Aspirin sensitizes osimertinib‐resistant NSCLC cells in?vitro and in?vivo via Bim‐dependent apoptosis induction

Rui Han; Shuai Hao; Conghua Lu; Chong Zhang; Caiyu Lin; Li Li; Yubo Wang; Chen Hu; Yong He

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Aspirin sensitizes osimertinib‐resistant NSCLC cells in?vitro and in?vivo via Bim‐dependent apoptosis induction

机译：阿司匹林通过BIM依赖性细胞凋亡诱导敏化口腔致致性的NSCLC细胞和体内抑制的细胞凋亡

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Osimertinib, a third‐generation irreversible epidermal growth factor receptor tyrosine kinase inhibitor (EGFR‐TKI), provides marked clinical benefit for patients with EGFR‐activating mutations. Unfortunately, limited treatments exist for patients who acquire osimertinib resistance. We observed two ‘special’ patients who regained an antitumor response with osimertinib plus aspirin treatment. As previous data indicate that aspirin induces antiproliferative effects in tumor cells, we designed a preclinical study to explore whether aspirin combined with osimertinib could synergistically sensitize osimertinib‐resistant non‐small‐cell lung cancer (NSCLC) cells. The effects of combined treatment with osimertinib and aspirin on osimertinib‐resistant NSCLC cell lines were examined in?vitro and in?vivo . The combination of osimertinib and aspirin induced strong antiproliferative and proapoptotic effects in osimertinib‐resistant NSCLC cells through inhibition of Akt/FoxO3a signaling component phosphorylation and increased Bim expression. Furthermore, Bim knockdown by siRNA significantly attenuated osimertinib resensitization by aspirin. In?vivo , combination of aspirin and osimertinib significantly decreased tumor growth of PC‐9GROR cell xenografts. Data of patients with NSCLC who received osimertinib treatment at Daping Hospital between January 2015 and January 2019 were reviewed retrospectively. According to clinical data for 45 patients with NSCLC, retrospective analysis showed that the median progression‐free survival was significantly longer in the osimertinib plus aspirin group than in the osimertinib group. In summary, aspirin synergistically enhances the antitumor activity of osimertinib in osimertinib‐resistant lung cancer cells through promoting Bim‐dependent apoptosis. This combination therapy may be effective in overcoming acquired resistance to osimertinib and prolonging survival in patients with NSCLC.

机译：Osimertinib，第三代不可逆表皮生长因子受体酪氨酸激酶抑制剂（EGFR-TKI）为EGFR活化突变的患者提供明显的临床益处。不幸的是，为获取Osimertinib抗性的患者存在有限的治疗方法。我们观察了两种“特殊”患者通过Osimertinib Plus Aspirin治疗恢复抗肿瘤反应。作为以前的数据表明阿司匹林诱导肿瘤细胞中的抗增殖作用，我们设计了一种临床前的研究，探讨阿司匹林是否与OSIMERTINIB联合可以协同敏感耐肺部抗性非小细胞肺癌（NSCLC）细胞。在β体外和体内检查与Osimertinib和阿司匹林组合治疗和阿司匹林对osimertinib抗性NSCLC细胞系的影响。通过抑制AKT / FOXO3A信号分量磷酸化和增加的BIM表达，Osimertinib和Aspirin的组合在Osimertinib抗性NMSCLC细胞中诱导了在Osimertinib抗性NMSCLC细胞中的强抗溶解效应。此外，SiRNA的BIM敲低显着减弱了阿司匹林的Osimertinib reszization。在α体内，阿司匹林和口莫特尼的组合显着降低了PC-9Gror细胞异种移植物的肿瘤生长。回顾性地审查了2015年1月至2019年1月至2019年1月在2019年1月至2019年1月期间接受Osimertinib治疗的NSCLC患者的数据。根据45例NSCLC患者的临床资料，回顾性分析表明，在OSIMERTINIB加阿司匹林组中，中位进展存活率比在Osimertinib组中显着更长。总之，阿司匹林通过促进BIM依赖性细胞凋亡协同增强Osimertinib抗性肺癌细胞中的Osimertinib的抗肿瘤活性。这种联合治疗可能有效地克服了对NSCLC患者的患者延长了患者的耐受性。

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《Molecular oncology. 》 |2020年第6期| 共18页
作者
Rui Han; Shuai Hao; Conghua Lu; Chong Zhang; Caiyu Lin; Li Li; Yubo Wang; Chen Hu; Yong He;
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apoptosisaspirinEGFR‐TKIosimertinibresistance;

机译：apoptiosaspirinegfr-tkiosimertinibribresistance.;

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机译：细胞周期蛋白依赖性激酶11（CDK11）是卵巢癌细胞体外和体内生长所必需的，其抑制作用导致细胞凋亡，并使细胞对紫杉醇敏感。
2. Phenylethanoid Glycosides from Cistanche tubulosa Inhibits the Growth of B16-F10 Cells both in Vitro and in Vivo by Induction of Apoptosis via Mitochondria-dependent Pathway [J] . Jinyu Li, Jinyao Li, Adila Aipire, Journal of Cancer . 2016 ,第13期

机译：肉Ci蓉中的苯乙醇类苷苷通过线粒体依赖性途径诱导细胞凋亡，从而抑制B16-F10细胞的体外和体内生长。
3. Lymphotoxin β receptor mediates caspase-dependent tumor cell apoptosis in vitro and tumor suppression in vivo despite induction of nf-κb activation [J] . HuX., ZimmermanM.A., BardhanK., Carcinogenesis . 2013 ,第5期

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4. Sensitization of human colorectal cancer cells to paclitaxel- induced apoptosis by inhibition of MEK/ERK pathway is caspase-4 dependent [C] . NIZAR M. MHAIDAT, SAIED A. JARADAT, ABDULHAMEED GHABKARI Recent researches in modern medicine . 2011

机译：通过抑制MEK / ERK途径使大肠癌细胞对紫杉醇诱导的细胞凋亡的敏感性取决于caspase-4
5. Autophagy induction in the quiescent state: In vitro and in vivo characterization of cellular self-cannibalism in quiescent cells. [D] . Haley, Erin Michelle. 2011

机译：处于静止状态的自噬诱导：静止细胞中细胞自相残杀的体外和体内表征。
6. Aspirin sensitizes osimertinib‐resistant NSCLC cells in vitro and in vivo via Bim‐dependent apoptosis induction [O] . Rui Han, Shuai Hao, Conghua Lu, 2020

机译：阿司匹林通过依赖Bim的凋亡诱导作用在体外和体内敏化对osimertinib耐药的NSCLC细胞
7. Aspirin sensitizes osimertinib‐resistant NSCLC cells in vitro and in vivo via Bim‐dependent apoptosis induction [O] . Rui Han, Shuai Hao, Conghua Lu, 2020

机译：阿司匹林通过BIM依赖性凋亡诱导在体外和体内敏感口腔抗性NMSCLC细胞敏化
8. Apoptosis-Dependent and Apoptosis-Independent Functions of Bim in Prostate Cancer Cells [R] . Tang, D. , Liu, J. 2005

机译：Bim在前列腺癌细胞中的凋亡依赖性和凋亡依赖性功能

Aspirin sensitizes osimertinib‐resistant NSCLC cells in?vitro and in?vivo via Bim‐dependent apoptosis induction

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