通过转录因子、激素、组织学和患者预后对胰腺神经内分泌肿瘤进行亚型分类。

Elisa Moser, Ayako Ura, Günter Klöppel, Atsuko Kasajima
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引用次数: 0

摘要

背景:胰腺神经内分泌肿瘤(PanNETs)在激素和转录因子(TF)表达方面表现出明显的异质性。ARX和PDX1等转录因子分别与α细胞型和β细胞型特征有关,并与患者的预后有部分关联。然而,目前还缺乏将激素表达、组织学和临床数据相关联的详细研究:本研究旨在确定与组织学、激素和预后结果相关的 PanNETs 亚型:根据四种TFs(ARX、PDX1、ISL1和CDX2)的表达情况,通过聚类分析将185例切除的PanNET分为五种亚型(A1、A2、B、C和D型),并与激素和DAXX/ATRX的表达、ALT激活状态、组织学和无进展生存期相关联:结果:A1亚组(ISL1+/ARX+/PDX-/CDX2-)最常见(46%),其次是B组(18%;ISL1+/ARX-/PDX+/CDX2-)、A2组(15%;ISL1+/ARX+/PDX+/CDX2-)、C组(15%;ISL1-/ARX-/PDX-/CDX2-)和D组(5%;ISL1-/ARX-/PDX+/CDX2+)。A1 和 A2 亚组与小梁生长模式以及胰高血糖素和胰多肽(PP)的表达密切相关(P 结论):泛NET可根据不同的TF特征分为五个亚组,它们与组织学、激素分泌、功能和患者预后密切相关。
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Subtyping of pancreatic neuroendocrine tumors by transcription factors, hormones, histology, and patient outcome.

Background: Pancreatic neuroendocrine tumors (PanNETs) show pronounced heterogeneity in terms of hormone and transcription factor (TF) expression. TFs such as ARX and PDX1 are related to alpha- and beta-cell-type features, respectively, and partly associate with patient outcome. However, detailed studies correlating hormone expression, histology, and clinical data are lacking.

Objective: The aim of this study was to identify subtypes of PanNETs that associate with histological, hormonal, and prognostic findings.

Methods: A total of 185 resected PanNETs were divided into five subtypes (types A1, A2, B, C, and D) by cluster analysis based on expression of four TFs (ARX, PDX1, ISL1, and CDX2) and correlated to the expression of hormones and DAXX/ATRX as well as ALT activation status, histology, and progression-free survival.

Results: Subgroup A1 (ISL1+/ARX+/PDX-/CDX2-) was most frequent (46%), followed by type B (18%; ISL1+/ARX-/PDX+/CDX2-), A2 (15%; ISL1+/ARX+/PDX+/CDX2-), C (15%; ISL1-/ARX-/PDX-/CDX2-), and D (5%; ISL1-/ARX-/PDX+/CDX2+). Subgroups A1 and A2 showed a strong association with a trabecular growth pattern and glucagon and pancreatic polypeptide (PP) expression (p < 0.001), while A2 was in addition associated with gastrin expression. Subgroup B was associated with insulin production (p < 0.001) and included all 17 insulinomas. Subgroup C was associated with solid morphology and expression of serotonin, calcitonin, and adrenocorticotropic hormone (ACTH). Subgroup D showed solid morphology, expression of ACTH, somatostatin, or serotonin and had the shortest disease-free survival (p < 0.01). ALT positivity was associated with poorer outcome in types A1 and A2 but not in other types.

Conclusion: PanNETs can be categorized into five subgroups based on different TF signatures, which associate strongly with histology, hormone production, functionality, and patient outcome.

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