Combination screen in multi-cell type tumor spheroids reveals interaction between aryl hydrocarbon receptor antagonists and E1 ubiquitin-activating enzyme inhibitor

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-10-01 DOI:10.1016/j.slasd.2024.100186
Thomas S. Dexheimer , Nathan P. Coussens , Thomas Silvers , Eric M. Jones , Li Chen , Jianwen Fang , Joel Morris , Jeffrey A. Moscow , James H. Doroshow , Beverly A. Teicher
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Abstract

The aryl hydrocarbon receptor (AhR) is a ligand-activated transcription factor that regulates genes of drug transporters and metabolic enzymes to detoxify small molecule xenobiotics. It has a complex role in cancer biology, influencing both the progression and suppression of tumors by modulating malignant properties of tumor cells and anti-tumor immunity, depending on the specific tumor type and developmental stage. This has led to the discovery and development of selective AhR modulators, including BAY 2416964 which is currently in clinical trials. To identify small molecule anticancer agents that might be combined with AhR antagonists for cancer therapy, a high-throughput combination screen was performed using multi-cell type tumor spheroids grown from malignant cells, endothelial cells, and mesenchymal stem cells. The AhR selective antagonists BAY 2416964, GNF351, and CH-223191 were tested individually and in combination with twenty-five small molecule anticancer agents. As single agents, BAY 2416964 and CH-223191 showed minimal activity, whereas GNF351 reduced the viability of some spheroid models at concentrations greater than 1 µM. The activity of most combinations aligned well with the single agent activity of the combined agent, without apparent contributions from the AhR antagonist. All three AhR antagonists sensitized tumor spheroids to TAK-243, an E1 ubiquitin-activating enzyme inhibitor. These combinations were active in spheroids containing bladder, breast, ovary, kidney, pancreas, colon, and lung tumor cell lines. The AhR antagonists also potentiated pevonedistat, a selective inhibitor of the NEDD8-activating enzyme E1 regulatory subunit, in several tumor spheroid models. In contrast, the AhR antagonists did not enhance the cytotoxicity of the proteasome inhibitor bortezomib.
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在多细胞型肿瘤球体中进行联合筛选,发现芳基烃受体拮抗剂与 E1 泛素激活酶抑制剂之间存在相互作用:芳基烃受体拮抗剂药物组合。
芳基烃受体(AhR)是一种配体激活的转录因子,可调节药物转运体和代谢酶的基因,从而对小分子异生物体进行解毒。它在癌症生物学中发挥着复杂的作用,根据具体的肿瘤类型和发育阶段,通过调节肿瘤细胞的恶性特性和抗肿瘤免疫,影响肿瘤的发展和抑制。这导致了选择性 AhR 调节剂的发现和开发,包括目前正在进行临床试验的 BAY 2416964。为了找出可与 AhR 拮抗剂联合用于癌症治疗的小分子抗癌剂,研究人员利用恶性细胞、内皮细胞和间充质干细胞培育的多细胞型肿瘤球体进行了高通量联合筛选。测试了 AhR 选择性拮抗剂 BAY 2416964、GNF351 和 CH-223191 单独使用以及与 25 种小分子抗癌剂联合使用的情况。作为单药,BAY 2416964 和 CH-223191 的活性极低,而 GNF351 在浓度超过 1 µM 时会降低一些球状模型的存活率。大多数组合药剂的活性与单一药剂非常一致,没有明显的 AhR 拮抗剂的作用。所有三种 AhR 拮抗剂都能使肿瘤球体对 E1 泛素激活酶抑制剂 TAK-243 敏感。这些组合对含有膀胱、乳腺、卵巢、肾脏、胰腺、结肠和肺部肿瘤细胞系的球形体具有活性。AhR拮抗剂还能增强pevonedistat(一种NEDD8激活酶E1调节亚基的选择性抑制剂)在几种肿瘤球状模型中的作用。相比之下,AhR拮抗剂没有增强蛋白酶体抑制剂硼替佐米的细胞毒性。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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