Genetic Drivers of Pancreatic Cancer Are Identical Between the Primary Tumor and a Secondary Lesion in a Long-Term (>5 Years) Survivor After a Whipple Procedure.

Journal of Pancreatic Cancer Pub Date : 2018-11-01 eCollection Date: 2018-01-01 DOI:10.1089/pancan.2018.0015
Tyler M Bauer, Teena Dhir, Adam Strickland, Henry Thomsett, Austin B Goetz, Shawnna Cannaday, Jonathan R Brody, Michael J Pishvaian, Charles J Yeo
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引用次数: 4

Abstract

Background: A new mass in the remnant pancreas of a patient with previously resected pancreatic ductal adenocarcinoma (PDA) typically represents either a recurrence of the initial primary tumor or a second primary tumor. Recent advances in next-generation sequencing (NGS) strategies allow us to compare the genetic makeup of primary and secondary lesions. Case presentation: A 50-year-old Caucasian female presented for a surgical evaluation of a new biopsy-proven PDA at the junction of the body and tail of the pancreas. Six years prior, in 2011, the patient was found to have a T3N0M0 PDA of the pancreatic head, which was surgically resected with a classic Whipple procedure and concurrent hemicolectomy. Pathology showed pancreatic intraepithelial neoplasia grade 2 and PDA with negative surgical margins, positive perineural spread, and negative lymphovascular spread, and the patient received adjuvant chemotherapy and local radiation. In 2017, she was diagnosed with a new PDA lesion in the remaining pancreatic body far from the previous anastomosis site and was taken to surgery for a completion pancreatectomy and revision of the gastrojejunostomy. NGS was performed on both specimens. Both lesions shared identical mutations in KRAS, TP53, and CDKN2A genes. Amplifications of MYC and mutant KRAS were identified in the 2017 tumor and an ACVR1B mutation was identified in the 2011 tumor, but was not found in the 2017 tumor. Conclusions: This case demonstrates the ability to evaluate similarities between key genetic drivers from a resected primary tumor and a PDA lesion that presented in the same patient 6 years later. Histological analysis and NGS can be used to understand potential differences and similarities between lesions and may be useful in future studies as predictive markers or to provide insight into resistance mechanisms (e.g., MYC amplification).

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胰腺癌的遗传驱动因素在长期(>5年)惠普尔手术后的原发肿瘤和继发病变之间是相同的。
背景:先前切除的胰导管腺癌(PDA)患者的残余胰腺中出现新的肿块,通常代表最初的原发肿瘤复发或第二原发肿瘤。新一代测序(NGS)策略的最新进展使我们能够比较原发性和继发性病变的基因组成。病例介绍:一名50岁的白人女性,因在身体和胰腺尾部交界处发现新的活检证实的PDA而接受手术评估。6年前,也就是2011年,患者被发现胰腺头部有T3N0M0型PDA,并通过经典的惠普尔手术和同期结肠切除术进行了手术切除。病理显示胰腺上皮内瘤变2级,PDA伴手术切缘阴性,神经周围扩散阳性,淋巴血管扩散阴性,患者接受辅助化疗和局部放疗。2017年,她被诊断出在远离先前吻合部位的剩余胰腺体中出现新的PDA病变,并被送往手术进行完整胰腺切除术和胃空肠吻合术翻修。对两种标本均进行NGS检测。两种病变都有相同的KRAS、TP53和CDKN2A基因突变。在2017年的肿瘤中发现了MYC和突变KRAS的扩增,在2011年的肿瘤中发现了ACVR1B突变,但在2017年的肿瘤中未发现。结论:该病例证明了评估原发性切除肿瘤和同一患者6年后出现的PDA病变关键遗传驱动因素之间相似性的能力。组织学分析和NGS可用于了解病变之间的潜在差异和相似之处,并可能在未来的研究中作为预测标记物或提供耐药机制(例如,MYC扩增)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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