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首页> 外文期刊>Cancer letters >Anterior Gradient-2 monoclonal antibody inhibits lung cancer growth and metastasis by upregulating p53 pathway and without exerting any toxicological effects: A preclinical study
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Anterior Gradient-2 monoclonal antibody inhibits lung cancer growth and metastasis by upregulating p53 pathway and without exerting any toxicological effects: A preclinical study

机译:前梯度-2单克隆抗体通过上调P53途径抑制肺癌生长和转移,而不施加任何毒理学作用:临床前研究

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摘要

Increased drug resistance and acute side effects on normal organs are the major disadvantages of traditional cancer chemotherapy and radiotherapy. This has increased the focus on targeted therapeutic strategies such as monoclonal antibody-based cancer therapies. The major advantage of antibody-based therapies is the specific inhibition of cancer-related targets, with reduced off-target side effects. Anterior gradient-2 (AGR2) is a pro-metastatic and proangiogenic tumor marker that is overexpressed in multiple cancers. Therefore, anti-AGR2 antibodies may be potential therapeutic agents for treating different cancers. In the present study, we examined a novel anti-AGR2 monoclonal antibody mAb18A4 and found that this antibody inhibited lung cancer progression and metastasis without exerting any adverse side effects on the major organs and blood in mice. Moreover, we found that mAb18A4 activated p53 pathway and attenuated ERK1/2-MAPK pathway. Furthermore, mAb18A4-treated cancer cell lines showed attenuated proliferation and colony formation, enhanced apoptosis, increased p53 expression, and reduced phosphorylated ERK1/2 expression. Treatment with mAb18A4 significantly reduced tumor size and suppressed tumor metastasis in and increased the survival of different xenograft tumor models. In addition, mAb18A4 potently suppressed AGR2-induced angiogenesis. Results of pharmacokinetic and toxicological analyses confirmed the safety of mAb18A4 as an antitumor treatment.
机译:增加耐药性和对正常器官的急性副作用是传统癌症化疗和放射疗法的主要缺点。这增加了对靶向治疗策略的关注,例如单克隆抗体的基于单克隆抗体的癌症疗法。基于抗体的疗法的主要优点是癌症相关靶标的特异性抑制,减少了偏离目标副作用。前梯度-2(AGR2)是一种促癌患者在多种癌症中过表达的Pro-Metapatic和致胰肿瘤标志物。因此,抗Agr2抗体可以是用于治疗不同癌症的潜在治疗剂。在本研究中,我们研究了一种新型抗AGR2单克隆抗体MAB11A4,发现该抗体抑制了肺癌进展和转移,而不会对小鼠的主要器官和血液产生任何不良副作用。此外,我们发现MAB18A4活化的P53途径和减毒ERK1 / 2-MAPK途径。此外,MAB18A4处理的癌细胞系显示衰减的增殖和菌落形成,增强的凋亡,增加的P53表达,并降低磷酸化ERK1 / 2表达。用MAB18A4治疗显着降低肿瘤大小和抑制肿瘤转移并增加了不同异种移植肿瘤模型的存活率。此外,MAB18A4有效地抑制了AGR2诱导的血管生成。药代动力学和毒理学分析的结果证实了MAB18A4作为抗肿瘤治疗的安全性。

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