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RNA加工激酶抑制剂和表观遗传抑制剂与肿瘤药物或研究性药物联合用于多细胞类型患者来源的肿瘤细胞系球体。

RNA processing kinase inhibitors and epigenetic inhibitors in combination with oncology drugs or investigational agents in multi-cell type patient-derived tumor cell line spheroids.

作者信息

Teicher Beverly A, Dexheimer Thomas S, Silvers Thomas, Coussens Nathan P, Jones Eric, Gore Steven D, Kunkel Mark, Doroshow James H

机构信息

National Cancer Institute.

Frederick National Laboratory for Cancer Research.

出版信息

Res Sq. 2025 May 15:rs.3.rs-6602839. doi: 10.21203/rs.3.rs-6602839/v1.

DOI:10.21203/rs.3.rs-6602839/v1
PMID:40470182
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12136186/
Abstract

The alternative splicing of mRNA precursors allows one gene to yield multiple proteins with distinct functions. CDC-like kinases (CLKs) serve as pivotal regulators of alternative splicing. Control of protein expression also occurs at the level of DNA through histone methylation and demethylation. We investigated the activity of two CLK inhibitors, cirtuvivint and CC-671, and the LSD1 inhibitor iadademstat alone and in combination with anticancer drugs or investigational agents. Well-characterized patient-derived cancer cell lines from the PDMR (https://pdmr.cancer.gov/models/database.htm) were used along with standard human cancer cell lines. Multi-cell type (mct) tumor spheroids were grown from a ratio of 6:2.5:1.5 malignant cells, endothelial cells, and mesenchymal stem cells. Following three days of growth, the spheroids were exposed to the single agents or combinations at concentrations up to the clinical C value for each agent, if known. After seven days of exposure, cell viability was assessed using the CellTiter-Glo 3D assay and spheroid volume was assessed by bright field imaging. Several of the targeted oncology drugs exhibited additive and greater-than-additive cytotoxicity when combined with a CLK inhibitor, or the LSD1 inhibitor. These agents included the XPO1 inhibitor, eltanexor, and the KRAS G12D specific inhibitor MRTX-1133 which had activity in tumor lines harboring the KRAS G12D mutation. LSD1 inhibition was effective with ubiquitin proteasome pathway inhibitors. The full data sets are available on PubChem.

摘要

mRNA前体的可变剪接使得一个基因能够产生多种具有不同功能的蛋白质。类细胞周期蛋白依赖性激酶(CLKs)作为可变剪接的关键调节因子。蛋白质表达的控制也通过组蛋白甲基化和去甲基化在DNA水平上发生。我们研究了两种CLK抑制剂cirtuvivint和CC - 671以及LSD1抑制剂iadademstat单独使用以及与抗癌药物或研究药物联合使用时的活性。使用了来自PDMR(https://pdmr.cancer.gov/models/database.htm)的特征明确的患者来源癌细胞系以及标准人类癌细胞系。多细胞类型(mct)肿瘤球体由恶性细胞、内皮细胞和间充质干细胞以6:2.5:1.5的比例培养而成。培养三天后,将球体暴露于单一药物或组合药物中,浓度最高可达每种药物已知的临床C值。暴露七天后,使用CellTiter - Glo 3D测定法评估细胞活力,并通过明场成像评估球体体积。几种靶向肿瘤药物与CLK抑制剂或LSD1抑制剂联合使用时表现出相加及大于相加的细胞毒性。这些药物包括XPO1抑制剂eltanexor和KRAS G12D特异性抑制剂MRTX - 1133,后者在携带KRAS G12D突变的肿瘤细胞系中具有活性。LSD1抑制与泛素蛋白酶体途径抑制剂联合有效。完整的数据集可在PubChem上获取。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22dc/12136186/a6b1f331e015/nihpp-rs6602839v1-f0007.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22dc/12136186/a6b1f331e015/nihpp-rs6602839v1-f0007.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22dc/12136186/26e8a7a5a595/nihpp-rs6602839v1-f0001.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22dc/12136186/390f49e9054f/nihpp-rs6602839v1-f0005.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22dc/12136186/ac3abe2b7296/nihpp-rs6602839v1-f0006.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22dc/12136186/a6b1f331e015/nihpp-rs6602839v1-f0007.jpg

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