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重新审视卵黄囊瘤。回顾其多样的面貌和名称。

Yolk sac tumours revisited. A review of their many faces and names.

机构信息

Pathology Department, San Cecilio University Hospital, University of Granada Medical School, Granada, Spain.

出版信息

Histopathology. 2012 Jun;60(7):1023-33. doi: 10.1111/j.1365-2559.2011.03889.x. Epub 2011 Oct 18.

Abstract

We review the current knowledge on human yolk sac tumours (YSTs) 50 years after their initial description. Their complex nomenclature and histogenesis stress the fact that they are not a discrete entity, but represent a multifaceted group of neoplasms, for which the term primitive endodermal tumours would be more appropriate, accounting for their capacity to differentiate into various extraembryonal and somatic cell types. Different histological patterns of human YSTs correlate with the developmental potential of primitive endoderm and mesenchyme, but they are also similar to some murine experimental tumours. Exceptionally, YSTs replicate the tubular structures of the human yolk sac and allantois. Endodermal somatic differentiation reproduces pulmonary, intestinal and hepatic tissues and are identical with some, embryonal-type endodermal, gastric and lung carcinomas, which are indistinguishable from YSTs. YSTs may show an overgrowth of their mesenchymal (sarcomatous) and epithelial components (such as mucinous carcinoma or carcinoid) and also be a source of haematological malignancies. YSTs associated with non-germ cell tumours probably originate from malignant pluripotent somatic stem cells. Only AFP and glypican-3 are characteristic immunohistochemical markers. Pluripotent antibodies (SALL4, Lin28, IMP-3) help in differential diagnoses, while some differentiation markers (CDX2, TTF-1, HepPar1) facilitate recognition of unusual variants of YSTs.

摘要

我们回顾了人类卵黄囊瘤(YST)最初描述 50 年后的现有知识。它们复杂的命名法和组织发生强调了这样一个事实,即它们不是一个离散的实体,而是代表了一组多方面的肿瘤,它们被称为原始内胚层肿瘤更为合适,因为它们有分化为各种胚胎外和体细胞类型的能力。人类 YST 的不同组织学模式与原始内胚层和间充质的发育潜力相关,但它们也与一些鼠类实验性肿瘤相似。例外的是,YST 复制了人类卵黄囊和尿囊的管状结构。内胚层体细胞分化再现了肺、肠和肝组织,与某些胚胎型内胚层、胃和肺癌相同,这些肿瘤与 YST 无法区分。YST 可能表现出其间充质(肉瘤样)和上皮成分(如黏液性癌或类癌)的过度生长,并且也是血液系统恶性肿瘤的来源。与非生殖细胞肿瘤相关的 YST 可能起源于恶性多能体干细胞。只有 AFP 和糖蛋白 3 是特征性免疫组织化学标志物。多能性抗体(SALL4、Lin28、IMP-3)有助于鉴别诊断,而一些分化标志物(CDX2、TTF-1、HepPar1)有助于识别 YST 的不寻常变体。

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