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大系统性血管未分化内膜肉瘤:14例报告及免疫组化分析并文献复习

Undifferentiated intimal sarcoma of large systemic blood vessels: report of 14 cases with immunohistochemical profile and review of the literature.

作者信息

Sebenik Matjaz, Ricci Andrew, DiPasquale Bruno, Mody Kokila, Pytel Peter, Jee Kowan Ja, Knuutila Sakari, Scholes John

机构信息

Department of Pathology, Staten Island University Hospital, Staten Island, NY 10305, USA.

出版信息

Am J Surg Pathol. 2005 Sep;29(9):1184-93. doi: 10.1097/01.pas.0000159774.70288.7d.

Abstract

Intimal sarcoma (IS) is defined as a malignant tumor arising in the tunica intima of large blood vessels. In systemic circulation, the majority of IS develop in the aorta, where close to three fourths of published cases lack specific differentiation and are called undifferentiated intimal sarcomas (UIS). The remaining cases are intima-associated sarcomas of recognized types, also called differentiated intimal sarcomas (DIS). In this report, we further characterize UIS, including its immunohistochemical profile and results of comparative genomic hybridization. A total of 14 cases of UIS were collected from 17 medical institutions, including slides, blocks, electron photomicrographs, clinical abstracts, and reports of surgical pathology specimens and autopsies. The patients, 7 women and 7 men, were 41 to 85 years of age (median, 65.6 years). Twelve tumors arose from the aorta, one from the left external iliac and femoral arteries, and one in a large systemic vein (the venous tumor was included due to histologic similarity with the arterial lesions). Tumors ranged from 1 cm to over 10 cm in diameter. Histopathology was that of a largely necrotic, poorly differentiated epithelioid and pleomorphic malignant neoplasm relating to the tunica intima. Usually there was only a thin layer of viable tumor cells overlying a large thrombus. All tumors stained at least focally with the endothelial markers CD31 and Fli-1; however, there was otherwise considerable variability in immunophenotype. The distinctive histopathologic appearance of the primary luminal lesion was lost whenever tumor invaded outside the vessel wall (into adventitia and beyond) or in metastatic sites. Such extravascular tumors assumed a variety of patterns reminiscent of undifferentiated pleomorphic sarcoma (UPS; in older literature also known as pleomorphic malignant fibrous histiocytoma, MFH) or other distinct types of sarcomas, including osteosarcoma, angiosarcoma, and rhabdomyosarcoma. The results of comparative genomic hybridization were nonspecific. Eleven patients died of the disease, in an average of 11 months after diagnosis. Three patients are still alive and free of disease at 4, 16, and 27 years. UIS of large systemic vessels represents a distinct clinical entity where intraluminal sarcoma presents with thrombosis and occlusion of large vessels. It is associated with a highly characteristic, although not entirely specific, histology and immunohistochemical phenotype. The histogenesis of UIS is not certain; however, it seems that the cell of origin must leave the confines of the vessel wall to show altered morphology. Although there are rare long-term survivors, UIS behaves as a fully malignant neoplasm that is almost uniformly associated with metastases and tumor-related death.

摘要

内膜肉瘤(IS)被定义为起源于大血管内膜的恶性肿瘤。在体循环中,大多数内膜肉瘤发生于主动脉,其中近四分之三的已发表病例缺乏特异性分化,被称为未分化内膜肉瘤(UIS)。其余病例为公认类型的内膜相关肉瘤,也称为分化型内膜肉瘤(DIS)。在本报告中,我们进一步描述了UIS的特征,包括其免疫组化特征和比较基因组杂交结果。从17家医疗机构共收集了14例UIS病例,包括玻片、组织块、电子显微镜照片、临床摘要以及手术病理标本和尸检报告。患者共14例,男女各7例,年龄在41至85岁之间(中位年龄为65.6岁)。12个肿瘤起源于主动脉,1个起源于左髂外动脉和股动脉,1个发生于一条大的体静脉(因组织学与动脉病变相似而纳入该静脉肿瘤)。肿瘤直径从1厘米到超过10厘米不等。组织病理学表现为与内膜相关的、大部分坏死、低分化的上皮样和多形性恶性肿瘤。通常在一大块血栓之上仅有一薄层存活的肿瘤细胞。所有肿瘤至少局灶性地表达内皮标志物CD31和Fli-1;然而,免疫表型在其他方面存在相当大的变异性。当肿瘤侵犯血管壁外(进入外膜及以外)或转移部位时,原发腔内病变独特的组织病理学外观就会消失。这种血管外肿瘤呈现出多种形态,让人联想到未分化多形性肉瘤(UPS;在旧文献中也称为多形性恶性纤维组织细胞瘤,MFH)或其他不同类型的肉瘤,包括骨肉瘤、血管肉瘤和横纹肌肉瘤。比较基因组杂交结果不具有特异性。11例患者死于该病,平均在诊断后11个月。3例患者仍存活,分别在4年、16年和27年后无病生存。大血管的UIS代表一种独特的临床实体,其中腔内肉瘤表现为大血管的血栓形成和阻塞。它与一种高度特征性但并非完全特异性的组织学和免疫组化表型相关。UIS的组织发生尚不确定;然而,似乎起源细胞必须离开血管壁的范围才能表现出形态改变。尽管有罕见的长期存活者,但UIS表现为一种完全恶性的肿瘤,几乎总是伴有转移和肿瘤相关死亡。

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