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Prox1 转录因子作为血管肿瘤标志物的评估——对 314 例血管内皮肿瘤和 1086 例非血管肿瘤的评估。

Prox1 transcription factor as a marker for vascular tumors-evaluation of 314 vascular endothelial and 1086 nonvascular tumors.

机构信息

Laboratory of Pathology, National Cancer Institute, Bethesda 20892, MD, USA.

出版信息

Am J Surg Pathol. 2012 Mar;36(3):351-9. doi: 10.1097/PAS.0b013e318236c312.

Abstract

Prox1, a transcription factor important in the regulation and maintenance of the lymphatic endothelial phenotype, is consistently expressed in lymphangiomas and Kaposi sarcoma and has also been reported in Kaposiform hemangioendothelioma. However, information on its distribution in vascular tumors, such as angiosarcoma, is limited. In this study, we examined selected normal tissues and 314 vascular endothelial and 1086 nonvascular tumors to get an insight into the biology of these tumors and on potential diagnostic use of Prox1 as an immunohistochemical marker. In adult tissues, Prox1 was essentially restricted to lymphatic endothelia, with expression in subsets of pancreatic and gastrointestinal epithelia. However, it was also detected in embryonic liver and heart. Prox1 was consistently expressed in lymphangiomas, venous hemangiomas, Kaposi sarcoma, in endothelia of spindle cell hemangioma, Kaposiform hemangioendothelioma, and retiform hemangioendothelioma, and in half of epithelioid hemangioendotheliomas. It was present in most cutaneous angiosarcomas from different sites but was less commonly expressed in deep soft tissue and visceral angiosarcomas. In contrast, Prox1 was generally absent in capillary and cavernous hemangiomas. In positive hemangiomas and angiosarcomas it was coexpressed with podoplanin, another marker of the lymphatic endothelial phenotype. There was an inverse correlation with CD34 expression. The expression in mesenchymal nonendothelial neoplasm was limited. Prox1 was detected in 5 of 27 synovial sarcomas, specifically in the epithelia of biphasic tumors. Four of 16 Ewing sarcomas and 5 of 15 paragangliomas were also positive. All melanomas and undifferentiated sarcomas were negative. Among epithelial neoplasms, Prox1 was detected in 18 of 38 colonic carcinomas and 10 of 15 cholangiocarcinomas and in a minority of pulmonary, prostatic, and endometrial adenocarcinomas. The common Prox1 expression in angiosarcoma and its rare presence in nonvascular mesenchymal tumors make this marker suitable for the diagnosis of angiosarcoma and Kaposi sarcoma. However, the presence of Prox1 in some malignant epithelial tumors necessitates caution in applying Prox1 as a marker for vascular tumors. Common Prox1 expression in angiosarcoma may reflect the lymphatic endothelial phenotype in these tumors. Its patterns of expression in hemangiomas and angiosarcoma may be diagnostically useful and offer a new parameter in the biological classification of vascular tumors.

摘要

Prox1 是一种在淋巴管内皮细胞表型的调节和维持中起重要作用的转录因子,在淋巴管瘤和卡波西肉瘤中持续表达,也在卡波西样血管内皮细胞瘤中报道过。然而,关于其在血管肿瘤(如血管肉瘤)中的分布信息有限。在这项研究中,我们检查了选定的正常组织和 314 例血管内皮肿瘤和 1086 例非血管肿瘤,以深入了解这些肿瘤的生物学特性,并探讨 Prox1 作为免疫组化标志物的潜在诊断用途。在成人组织中,Prox1 主要局限于淋巴管内皮细胞,在胰腺和胃肠道上皮的亚群中表达。然而,它也在胚胎肝脏和心脏中被检测到。Prox1 在淋巴管瘤、静脉血管瘤、卡波西肉瘤、梭形细胞血管瘤、卡波西样血管内皮细胞瘤和网状血管内皮细胞瘤的内皮中持续表达,并且在一半的上皮样血管内皮细胞瘤中表达。它存在于来自不同部位的大多数皮肤血管肉瘤中,但在深部软组织和内脏血管肉瘤中表达较少。相比之下,Prox1 通常不存在于毛细血管和海绵状血管瘤中。在阳性的血管瘤和血管肉瘤中,它与 podoplanin 共同表达,后者是淋巴管内皮表型的另一个标志物。它与 CD34 表达呈负相关。在间充质非内皮肿瘤中的表达有限。Prox1 在 27 例滑膜肉瘤中的 5 例中被检测到,特别是在双相肿瘤的上皮中。16 例尤因肉瘤中的 4 例和 15 例副神经节瘤中的 5 例也是阳性的。所有黑色素瘤和未分化肉瘤均为阴性。在上皮性肿瘤中,Prox1 在 38 例结肠腺癌中的 18 例和 15 例胆管癌中的 10 例中被检测到,并且在少数肺、前列腺和子宫内膜腺癌中也有少量表达。Prox1 在血管肉瘤中的常见表达和在非血管间充质肿瘤中的罕见存在使得该标志物适合诊断血管肉瘤和卡波西肉瘤。然而,Prox1 在一些恶性上皮肿瘤中的存在需要谨慎应用 Prox1 作为血管肿瘤的标志物。在这些肿瘤中,Prox1 的共同表达可能反映了它们的淋巴管内皮表型。其在血管瘤和血管肉瘤中的表达模式可能具有诊断价值,并为血管肿瘤的生物学分类提供了一个新的参数。

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