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Endocervical Adenocarcinoma With Morphologic Features of Both Usual and Gastric Types: Clinicopathologic and Immunohistochemical Analyses and High-risk HPV Detection by In Situ Hybridization.

同时具有普通型和胃型形态学特征的宫颈腺癌:临床病理和免疫组织化学分析以及高危型HPV的原位杂交检测

Wada T,Ohishi Y,Kaku T,Aman M,Imamura H,Yasutake N,Sonoda K,Kato K,Oda Y

Abstract

The fourth edition of the World Health Organization classification set up new entities of endocervical adenocarcinoma (ECA), namely the "usual type" and "gastric type." These 2 types are considered to be distinct histogenetically because of their differing immunophenotypes, human papillomavirus (HPV) status, and prognoses. Usual-type ECAs (U-ECAs) are virtually always associated with high-risk human papillomavirus (HR-HPV) infection. Gastric-type ECAs (G-ECAs) are believed not to be associated with HR-HPV infection. Morphologically, U-ECA cells are characterized by mucin-poor and eosinophilic cytoplasm, resembling endometrioid carcinoma (a pseudoendometrioid feature). G-ECA cells are characterized by abundant clear or pale, mucinous cytoplasm and distinct cell borders. However, in routine practice we noticed that some ECAs contain morphologically usual type-like components and gastric type-like components in a single tumor; we have named these "G+U" ECAs. The histogenesis of such tumors has not been investigated. We conducted the present study to clarify the clinicopathologic and immunohistochemical features and HPV status of G+U ECAs, and to determine whether G+U ECAs are genuine G-ECAs mimicking U-ECAs or genuine U-ECAs with gastric type-like morphology. We retrospectively analyzed a series of 70 consecutive cases of ECA diagnosed as mucinous ECA, endocervical type, and we reclassified them on the basis of the latest World Health Organization classification. We identified 48 (69%) pure U-ECAs, 9 pure G-ECAs, and 13 G+U ECAs. Ten of the 13 G+U ECAs (77%) showed no HR-HPV infection by in situ hybridization (HPV-unrelated G+U ECAs) and showed frequent HIK1083 expression and aberrant p53 expression in both usual type-like and gastric type-like components. The other 3 G+U ECAs showed HR-HPV infection (HPV-related G+U EACs) and frequent p16+/p53-/HIK1083- immunophenotype in both usual type-like and gastric type-like components. The U-ECAs were characterized by HR-HPV infection detected by in situ hybridization and frequent p16+/p53-/HIK1083- immunophenotype, similar to that of the HPV-related G+U ECAs. In contrast, the pure G-ECAs were characterized by the absence of HPV infection and frequent HIK1083 expression and aberrant p53 expression, similar to that of HPV-unrelated G+U ECAs. G+U ECAs thus represent a heterogenous group composed of genuine G-ECAs and genuine U-ECAs. Most of the G+U ECAs we examined were genuine HPV-unrelated G-ECAs with usual type-like components showing mucin-poor, eosinophilic cytoplasm (pseudoendometrioid morphology). A small population of G+U ECAs was genuine HPV-related U-ECAs with gastric type-like components showing mucin-rich, voluminous cytoplasm. Thus, both types of ECAs can occasionally display patterns of differentiation suggesting a component of the other type but true mixed tumors do not appear to exist. Ancillary techniques (immunohistochemical analysis of p16, p53, and HPV DNA detection assays) should be used to assure proper classification of tumors with mixed morphologic features.

摘要

第四版WHO分类新增了宫颈腺癌(ECA)的亚型,命名为“普通型”和“胃型”。这两种亚型的免疫表型、人乳头状瘤病毒(HPV)状态和预后完全不同,因此认为其组织发生不同。普通型宫颈腺癌(U-ECAs)通常与高危型HPV(HR-HPV)感染相关,而胃型宫颈腺癌(G-ECAs)则反之。形态学上,U-ECA的肿瘤细胞以寡黏液和嗜酸性胞质为特征,与子宫内膜样癌(一种假内膜样排列方式)相似。G-ECA的肿瘤细胞则是以胞质丰富、透明或苍白,富含黏液以及细胞界限清楚为特征。然而,在日常工作中我们发现一些发生在同一肿物中的ECAs可以同时具有普通型和胃型的形态学改变,我们将其命名为“G+U”ECAs。 此类肿瘤的组织发生尚无研究。本研究旨在阐明G+U ECAs的临床病理特征、免疫组织化学特征和HPV的状态,以及判断G+U ECAs究竟是与U-ECAs相仿但实质为真正的G-ECAs,还是伴有胃型形态学改变的U-ECAs。我们对70例之前诊断为黏液型和子宫内膜型的宫颈腺癌进行了回顾性分析,并且按照最新的WHO分类将其重新诊断分组。48例(69%)被诊断为纯U-ECAs,9例为纯G-ECAs,13例为G+U ECAs。13例G+U ECAs中的10例经原位杂交检测证实无HR-HPV感染,且无论在普通型宫颈腺癌样成分还是在胃型成分中常常可观察到HIK1083的表达和P53的异常表达。另外3例G+U ECAs则检测出HR-HPV感染(HPV-相关的G+U ECAs),两种肿瘤成分常表达 p16+/p53-/HIK1083- 。U-ECAs的特征为:原位杂交检测证实的HR-HPV感染和p16+/p53-/HIK1083- 的免疫表型,这些特性与HPV-相关的G+U ECAs相似。不同的是,纯G-ECAs以无HPV感染、HIK1083的高频率阳性表达和P53的异常表达为特点,这几点则与HPV-无关的G+U ECAs相似。G+U ECAs应该代表的是一组异质性病变,它的组成涵盖真正的G-ECAs和U-ECAs。实际上,我们判定的G+U ECAs中大部分为真正的HPV无关的G-ECAs伴普通型宫颈腺癌成分,即寡黏液和嗜酸性胞质(假内膜样形态学特点)。小部分的G+U ECAs则是真正的HPV相关的U-ECAs伴胃型宫颈腺癌成分,即大量黏液和丰富胞质。因此,ECAs的两种亚型可以偶尔表现其他类型的分化,这仅说明它包含另一亚型的某些特点,而非是一类真正的混合性肿瘤。辅助诊断(p16、p53的免疫组织化学分析和HPV的DNA检测)在分类这些具有混合的形态学特点的肿瘤时具有重要作用。

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