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From Molecular Classification to Targeted Therapeutics: The Changing Face of Systemic Therapy in Metastatic Gastroesophageal Cancer

机译:从分子分类到靶向治疗:转移性胃食管癌全身治疗的变化面貌

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Histological classification of adenocarcinoma or squamous cell carcinoma for esophageal cancer or using the Lauren classification for intestinal and diffuse type gastric cancer has limited clinical utility in the management of advanced disease. Germline mutations in E-cadherin (CDH1) or mismatch repair genes (Lynch syndrome) were identified many years ago but given their rarity, the identification of these molecular alterations does not substantially impact treatment in the advanced setting. Recent molecular profiling studies of upper GI tumors have added to our knowledge of the underlying biology but have not led to an alternative classification system which can guide clinician’s therapeutic decisions. Recently the Cancer Genome Atlas Research Network has proposed four subtypes of gastric cancer dividing tumors into those positive for Epstein-Barr virus, microsatellite unstable tumors, genomically stable tumors, and tumors with chromosomal instability. Unfortunately to date, many phase III clinical trials involving molecularly targeted agents have failed to meet their survival endpoints due to their use in unselected populations. Future clinical trials should utilize molecular profiling of individual tumors in order to determine the optimal use of targeted therapies in preselected patients.
机译:对于食道癌,腺癌或鳞状细胞癌的组织学分类,或对肠和弥漫型胃癌使用Lauren分类,在晚期疾病管理中的临床应用受到限制。 E-钙黏着蛋白(CDH1)或不匹配修复基因(Lynch综合征)的种系突变已在很多年前被发现,但是鉴于它们的稀有性,这些分子改变的识别对高龄患者的治疗没有实质性影响。最近关于上消化道肿瘤的分子谱研究增加了我们对基础生物学的知识,但并未导致替代分类系统指导临床医师的治疗决策。最近,癌症基因组图谱研究网络提出了四种胃癌亚型,将肿瘤分为对爱泼斯坦-巴尔病毒呈阳性的肿瘤,微卫星不稳定的肿瘤,基因组稳定的肿瘤和染色体不稳定的肿瘤。不幸的是,迄今为止,由于涉及分子靶向药物的许多III期临床试验均未在某些人群中使用,因此未能达到其生存终点。未来的临床试验应利用单个肿瘤的分子谱分析,以确定在预选患者中靶向治疗的最佳用途。

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