GNAS和KRAS突变在导管内乳头状黏液性肿瘤相关癌中定义了不同的进展途径。
GNAS and KRAS Mutations Define Separate Progression Pathways in Intraductal Papillary Mucinous Neoplasm-Associated Carcinoma.
作者信息
Tan Marcus C, Basturk Olca, Brannon A Rose, Bhanot Umesh, Scott Sasinya N, Bouvier Nancy, LaFemina Jennifer, Jarnagin William R, Berger Michael F, Klimstra David, Allen Peter J
机构信息
Department of Surgery, Memorial Sloan-Kettering Cancer Center, New York, NY.
Department of Pathology, Memorial Sloan-Kettering Cancer Center, New York, NY.
出版信息
J Am Coll Surg. 2015 May;220(5):845-854.e1. doi: 10.1016/j.jamcollsurg.2014.11.029. Epub 2015 Feb 11.
BACKGROUND
Intraductal papillary mucinous neoplasms (IPMN) are being increasingly recognized as important precursors to pancreatic adenocarcinoma. Elucidation of the genetic changes underlying IPMN carcinogenesis may improve the diagnosis and management of IPMN. We sought to determine whether different histologic subtypes of IPMN would exhibit different frequencies of specific genetic mutations.
STUDY DESIGN
Patients with resected IPMN-associated invasive carcinoma (IPMN-INV) between 1997 and 2012 were reviewed. Areas of carcinoma, high-grade dysplasia, and low-grade dysplasia were micro-dissected from each pathologic specimen. Targeted, massively parallel sequencing was then performed on a panel of 275 genes (including KRAS, GNAS, and RNF43).
RESULTS
Thirty-eight patients with resected IPMN-INV and sufficient tissue for micro-dissection were identified. Median follow-up was 2.6 years. Mutations in GNAS were more prevalent in colloid-type IPMN-INV than tubular-type IPMN-INV (89% vs 32% respectively; p = 0.0003). Conversely, KRAS mutations were more prevalent in tubular-type than colloid-type IPMN-INV (89% vs 52%, respectively; p = 0.01). For noninvasive IPMN subtypes, GNAS mutations were more prevalent in intestinal (74%) compared with pancreatobiliary (31%) and gastric (50%) subtypes (p = 0.02). The presence of these mutations did not vary according to the degree of dysplasia (GNAS: invasive 61%, high-grade 59%, low-grade 53%; KRAS: invasive 71%, high-grade 62%, low-grade 74%), suggesting that mutations in these genes occur early in IPMN carcinogenesis.
CONCLUSIONS
Colloid carcinoma associated with IPMN and its intestinal-type preinvasive precursor are associated with high frequencies of GNAS mutations. The mutation profile of tubular carcinoma resembles that of conventional pancreatic adenocarcinoma. Preoperative determination of mutational status may assist with clinical treatment decisions.
背景
导管内乳头状黏液性肿瘤(IPMN)越来越被认为是胰腺腺癌的重要前体。阐明IPMN致癌作用背后的基因变化可能会改善IPMN的诊断和管理。我们试图确定IPMN的不同组织学亚型是否会表现出不同频率的特定基因突变。
研究设计
回顾了1997年至2012年间接受切除的IPMN相关浸润性癌(IPMN-INV)患者。从每个病理标本中显微切割出癌灶、高级别异型增生和低级别异型增生区域。然后对一组275个基因(包括KRAS、GNAS和RNF43)进行靶向大规模平行测序。
结果
确定了38例接受切除的IPMN-INV且有足够组织进行显微切割的患者。中位随访时间为2.6年。GNAS突变在胶样型IPMN-INV中比管状型IPMN-INV更常见(分别为89%和32%;p = 0.0003)。相反,KRAS突变在管状型IPMN-INV中比胶样型更常见(分别为89%和52%;p = 0.01)。对于非浸润性IPMN亚型,GNAS突变在肠型(74%)中比胰胆管型(31%)和胃型(50%)更常见(p = 0.02)。这些突变的存在并不因异型增生程度而异(GNAS:浸润性61%,高级别59%,低级别53%;KRAS:浸润性71%,高级别62%,低级别74%),这表明这些基因的突变在IPMN致癌作用的早期就发生了。
结论
与IPMN相关的胶样癌及其肠型浸润前体与高频率的GNAS突变相关。管状癌的突变谱类似于传统胰腺腺癌。术前确定突变状态可能有助于临床治疗决策。
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