靶向 PLK1 治疗 TERT 启动子突变型肝细胞癌。

Therapeutic targeting of PLK1 in TERT promoter-mutant hepatocellular carcinoma.

机构信息

Department of Radiation Oncology, The First Affiliated Hospital, Sun Yat-sen University, Guangzhou, China.

Institute of Precision Medicine, The First Affiliated Hospital, Sun Yat-sen University, Guangzhou, China.

出版信息

Clin Transl Med. 2024 May;14(5):e1703. doi: 10.1002/ctm2.1703.

DOI:10.1002/ctm2.1703

PMID:38769666

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11106514/

Abstract

BACKGROUND

Hotspot mutations in the promoter of telomerase reverse transcriptase (TERT) gene are the most common genetic variants in hepatocellular carcinoma (HCC) and associated with poor prognosis of the disease. However, no drug was currently approved for treating TERT promoter mutation positive HCC patients. Here, we aim to explore the potential therapeutic strategy for targeting TERT promoter mutation in HCC.

METHODS

The Liver Cancer Model Repository database was used for screening potential drugs to selectively suppress the growth of TERT promoter mutant HCC cells. RNA-seq, CRISPR-Cas9 technology and siRNA transfection were performed for mechanistic studies. Cell counting kit-8 (CCK8) assay and the xenograft tumour models were used for cell growth detection in vitro and in vivo, respectively. Cell apoptosis and cell cycle arrest were analysed by Annexin V-FITC staining and/or propidium iodide staining.

RESULTS

PLK1 inhibitors were remarkably more sensitive to HCC cells harbouring TERT promoter mutation than wild-type cells in vitro and in vivo, which were diminished after TERT promoter mutation was edited to the wild-type nucleotide. Comparing the HCC cells with wild-type promoter of TERT, PLK1 inhibitors specifically downregulated Smad3 to regulate TERT for inducing apoptosis and G2/M arrest in TERT mutant HCC cells. Moreover, knockout of Smad3 counteracted the effects of PLK1 inhibitors in TERT mutant HCC cells. Finally, a cooperative effect of PLK1 and Smad3 inhibition was observed in TERT mutant cells.

CONCLUSIONS

PLK1 inhibition selectively suppressed the growth of TERT mutant HCC cells through Smad3, thus contributed to discover a novel therapeutic strategy to treat HCC patients harbouring TERT promoter mutations.

KEY POINTS

TERT promoter mutation confers sensitivity to PLK1 inhibitors in HCC. The selective growth inhibition of TERT mutant HCC cells induced by PLK1 inhibitor was mediated by Smad3. Combined inhibition of PLK1 and Smad3 showed a cooperative anti-tumor effect in TERT mutant HCC cells.

摘要

背景

端粒酶逆转录酶（TERT）基因启动子中的热点突变是肝细胞癌（HCC）中最常见的遗传变异，与疾病的预后不良相关。然而，目前尚无药物被批准用于治疗 TERT 启动子突变阳性 HCC 患者。在这里，我们旨在探索针对 HCC 中 TERT 启动子突变的潜在治疗策略。

方法

使用肝癌模型库数据库筛选出潜在的药物，以选择性抑制 TERT 启动子突变 HCC 细胞的生长。进行 RNA-seq、CRISPR-Cas9 技术和 siRNA 转染以进行机制研究。使用细胞计数试剂盒-8（CCK8）测定和异种移植肿瘤模型分别在体外和体内检测细胞生长。通过 Annexin V-FITC 染色和/或碘化丙啶染色分析细胞凋亡和细胞周期停滞。

结果

PLK1 抑制剂在体外和体内对携带 TERT 启动子突变的 HCC 细胞比对野生型细胞更为敏感，而在 TERT 启动子突变被编辑为野生型核苷酸后，这种敏感性降低。与具有野生型 TERT 启动子的 HCC 细胞相比，PLK1 抑制剂特异性地下调 Smad3 以调节 TERT，从而在 TERT 突变 HCC 细胞中诱导细胞凋亡和 G2/M 期阻滞。此外，在 TERT 突变 HCC 细胞中敲除 Smad3 可抵消 PLK1 抑制剂的作用。最后，在 TERT 突变细胞中观察到 PLK1 和 Smad3 抑制的协同作用。

结论

PLK1 抑制通过 Smad3 选择性地抑制 TERT 突变 HCC 细胞的生长，从而有助于发现一种治疗携带 TERT 启动子突变的 HCC 患者的新治疗策略。

关键点

TERT 启动子突变赋予 HCC 中 PLK1 抑制剂敏感性。PLK1 抑制剂诱导的 TERT 突变 HCC 细胞的选择性生长抑制是通过 Smad3 介导的。在 TERT 突变 HCC 细胞中，PLK1 和 Smad3 的联合抑制显示出协同的抗肿瘤作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff0e/11106514/1074364c861f/CTM2-14-e1703-g005.jpg

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靶向 PLK1 治疗 TERT 启动子突变型肝细胞癌。

Therapeutic targeting of PLK1 in TERT promoter-mutant hepatocellular carcinoma.

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSIONS

KEY POINTS

背景

方法

结果

结论

关键点

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