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血管肉瘤:一项具有诊断意义的组织芯片研究

Angiosarcoma: a tissue microarray study with diagnostic implications.

作者信息

Rao Priya, Lahat Guy, Arnold Christina, Gavino Alde Carlo, Lahat Sharon, Hornick Jason L, Lev Dina, Lazar Alexander J

机构信息

Department of Pathology, The University of Texas MD Anderson Cancer Center, Houston, TX 77030-4009, USA.

出版信息

Am J Dermatopathol. 2013 Jun;35(4):432-7. doi: 10.1097/DAD.0b013e318271295a.

Abstract

BACKGROUND

Angiosarcoma (AS) is a rare soft tissue sarcoma showing endothelial differentiation as indicated by morphology and expression of CD31 (blood), D2-40 (lymphatic), factor VIII, and CD34 (both). We sought to examine the pattern of immunohistochemical markers of differentiation in AS and correlate these with outcome.

DESIGN

An AS tissue microarray (n = 70 specimens) was constructed for immunohistochemical analysis of CD31, CD34, factor VIII, D2-40, and pan-cytokeratin. Samples on this array were linked to clinicopathologic and outcome data for these patients. Univariate analyses were used to explore disease-specific survival (DSS) factors.

RESULTS

Nine metastatic, 23 localized, and 4 recurrent cases were included. Information about the tissue status (ie, primary or metastasis) was unavailable in 4 patients. Primary sites for the tumor included bone (n = 1), breast parenchyma (n = 11), breast skin (n = 4), heart (n = 5), skin (n = 8), soft tissue (n = 7), and unknown (n = 3). Three patients presented with multifocal disease (primary sites in these patients included breast, skin, and soft tissue). Metastatic sites included lung, bone, lymph nodes, brain, liver, and parotid. Of the 40 cases, 8 (20%) showed a pure or predominant epithelioid histology. Of the biomarkers evaluated by tissue microarray, 92% of tumors expressed at least one endothelial marker (factor VIII = 83%, CD31 = 80%, CD34 = 63%, and D2-40 = 43%) with 88% expressing 2 or more markers. Eighty-eight percent of tumors expressing D2-40 coexpressed CD31, an unusual combination in normal vessels. No endothelial marker clearly associated with disease-specific survival. Fifty percent (4/8) of epithelioid cases and 9% (3/32) of nonepithelioid cases showed keratin expression.

CONCLUSIONS

Unusual patterns and loss of endothelial markers are common in AS, suggesting use of multiple markers in challenging cases and perhaps indicating important biologic characteristics.

摘要

背景

血管肉瘤(AS)是一种罕见的软组织肉瘤,其形态学以及CD31(血管内皮)、D2-40(淋巴管内皮)、凝血因子VIII和CD34(两者均表达)的表达均显示出内皮分化特征。我们试图研究血管肉瘤中免疫组化分化标志物的模式,并将其与预后相关联。

设计

构建了一个血管肉瘤组织微阵列(70个标本),用于对CD31、CD34、凝血因子VIII、D2-40和全细胞角蛋白进行免疫组化分析。该阵列上的样本与这些患者的临床病理和预后数据相关联。采用单因素分析来探索疾病特异性生存(DSS)因素。

结果

纳入9例转移病例、23例局限性病例和4例复发病例。4例患者无法获得有关组织状态(即原发或转移)的信息。肿瘤的原发部位包括骨(1例)、乳腺实质(11例)、乳腺皮肤(4例)、心脏(5例)、皮肤(8例)、软组织(7例)和不明部位(3例)。3例患者表现为多灶性疾病(这些患者的原发部位包括乳腺、皮肤和软组织)。转移部位包括肺、骨、淋巴结、脑、肝和腮腺。在40例病例中,8例(20%)表现为纯上皮样或主要为上皮样组织学类型。在通过组织微阵列评估的生物标志物中,92%的肿瘤表达至少一种内皮标志物(凝血因子VIII = 83%,CD31 = 80%,CD34 = 63%,D2-40 = 43%),88%的肿瘤表达两种或更多标志物。88%表达D2-40的肿瘤同时表达CD31,这在正常血管中是一种不寻常的组合。没有内皮标志物与疾病特异性生存明显相关。50%(4/8)的上皮样病例和9%(3/32)的非上皮样病例显示角蛋白表达。

结论

血管肉瘤中内皮标志物的异常模式和缺失很常见,这表明在具有挑战性的病例中应使用多种标志物,这可能也表明了重要的生物学特征。

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