Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, NY, USA.
Thoracic Oncology Service, Department of Medicine, Division of Solid Tumor Oncology, Memorial Sloan Kettering Cancer Center, New York, NY, USA.
Mod Pathol. 2018 Jan;31(1):111-121. doi: 10.1038/modpathol.2017.110. Epub 2017 Sep 8.
Pulmonary large cell neuroendocrine carcinoma (LCNEC) is a highly aggressive malignancy, which was recently found to comprise three major genomic subsets: small cell carcinoma-like, non-small cell carcinoma (predominantly adenocarcinoma)-like, and carcinoid-like. To further characterize adenocarcinoma-like subset, here we analyzed the expression of exocrine marker napsin A, along with TTF-1, in a large series of LCNECs (n=112), and performed detailed clinicopathologic and genomic analysis of napsin A-positive cases. For comparison, we analyzed napsin A expression in other lung neuroendocrine neoplasms (177 carcinoids, 37 small cell carcinomas) and 60 lung adenocarcinomas. We found that napsin A was expressed in 15% of LCNEC (17/112), whereas all carcinoids and small cell carcinomas were consistently negative. Napsin A reactivity in LCNEC was focal in 12/17 cases, and weak or moderate in intensity in all cases, which was significantly lower in the extent and intensity than seen in adenocarcinomas (P<0.0001). The combination of TTF-1-diffuse/napsin A-negative or focal was typical of LCNEC but was rare in adenocarcinoma, and could thus serve as a helpful diagnostic clue. The diagnosis of napsin A-positive LCNECs was confirmed by classic morphology, diffuse labeling for at least one neuroendocrine marker, most consistently synaptophysin, and the lack of distinct adenocarcinoma component. Genomic analysis of 14 napsin A-positive LCNECs revealed the presence of mutations typical of lung adenocarcinoma (KRAS and/or STK11) in 11 cases. In conclusion, LCNECs are unique among lung neuroendocrine neoplasms in that some of these tumors exhibit low-level expression of exocrine marker napsin A, and harbor genomic alterations typical of adenocarcinoma. Despite the apparent close biological relationship, designation of adeno-like LCNEC as a separate entity from adenocarcinoma is supported by their distinctive morphology, typically diffuse expression of neuroendocrine marker(s) and aggressive behavior. Further studies are warranted to assess the clinical utility and optimal method of identifying adenocarcinoma-like and other subsets of LCNEC in routine practice.
肺大细胞神经内分泌癌(LCNEC)是一种高度侵袭性的恶性肿瘤,最近发现它主要由三个基因组亚型组成:小细胞癌样、非小细胞癌(主要是腺癌)样和类癌样。为了进一步描述腺癌样亚型,我们在此分析了外分泌标志物 Napsin A 在一系列 LCNEC(n=112)中的表达,并对 Napsin A 阳性病例进行了详细的临床病理和基因组分析。为了比较,我们还分析了 Napsin A 在其他肺神经内分泌肿瘤(177 个类癌、37 个小细胞癌)和 60 个肺腺癌中的表达。我们发现 Napsin A 在 15%的 LCNEC(17/112)中表达,而所有的类癌和小细胞癌均始终为阴性。Napsin A 在 LCNEC 中的反应性在 12/17 例中为局灶性,在所有病例中为弱或中度,其在程度和强度上明显低于腺癌(P<0.0001)。TTF-1 弥漫性/Napsin A 阴性或局灶性的组合是 LCNEC 的典型特征,但在腺癌中很少见,因此可作为一个有帮助的诊断线索。Napsin A 阳性 LCNEC 的诊断通过经典形态学、至少一种神经内分泌标志物的弥漫性标记(最常见的是突触素)和缺乏明显的腺癌成分得到确认。对 14 例 Napsin A 阳性 LCNEC 的基因组分析显示,11 例存在典型的肺腺癌突变(KRAS 和/或 STK11)。总之,LCNEC 与肺神经内分泌肿瘤不同,其中一些肿瘤表现出外分泌标志物 Napsin A 的低水平表达,并具有典型的腺癌基因组改变。尽管存在明显的密切生物学关系,但将腺样 LCNEC 指定为与腺癌不同的实体仍然是基于其独特的形态学、神经内分泌标志物的典型弥漫性表达和侵袭性行为。进一步的研究是必要的,以评估在常规实践中识别腺样和其他 LCNEC 亚型的临床实用性和最佳方法。
Zotero 插件
