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首页> 外文期刊>Expert opinion on biological therapy >The immunocheckpoints in modern oncology: the next 15 years
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The immunocheckpoints in modern oncology: the next 15 years

机译:现代肿瘤学中的免疫检查点:未来15年

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摘要

The notion that the immune system can act as a key factor in controlling cancer cell proliferation and thus its stimulation may be an important resource for cancer therapy has long been known. Tumors can elude the immune system by deploying proteins that shut down the immune response by binding to specific surface receptors on immure cells. Several promising strategies have been designed to overcome cancer cells' ability to suppress the immune surveillance. Immune checkpoint molecules that block cytotoxic T-lymphocyte associated antigen-4 (ipilimumab) or the programmed death-1/programmed death-ligand 1 axis (i.e., nivolumab and pembrolizumab) promote antitumor immunity, reactivating T-cell proliferation and activity. This efficient strategy currently represents one of the major oncological breakthroughs, with impressive clinically durable responses observed in cancer patients, particularly in melanoma, renal cell carcinoma, NSCLC and more recently in bladder cancer patients. Fifteen years ago, we replaced the IL-2 and INF-alpha for molecular targeted therapies. Today, we believe that immune therapy will represent the future, perhaps as part of a combination of different therapeutic strategies that act synergistically in each tumor and individual patient.
机译:人们早就知道免疫系统可以作为控制癌细胞增殖的关键因素,因此其刺激可能是癌症治疗的重要资源的观点。肿瘤可以通过部署蛋白质来逃避免疫系统,该蛋白质通过与未成熟细胞上的特定表面受体结合而关闭免疫反应。已经设计了几种有希望的策略来克服癌细胞抑制免疫监视的能力。阻断细胞毒性T淋巴细胞相关抗原4(ipilimumab)或程序性死亡1 /程序性死亡配体1轴(即nivolumab和pembrolizumab)的免疫检查点分子可促进抗肿瘤免疫力,重新激活T细胞增殖和活性。该有效策略目前代表着主要的肿瘤学突破之一,在癌症患者中观察到令人印象深刻的临床持久反应,尤其是在黑色素瘤,肾细胞癌,NSCLC中,最近在膀胱癌患者中也观察到。十五年前,我们用IL-2和INF-alpha取代了分子靶向疗法。今天,我们相信免疫疗法将代表未来,也许是在每个肿瘤和个体患者中协同发挥作用的不同治疗策略的组合的一部分。

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