The anticancer potential of the CLK kinases inhibitors 1C8 and GPS167 revealed by their impact on the epithelial-mesenchymal transition and the antiviral immune response.

Q2 Medicine Oncotarget Pub Date : 2024-05-16 DOI:10.18632/oncotarget.28585
Lulzim Shkreta, Johanne Toutant, Aurélie Delannoy, David Durantel, Anna Salvetti, Sophie Ehresmann, Martin Sauvageau, Julien A Delbrouck, Alice Gravel-Trudeau, Christian Comeau, Caroline Huard, Jasmin Coulombe-Huntington, Mike Tyers, David Grierson, Pierre-Luc Boudreault, Benoit Chabot
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Abstract

The diheteroarylamide-based compound 1C8 and the aminothiazole carboxamide-related compound GPS167 inhibit the CLK kinases, and affect the proliferation of a broad range of cancer cell lines. A chemogenomic screen previously performed with GPS167 revealed that the depletion of components associated with mitotic spindle assembly altered sensitivity to GPS167. Here, a similar screen performed with 1C8 also established the impact of components involved in mitotic spindle assembly. Accordingly, transcriptome analyses of cells treated with 1C8 and GPS167 indicated that the expression and RNA splicing of transcripts encoding mitotic spindle assembly components were affected. The functional relevance of the microtubule connection was confirmed by showing that subtoxic concentrations of drugs affecting mitotic spindle assembly increased sensitivity to GPS167. 1C8 and GPS167 impacted the expression and splicing of transcripts in pathways relevant to tumor progression, including MYC targets and the epithelial mesenchymal transition (EMT). Finally, 1C8 and GPS167 altered the expression and alternative splicing of transcripts involved in the antiviral immune response. Consistent with this observation, depleting the double-stranded RNA sensor DHX33 suppressed GPS167-mediated cytotoxicity on HCT116 cells. Our study uncovered molecular mechanisms through which 1C8 and GPS167 affect cancer cell proliferation as well as processes critical for metastasis.

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CLK 激酶抑制剂 1C8 和 GPS167 对上皮-间质转化和抗病毒免疫反应的影响揭示了它们的抗癌潜力。
二卤代芳基酰胺类化合物 1C8 和氨基噻唑羧酰胺相关化合物 GPS167 可抑制 CLK 激酶,并影响多种癌细胞株的增殖。之前对 GPS167 进行的化学基因组筛选显示,与有丝分裂纺锤体组装相关的成分的缺失会改变对 GPS167 的敏感性。在这里,用 1C8 进行的类似筛选也确定了参与有丝分裂纺锤体组装的成分的影响。因此,用 1C8 和 GPS167 处理的细胞的转录组分析表明,编码有丝分裂纺锤体组装成分的转录本的表达和 RNA 剪接受到了影响。影响有丝分裂纺锤体组装的药物的亚毒性浓度增加了对 GPS167 的敏感性,从而证实了微管连接的功能相关性。1C8和GPS167影响了与肿瘤进展相关的通路中转录本的表达和剪接,包括MYC靶标和上皮间质转化(EMT)。最后,1C8 和 GPS167 改变了参与抗病毒免疫反应的转录本的表达和替代剪接。与这一观察结果一致的是,消耗双链 RNA 传感器 DHX33 会抑制 GPS167 介导的对 HCT116 细胞的细胞毒性。我们的研究揭示了 1C8 和 GPS167 影响癌细胞增殖以及转移关键过程的分子机制。
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来源期刊
Oncotarget
Oncotarget Oncogenes-CELL BIOLOGY
CiteScore
6.60
自引率
0.00%
发文量
129
审稿时长
1.5 months
期刊介绍: Information not localized
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