Department of Oncology, Sheba Medical Center, Tel HaShomer
Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel
J Natl Compr Canc Netw. 2017 Aug;15(8):1063-1069. doi: 10.6004/jnccn.2017.0133.
Pancreatic ductal adenocarcinoma (PDAC) has a dismal prognosis, with a 5-year survival rate of ≤7% across all stages. The limited success of conventional therapies for PDAC is at least partially attributable to its genetic heterogeneity. Precision targeting of known PDAC subtypes may positively affect the outcome of this disease. An important actionable subtype in this cancer is associated with DNA repair dysfunction, including cases with germline mutations. This subtype can be targeted by inhibitors of poly(ADP-ribose) polymerase (PARP). mutation-associated PDAC may be the first biomarker-driven subtype in this disease that can be successfully targeted. However, DNA repair defects can extend beyond the narrow spectrum of mutations in PDAC and are present in a large proportion of patients with familial PDAC. This review describes the subgroup of patients with PDAC with aberrant DNA repair and discusses diagnostic and therapeutic options.
胰腺导管腺癌 (PDAC) 预后极差,各期 5 年生存率均≤7%。传统 PDAC 治疗方法的有限成功至少部分归因于其遗传异质性。针对已知 PDAC 亚型的精准靶向治疗可能会对该疾病的结局产生积极影响。在这种癌症中,一个重要的可靶向治疗的亚型与 DNA 修复功能障碍相关,包括伴有种系突变的病例。该亚型可以被聚 ADP 核糖聚合酶 (PARP) 抑制剂靶向。与 突变相关的 PDAC 可能是这种疾病中首个可成功靶向的基于生物标志物的亚型。然而,DNA 修复缺陷的范围超出了 PDAC 中 突变的狭窄范围,并且存在于很大一部分有家族性 PDAC 的患者中。本综述描述了具有异常 DNA 修复的 PDAC 患者亚组,并讨论了诊断和治疗选择。
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