研究委员会批准。结果:连续给药的胆-let-7a肿瘤大小分别为胆- mirctrl组和空白异种移植组的35.86%和40.02% (P < 0.01和P < 0.01),间歇给药的胆-let-7a肿瘤大小分别为胆- mirctrl组和空白对照组的65.42%和56.66% (P < 0.05和P < 0.05)。此外,一些组织病理学和超病理学特征仅在两种胆固醇共轭分子治疗后观察到,而间歇性给药的chollet -7a治疗轻微,如弥漫性窦状静脉扩张和水肿,主要是在肝组织的小叶中央静脉周围;肾组织轻度细胞增多伴毛细血管管腔扩张;在肝和肾细胞中发现一些细胞器异常。此外,全动物成像显示,注射后胆碱-let-7a和胆碱- mirctrl主要分布在肝脏、肾脏和膀胱区域,并且在异种移植动物肾脏和膀胱中胆碱-let-7a和胆碱- mirctrl浓度下降非常缓慢,尤其是在胆碱- mirctrl组。最后,RT-PCR分析显示,与cl - mirctrl组(P=0.003)和空白异种移植物组(P=0.001)相比,cl -let-7a处理的异种移植物中let-7a水平显著升高;但其含量仅相当于正常小鼠癌旁肝组织和肝组织的50.6%和40.7%。结论:连续或间歇给药胆-let-7a均具有良好的抗肿瘤作用。choll -let-7a有一些脱靶效应,如轻度急性肝炎样炎症和非特异性药物性肾损伤。与连续给药方案相比,间歇给药方案的损伤更小,同时保持了相对满意的抗肿瘤效果,这对未来miRNA治疗方案的研究和可能的临床应用有帮助。
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发文量
105
审稿时长
10 weeks
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Antitumor and off-target effects of cholesterol-conjugated let-7a mimics in an orthotopic hepatocellular carcinoma xenograft nude mouse model. Thrombosis after SARS-CoV2 infection or COVID-19 vaccination: will a nonpathologic anti-PF4 antibody be a solution?-A narrative review. Corrigendum: In vivo detection of metabolic 2H-incorporation upon ingestion of 2H2O. Corrigendum: PA1426 regulates Pseudomonas aeruginosa quorum sensing and virulence: an in vitro study. The novel coronavirus and humans: who can dominate who?
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