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Neuroendocrine Carcinoma of the Uterine Cervix: A Clinicopathologic and Immunohistochemical Study with Focus on Novel Markers (Sst2–Sst5)

机译:子宫颈的神经内分泌癌:临床病理学和免疫组织化学研究重点关注新型标志物(Sst2–Sst5)

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摘要

Background. Gynecological neuroendocrine neoplasms (NENs) are extremely rare, accounting for 1.2–2.4% of the NENs. The aim of this study was to test cervical NENs for novel markers of potential utility for differential diagnosis and target therapy. Methods. All cases of our center ( = 16) were retrieved and tested by immunohistochemistry (IHC) for 12 markers including markers of neuroendocrine differentiation (chromogranin A, synaptophysin, CD56), transcription factors (CDX2 and TTF1), proteins p40, p63, p16INK4a, and p53, somatostatin receptors subtypes (SST2-SST5) and the proliferation marker Ki67 (MIB1). Results. All cases were poorly differentiated neuroendocrine carcinomas (NECs), 10 small cell types (small cell–neuroendocrine carcinomas, SCNECs) and 6 large cell types (large cell–neuroendocrine carcinomas, LCNECs); in 3 cases a predominant associated adenocarcinoma component was observed. Neuroendocrine cancer cells expressed at least 2 of the 3 tested neuroendocrine markers; p16 was intensely expressed in 14 (87.5%) cases; SST5 in 11 (56.25%, score 2–3, in 9 cases); SST2 in 8 (50%, score 2–3 in 8), CDX2 in 8 (50%), TTF1 in 5 (31.25%), and p53 in 1 case (0.06%). P63 and p40 expressions were negative, with the exception of one case that showed moderate expression for p63. Conclusions. P40 is a more useful marker for the differential diagnosis compared to squamous cell carcinoma. Neither CDX2 nor TTF1 expression may help the differential diagnosis versus potential cervical metastasis. P16 expression may suggest a cervical origin of NEC; however, it must be always integrated by clinical and instrumental data. The expression of SST2 and SST5 could support a role for SSAs (Somatostatin Analogues) in the diagnosis and therapy of patients with cervical NECs.
机译:背景。妇科神经内分泌肿瘤(NEN)极为罕见,占NEN的1.2–2.4%。这项研究的目的是测试宫颈NENs的新标记物,这些新标记物可用于鉴别诊断和靶标治疗。方法。我们中心的所有病例(= 16)均被检索并通过免疫组织化学(IHC)测试了12种标记物,包括神经内分泌分化标记物(嗜铬粒蛋白A,突触素,CD56),转录因子(CDX2和TTF1),蛋白p40,p63,p16INK4a, p53,生长抑素受体亚型(SST2-SST5)和增殖标记Ki67(MIB1)。结果。所有病例均为低分化神经内分泌癌(NEC),10种小细胞类型(小细胞-神经内分泌癌,SCNECs)和6种大细胞类型(大细胞-神经内分泌癌,LCNEC)。在3例病例中,观察到主要的相关腺癌成分。神经内分泌癌细胞表达了3种测试的神经内分泌标记物中的至少2种; p16在14例(87.5%)病例中被强烈表达; SST5 11例(56.25%,2-3分,9例); SST2为8(50%,得分2-3在8中),CDX2为8(50%),TTF1为5(31.25%),p53为1例(0.06%)。 P63和p40表达为阴性,除了一例显示p63中等表达的病例。结论。与鳞状细胞癌相比,P40是用于鉴别诊断的更有用的标记物。 CDX2和TTF1的表达都不能帮助鉴别诊断和潜在的宫颈转移。 P16表达可能提示NEC的子宫颈起源。但是,必须始终将其与临床和仪器数据结合在一起。 SST2和SST5的表达可能支持SSA(Somatostatin类似物)在宫颈NEC患者的诊断和治疗中的作用。

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