The Combination of Afatinib With Dasatinib or Miransertib Results in Synergistic Growth Inhibition of Stomach Cancer Cells.

IF 2.1 Q3 ONCOLOGY World Journal of Oncology Pub Date : 2024-04-01 Epub Date: 2024-03-21 DOI:10.14740/wjon1769
Tina Al-Janaby, Narmin Nahi, Alan Seddon, Izhar Bagwan, Said Khelwatty, Helmout Modjtahedi
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Abstract

Background: Of various human epidermal growth factor receptor (HER) inhibitors, only the anti-HER2 monoclonal antibody (mAb) Herceptin/trastuzumab and the antibody-drug conjugate trastuzumab deruxtecan (T-Dxd) has been approved for the treatment of patients with stomach cancer. However, the duration of response may be short in many patients, with tumor heterogeneity being one contributing factor.

Methods: We investigated the effect of various types of targeted agents on growth in vitro and migration of a panel of human stomach cancer cells (HSCCLs) and the impact of cell proliferation rate on the anti-tumor activities of these agents. We also investigated the association between the cell surface expression of the HER family members, hepatocyte growth factor receptor (c-Met), anaplastic lymphoma kinase (ALK)7 and cancer stem cell markers CD44 and CD133, and the response to the targeted agents.

Results: Of the 18 agents examined, the cyclin dependent kinase (CDK) 1/2/5/9 inhibitor dinaciclib was the most effective and inhibited the growth of all human HSCCLs at 50% inhibitory concentration (IC50) values between 9 nM to 23 nM. Of various HER inhibitors, the irreversible pan-HER family inhibitors (e.g., afatinib) were more effective than the reversible dual epidermal growth factor receptor (EGFR)/HER2 tyrosine kinase inhibitor (TKI) lapatinib and the EGFR-specific TKI erlotinib in inhibiting the growth of HSCCLs. Of agents targeting different downstream cell signaling molecules, dasatinib targeting Ab1/Src/C-Kit, trametinib targeting MERK1/2 and miransertib targeting AKT1/2/3 inhibited growth of majority of HSCCLs, with the IC50 values ranging from 2 nM to 7 µM. Many of these agents were more effective in inhibiting the growth of HSCCLs when they were proliferating at a slower rate. Treatment with neratinib, afatinib, dinaciclib, dasatinib, stattic, miransertib and paclitaxel significantly inhibited migration of stomach cancer cells. Interestingly, treatment with a combination of afatinib and dasatinib or afatinib and miransertib resulted in synergistic and additive growth inhibition of stomach cancer cells.

Conclusions: These results suggest that treatment with a combination of these agents may be of therapeutic value in stomach cancer and warrants further investigations.

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阿法替尼与达沙替尼或米兰色替尼联用可协同抑制胃癌细胞生长
背景:在各种人类表皮生长因子受体(HER)抑制剂中,只有抗HER2单克隆抗体(mAb)赫赛汀/曲妥珠单抗和抗体药物结合物曲妥珠单抗德鲁司坦(T-Dxd)已被批准用于治疗胃癌患者。然而,许多患者的反应持续时间可能很短,肿瘤异质性是其中一个原因:我们研究了各类靶向药物对一组人类胃癌细胞(HSCCLs)体外生长和迁移的影响,以及细胞增殖率对这些药物抗肿瘤活性的影响。我们还研究了HER家族成员、肝细胞生长因子受体(c-Met)、无性淋巴瘤激酶(ALK)7以及癌症干细胞标志物CD44和CD133的细胞表面表达与靶向药物反应之间的关联:在检测的18种药物中,细胞周期蛋白依赖性激酶(CDK)1/2/5/9抑制剂dinaciclib最有效,它能抑制所有人类HSCCL的生长,其50%抑制浓度(IC50)值在9 nM至23 nM之间。在各种HER抑制剂中,不可逆的泛HER家族抑制剂(如阿法替尼)比可逆的表皮生长因子受体(EGFR)/HER2双重酪氨酸激酶抑制剂(TKI)拉帕替尼和EGFR特异性TKI厄洛替尼更能有效抑制HSCCL的生长。在靶向不同下游细胞信号分子的药物中,靶向Ab1/Src/C-Kit的达沙替尼、靶向MERK1/2的曲美替尼和靶向AKT1/2/3的米兰色替尼抑制了大多数HSCCL的生长,IC50值从2 nM到7 µM不等。其中许多药物在HSCCL增殖速度较慢时抑制其生长的效果更好。neratinib、afatinib、dinaciclib、dasatinib、stattic、miransertib和紫杉醇能显著抑制胃癌细胞的迁移。有趣的是,阿法替尼和达沙替尼或阿法替尼和米兰色替尼联合治疗可协同和相加抑制胃癌细胞的生长:这些结果表明,这些药物的联合治疗可能对胃癌有治疗价值,值得进一步研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
6.10
自引率
15.40%
发文量
37
期刊介绍: World Journal of Oncology, bimonthly, publishes original contributions describing basic research and clinical investigation of cancer, on the cellular, molecular, prevention, diagnosis, therapy and prognosis aspects. The submissions can be basic research or clinical investigation oriented. This journal welcomes those submissions focused on the clinical trials of new treatment modalities for cancer, and those submissions focused on molecular or cellular research of the oncology pathogenesis. Case reports submitted for consideration of publication should explore either a novel genomic event/description or a new safety signal from an oncolytic agent. The areas of interested manuscripts are these disciplines: tumor immunology and immunotherapy; cancer molecular pharmacology and chemotherapy; drug sensitivity and resistance; cancer epidemiology; clinical trials; cancer pathology; radiobiology and radiation oncology; solid tumor oncology; hematological malignancies; surgical oncology; pediatric oncology; molecular oncology and cancer genes; gene therapy; cancer endocrinology; cancer metastasis; prevention and diagnosis of cancer; other cancer related subjects. The types of manuscripts accepted are original article, review, editorial, short communication, case report, letter to the editor, book review.
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