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Molecular markers for gastric adenocarcinoma: an update.

机译:胃腺癌的分子标记:更新。

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Gastric cancer is the second most common cancer worldwide. Treatment of localized gastric cancer relies primarily on surgical intervention, although growing evidence suggests that the addition of chemoradiation may improve disease-free intervals and overall survival. In this regard, the current high rates of recurrence and subsequent poor survival have prompted an ever-increasing use of multimodal strategies, even for early-stage disease. However, these therapies are often limited by debilitating toxicities and varying degrees of response efficacy. As a result, pharmacogenomics, the study of specific genetic and molecular signatures that may be predictive of treatment outcomes, has gained considerable interest. For example, studies have demonstrated that the expression of enzymes involved in the metabolism or conjugation of commonly used chemotherapy agents, such as fluoropyrimidines and cisplatin, can serve as surrogate markers predictive of chemotherapy response. Polymorphisms in the genes encoding these enzymes have also been identified and may further account for altered expression patterns, resulting in varied clinical responses. Future work is necessary to further refine the list of molecular genetic markers and to identify novel markers for prognostic and predictive purposes. Technologies such as microarray analysis may be useful in identifying new molecular genetic markers, and further work may determine whether these markers can be employed to help stratify patients into different multimodal treatment regimens.
机译:胃癌是全球第二大最常见的癌症。局限性胃癌的治疗主要依靠外科手术干预,尽管越来越多的证据表明,化学放疗的加入可以改善无病间隔和总体生存期。在这方面,当前的高复发率和随后的低存活率促使人们甚至在早期疾病中也越来越多地采用多峰策略。但是,这些疗法通常受到使人衰弱的毒性和不同程度的反应功效的限制。结果,药物基因组学,即可以预测治疗结果的特定遗传和分子标志的研究,引起了人们的极大兴趣。例如,研究表明,与常用化疗药物(例如氟嘧啶和顺铂)的代谢或结合相关的酶的表达可作为预测化疗反应的替代标志物。还已经确定了编码这些酶的基因中的多态性,并可能进一步解释了表达模式的改变,从而导致了不同的临床反应。未来的工作对于进一步完善分子遗传标记的清单以及识别用于预后和预测目的的新标记是必要的。诸如微阵列分析之类的技术可能对识别新的分子遗传标记有用,进一步的工作可能确定这些标记是否可用于帮助将患者分为不同的多峰治疗方案。

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