Garvan Institute of Medical Research & The Kinghorn Cancer Centre, Cancer Division, Sydney, New South Wales, Australia.
St Vincent's Clinical School, Faculty of Medicine, University of New South Wales, Sydney, New South Wales, Australia.
Gut. 2019 Apr;68(4):742-758. doi: 10.1136/gutjnl-2018-316822. Epub 2018 Nov 5.
Pancreatic ductal adenocarcinoma (PDAC) is among the most deadly solid tumours. This is due to a generally late-stage diagnosis of a primarily treatment-refractory disease. Several large-scale sequencing and mass spectrometry approaches have identified key drivers of this disease and in doing so highlighted the vast heterogeneity of lower frequency mutations that make clinical trials of targeted agents in unselected patients increasingly futile. There is a clear need for improved biomarkers to guide effective targeted therapies, with biomarker-driven clinical trials for personalised medicine becoming increasingly common in several cancers. Interestingly, many of the aberrant signalling pathways in PDAC rely on downstream signal transduction through the mitogen-activated protein kinase and phosphoinositide 3-kinase (PI3K) pathways, which has led to the development of several approaches to target these key regulators, primarily as combination therapies. The following review discusses the trend of PDAC therapy towards molecular subtyping for biomarker-driven personalised therapies, highlighting the key pathways under investigation and their relationship to the PI3K pathway.
胰腺导管腺癌 (PDAC) 是最致命的实体肿瘤之一。这主要是由于该病的诊断通常较晚,且主要对治疗具有抗性。几项大规模的测序和质谱分析方法已经确定了该疾病的关键驱动因素,同时也突出了低频率突变的巨大异质性,这使得针对未经选择的患者的靶向药物临床试验越来越没有效果。显然需要改进生物标志物来指导有效的靶向治疗,生物标志物驱动的个性化医学临床试验在多种癌症中越来越普遍。有趣的是,PDAC 中的许多异常信号通路依赖于丝裂原活化蛋白激酶和磷酸肌醇 3-激酶 (PI3K) 途径的下游信号转导,这导致了针对这些关键调节剂的几种方法的发展,主要是作为联合疗法。本文综述了 PDAC 治疗方法向基于分子亚型的生物标志物驱动的个体化治疗的趋势,强调了正在研究的关键途径及其与 PI3K 途径的关系。
