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Endocrine Neoplasms of the Pancreas: Pathologic and Genetic Features

机译:胰腺内分泌肿瘤:病理和遗传特征

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CONTEXT: Pancreatic endocrine neoplasms (PENs) are diagnostically challenging tumors whose natural history is largely unknown. Histopathology allows the distinction of 2 categories: poorly differentiated high-grade carcinomas and well-differentiated neoplasms. The latter include more than 90% of PENs whose clinical behavior varies from indolent to malignant and cannot be predicted by their morphology. OBJECTIVES: To review the literature and report on additional primary material about the clinicopathologic features, classification, staging, grading, and genetic features of PENs. DATA SOURCES: Literature review of relevant articles indexed in PubMed (US National Library of Medicine) and primary material from the authors' institution. CONCLUSIONS: The diagnosis of PEN is generally easy, but unusual features may induce misdiagnosis. Immunohistochemistry solves the issue, provided that the possibility of a PEN has been considered. Morphology allows the distinction of poorly differentiated aggressive carcinomas from well-differentiated neoplasms. The World Health Organization classification criteria allow for the discernment of the latter into neoplasms and carcinomas with either benign or uncertain behavior. The recently proposed staging and grading systems hold great promise for permitting a stratification of carcinomas into clinically significant risk categories. To date, inactivation of the MEN1 gene remains the only ascertained genetic event involved in PEN genesis. It is inactivated in roughly one-third of PENs. The degree of genomic instability correlates with the aggressiveness of the neoplasm. Gene silencing by promoter methylation has been advocated, but a formal demonstration of the involvement of specific genes is still lacking. Expression profiling studies are furnishing valuable lists of mRNAs and noncoding RNAs that may advance further the research to discover novel markers and/or therapeutic targets.
机译:背景:胰腺内分泌肿瘤(PENs)是诊断挑战性肿瘤,其自然病程很大程度上未知。组织病理学可分为两类:低分化的高级别癌和高分化的肿瘤。后者包括超过90%的PEN,其临床表现从惰性到恶性不等,无法通过其形态来预测。目的:回顾文献并报告有关PENs的临床病理特征,分类,分期,分级和遗传特征的其他主要材料。数据来源:PubMed(美国国家医学图书馆)收录的相关文章的文献综述以及来自作者机构的主要材料。结论:PEN的诊断通常很容易,但异常特征可能会引起误诊。免疫组织化学解决了这个问题,但前提是已经考虑了使用PEN的可能性。形态学可以区分低分化的侵袭性癌和高分化的肿瘤。世界卫生组织的分类标准允许将后者区分为良性或不确定性行为的肿瘤和癌。最近提出的分期和分级系统为将癌分层到临床上具有重大风险的类别提供了广阔的前景。迄今为止,MEN1基因的失活仍然是PEN发生中唯一确定的遗传事件。大约有三分之一的PEN禁用了它。基因组不稳定性的程度与肿瘤的侵袭性相关。有人提倡通过启动子甲基化使基因沉默,但仍缺乏有关特定基因参与的正式证明。表达谱研究正在提供有价值的mRNA和非编码RNA列表,这些列表可能会进一步推动发现新标记和/或治疗靶标的研究。

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    《Archives of Pathology & Laboratory Medicine》 |2009年第3期|p.350-364|共15页
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    Paola Capelli, MD, Guido Martignoni, MD, Federica Pedica, MD, Massimo Falconi, MD, Davide Antonello, PhD, Giorgio Malpeli, PhD, Aldo Scarpa, MD, PhDAccepted for publication November 13, 2008.From the Departments of Pathology (Drs Capelli, Martignoni, Pedica, Antonello, and Scarpa) and Surgical and Gastroenterological Sciences (Drs Falconi and Malpeli), University of Verona, Verona, Italy.The authors have no relevant financial interest in the products or companies described in this article.Reprints: Paola Capelli, MD, Department of Pathology, Section of Anatomical Pathology, Policlinico G. B. Rossi, 37134 Verona, Italy (e-mail: paola.capelli@azosp.vr.it).,;

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