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Immunotherapy for advanced gastric and esophageal cancer: preclinical rationale and ongoing clinical investigations

机译:晚期胃癌和食道癌的免疫治疗:临床前理论基础和正在进行的临床研究

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摘要

Gastric and esophageal cancers represent a major global cancer burden and novel approaches are needed. Despite recent improvements in outcomes with trastuzumab and ramucirumab the prognosis for advanced disease remains poor, with a median overall survival of 1 year. Comprehensive genomic characterization has defined molecular subgroups and potentially actionable genomic alterations, but the majority of patients do not yet benefit from molecularly directed therapies. Breakthroughs in immune checkpoint blockade have provided new therapeutic avenues in melanoma, and continue to expand into other tumor types, with ongoing investigations in gastrointestinal (GI) malignancies. The frequency of programmed death ligand 1 (PD-L1) overexpression, a putative response biomarker, approaches forty percent in gastric cancers. Translational studies and molecular classification suggest gastric and esophageal cancers are candidate malignancies for immune checkpoint inhibition trials and early clinical data is promising. Here we review the mechanisms, preclinical, and early clinical data supporting the role for immune checkpoint blockade in gastric and esophageal cancer.
机译:胃癌和食道癌代表了主要的全球癌症负担,需要新颖的方法。尽管最近使用曲妥珠单抗和雷莫昔单抗改善了预后,但晚期疾病的预后仍然很差,平均总生存期为1年。全面的基因组表征已定义了分子亚组和潜在可操作的基因组改变,但是大多数患者尚未从分子定向疗法中受益。免疫检查点封锁的突破为黑色素瘤提供了新的治疗途径,并且随着胃肠道(GI)恶性肿瘤的不断研究,其继续扩展到其他类型的肿瘤。在胃癌中,程序性死亡配体1(PD-L1)过表达(一种可能的应答生物标志物)的频率接近40%。转化研究和分子分类表明,胃癌和食道癌是免疫检查点抑制试验的候选恶性肿瘤,早期的临床数据很有希望。在这里,我们回顾了支持免疫检查点封锁在胃癌和食道癌中的作用的机制,临床前和早期临床数据。

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