Department of Pathology, TUM School of Medicine and Health, Technical University Munich, Munich, Germany.
Department of Nuclear Medicine, TUM School of Medicine and Health, Technical University Munich, Munich, Germany.
Mod Pathol. 2024 Nov;37(11):100595. doi: 10.1016/j.modpat.2024.100595. Epub 2024 Aug 13.
Many pancreatic neuroendocrine tumors (PanNETs) fall into 2 major prognostic subtypes based on DAXX/ATRX-induced alternative lengthening of telomerase phenotype and alpha- and beta-cell-like epigenomic profiles. However, these PanNETs are still flanked by other PanNETs that do not fit into either subtype. Furthermore, despite advanced genotyping, PanNETs are generally not well-characterized in terms of their histologic and hormonal phenotypes. We aimed to identify new subgroups of PanNETs by extending the currently used transcription factor signatures and investigating their correlation with histologic, hormonal, molecular, and prognostic findings. One hundred eighty-five PanNETs (nonfunctioning 165 and functioning 20), resected between 1996 and 2023, were classified into 5 subgroups (A1, A2, B, C, and D) by cluster analysis based on ARX, PDX1, islet-1 (ISL1), and CDX2 expressions and correlated with trabecular vs solid histology, expression of insulin, glucagon, polypeptide (PP), somatostatin, serotonin, gastrin, calcitonin, adrenocorticotropic hormone (ACTH), DAXX/ATRX, MEN1, and alternative lengthening of telomerase status by fluorescence in situ hybridization, and disease-free survival. A1 (46%, ARX+/ISL1+/PDX1-/CDX2-) and A2 (15%, ARX+/ISL1+/PDX1+/CDX2-) showed trabecular histology and glucagon/PP expression, with A2 also showing gastrin expression. B (18%, PDX1+/ISL1+/ARX-/CDX2-) showed solid histology, insulin, and somatostatin expression (P < .001). It included all insulinomas and had the best outcome (P < .01). C (15%, ARX-/PDX1-/ISL1-/CDX2-) showed solid histology and frequent expression of serotonin, calcitonin, and ACTH. D (5%, PDX1+/CDX2+/ISL1-/ARX-) showed solid histology, expressed ACTH/serotonin, and was an independent poor prognosticator (P < .01). Differential expressions of ARX, PDX1, ISL1, and CDX2 stratified PanNETs into 5 subgroups with different histologies, hormone expressions, and outcomes. Subgroups A1 and A2 resembled the alpha-cell-like type, and subgroup B, the beta-cell-like type. Subgroup C with almost no transcription factor signature was unclear in cell lineage, whereas the PDX+/CDX2+ signature of subgroup D suggested a pancreatic/intestinal cell lineage. Assigning PanNETs to the subgroups may help establish the diagnosis, predict the outcome, and guide the treatment.
许多胰腺神经内分泌肿瘤 (PanNETs) 根据 DAXX/ATRX 诱导的端粒酶表型和 alpha 和 beta 细胞样表观基因组特征分为 2 种主要的预后亚型。然而,这些 PanNETs 仍然被其他不符合任何亚型的 PanNETs 所包围。此外,尽管进行了先进的基因分型,但 PanNETs 在其组织学和激素表型方面通常没有得到很好的描述。我们旨在通过扩展当前使用的转录因子特征来识别新的 PanNET 亚组,并研究它们与组织学、激素、分子和预后发现的相关性。1996 年至 2023 年间切除的 185 个 PanNETs(无功能 165 个,有功能 20 个),根据 ARX、PDX1、胰岛-1(ISL1)和 CDX2 的表达进行聚类分析,分为 5 个亚组(A1、A2、B、C 和 D),并与小梁状与实性组织学、胰岛素、胰高血糖素、多肽(PP)、生长抑素、血清素、胃泌素、降钙素、促肾上腺皮质激素(ACTH)、DAXX/ATRX、MEN1 和端粒酶的荧光原位杂交的延长状态以及无病生存相关。A1(46%,ARX+/ISL1+/PDX1-/CDX2-)和 A2(15%,ARX+/ISL1+/PDX1+/CDX2-)表现为小梁状组织学和胰高血糖素/PP 表达,A2 还表现为胃泌素表达。B(18%,PDX1+/ISL1+/ARX-/CDX2-)表现为实性组织学、胰岛素和生长抑素表达(P<0.001)。它包括所有胰岛素瘤,并且具有最好的预后(P<0.01)。C(15%,ARX-/PDX1-/ISL1-/CDX2-)表现为实性组织学和频繁表达血清素、降钙素和 ACTH。D(5%,PDX1+/CDX2+/ISL1-/ARX-)表现为实性组织学,表达 ACTH/血清素,是独立的不良预后因素(P<0.01)。ARX、PDX1、ISL1 和 CDX2 的差异表达将 PanNETs 分为具有不同组织学、激素表达和预后的 5 个亚组。亚组 A1 和 A2 类似于 alpha 细胞样类型,而亚组 B 类似于 beta 细胞样类型。亚组 C 几乎没有转录因子特征,其细胞谱系尚不清楚,而亚组 D 的 PDX+/CDX2+特征提示其来自胰腺/肠细胞谱系。将 PanNETs 分配到亚组中有助于建立诊断、预测预后并指导治疗。
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