Early onset esophageal adenocarcinoma: a distinct molecular entity?

A. Nistelrooij, Ronald van Marion, K. Biermann, M. Spaander, J. Lanschot, B. Wijnhoven, W. Dinjens, I. Lijnschoten, Marieke C.H. Hogenes
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引用次数: 10

Abstract

Esophageal adenocarcinoma (EAC) is typically diagnosed in elderly with a median age of 68 years. The incidence of EAC has been rising over the last decades, also among young adults. The aim of the study was to investigate whether early onset EAC is a distinct molecular entity. To identify early onset EACs, the nationwide network and registry of histo- and cytopathology in the Netherlands (PALGA) was searched. Twenty-eight tumors of patients aged ≤40 years were selected and matched with 27 tumors of patients aged ≥68 years. DNA was isolated from surgically resected specimen and sequenced on the Ion Torrent Personal Genome Machine with the Ion AmpliSeq Cancer Panel. No differences in mutational load between early onset and conventional EACs were observed (P=0.196). The most frequently mutated genes were TP53 (73%) and P16 (16%). Additional mutations in early onset EACs occurred exclusively in: APC, CDH1, CTNNB1, FGFR2, and STK11. In the conventional EACs additional mutations were exclusively identified in: ABL1, FBXW7, GNA11, GNAS, KRAS, MET, SMAD4, and VHL. Additional mutations besides TP53 and P16 seem to occur in different genes related to cell fate pathways for early onset EACs, while the additional mutations in conventional EACs are related to survival pathways.
早发性食管腺癌:一个独特的分子实体?
食管腺癌(EAC)通常在中位年龄为68岁的老年人中诊断出来。在过去的几十年里,EAC的发病率一直在上升,在年轻人中也是如此。该研究的目的是调查早发性EAC是否是一种独特的分子实体。为了确定早发性EACs,我们检索了荷兰的组织和细胞病理学全国网络和登记处(PALGA)。选取年龄≤40岁患者28例肿瘤与年龄≥68岁患者27例肿瘤进行配对。从手术切除的标本中分离DNA,并在Ion Torrent个人基因组机上与Ion AmpliSeq癌症面板进行测序。早发性EACs与常规EACs的突变负荷无差异(P=0.196)。最常见的突变基因是TP53(73%)和P16(16%)。早发性EACs的其他突变仅发生在APC、CDH1、CTNNB1、FGFR2和STK11中。在传统的EACs中,额外的突变只在:ABL1、FBXW7、GNA11、GNAS、KRAS、MET、SMAD4和VHL中被鉴定出来。除了TP53和P16外,其他突变似乎发生在与早发性EACs细胞命运途径相关的不同基因中,而常规EACs中额外的突变与生存途径有关。
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