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成血管细胞瘤中基质细胞的血管生成性组织发生:超微结构和免疫组织化学研究

Angiogenic histogenesis of stromal cells in hemangioblastoma: ultrastructural and immunohistochemical study.

作者信息

Lach B, Gregor A, Rippstein P, Omulecka A

机构信息

Department of Laboratory Medicine and Pathology, University of Ottawa, Canada.

出版信息

Ultrastruct Pathol. 1999 Sep-Oct;23(5):299-310. doi: 10.1080/019131299281446.

Abstract

Controversy regarding the origin of characteristic stromal cells (SC) is responsible for the placement of hemangioblastoma as a single entity in the category of "tumors of uncertain histogenesis" in the current WHO classification of brain tumors. This subclassification of hemangioblastoma is, to a large extent, a consequence of a remarkable antigenic heterogeneity of SC demonstrated in many, often contradictory immunohistochemical studies. In contrast, most of the electron microscopic studies demonstrated a number of features indicating angiogenic nature of SC and, therefore, hemangioblastoma. This study reevaluated the histogenesis of SC, applying immunohistochemistry as well as electron microscopy and immunoelectron microscopy. Immunohistochemical studies confirmed most of the previous results indicating a very frequent expression of vimentin, S-100 protein, neuron-specific enolase, and cytokeratins. SC were less commonly immunoreactive for desmin, factor XIIIa, and Ricinus communis lectin receptors, and only occasionally for factor VIII and Ulex europeus lectin. They were negative for other markers of endothelial, neuronal, glial, neuroendocrine, and smooth muscle differentiation. Approximately 1% of SC showed Ki67 immunoreactivity, indicating their slight proliferative activity, consistent with the benign nature of the tumor. In contrast to the inconclusive results of the immunohistochemistry, electron microscopy demonstrated a clear relationship of SC to endothelial cells, smooth muscle cells, and pericytes. Occasional SC were found within the vascular lumina. SC often showed intracellular caveolae consistent with the formation of early capillary lumina. Moreover, occasional SC contained small Weibel-Palade bodies positive for factor VIII in immunoelectron microscopy. SC represent a heterogeneous population of abnormally differentiating mesenchymal cells of angiogenic lineage, with some morphological features of endothelium, pericytes, and smooth muscle cells. Occurrence of SC in hemangioblastoma could be related to a limited ability of angioformative stromal cells to develop an architecture of capillary lumina integrated with the vascular network of the tumor. Hemangioblastoma should be reclassified and included together with other vascular tumors of the central nervous system.

摘要

关于特征性基质细胞(SC)起源的争议,导致在当前世界卫生组织(WHO)脑肿瘤分类中,成血管细胞瘤被列为“组织发生不确定的肿瘤”类别中的单一实体。成血管细胞瘤的这种亚分类在很大程度上是许多免疫组织化学研究中所显示的SC显著抗原异质性的结果,这些研究结果往往相互矛盾。相比之下,大多数电子显微镜研究显示了一些特征,表明SC以及成血管细胞瘤具有血管生成的性质。本研究重新评估了SC的组织发生,应用了免疫组织化学以及电子显微镜和免疫电子显微镜技术。免疫组织化学研究证实了之前的大多数结果,表明波形蛋白、S-100蛋白、神经元特异性烯醇化酶和细胞角蛋白的表达非常频繁。SC对结蛋白、因子ⅩⅢa和蓖麻凝集素受体的免疫反应性较低,对因子Ⅷ和欧洲荆豆凝集素仅偶尔有反应。它们对内皮、神经元、神经胶质、神经内分泌和平滑肌分化的其他标志物呈阴性。约1%的SC显示Ki67免疫反应性,表明其轻微的增殖活性,这与肿瘤的良性性质一致。与免疫组织化学的不确定结果相反,电子显微镜显示SC与内皮细胞、平滑肌细胞和周细胞有明确的关系。偶尔在血管腔内发现SC。SC常显示细胞内小窝,与早期毛细血管腔的形成一致。此外,在免疫电子显微镜下,偶尔有SC含有对因子Ⅷ呈阳性的小魏-帕拉德小体。SC代表血管生成谱系中异常分化的间充质细胞的异质性群体,具有内皮细胞、周细胞和平滑肌细胞的一些形态学特征。成血管细胞瘤中SC的出现可能与血管形成性基质细胞发展与肿瘤血管网络整合的毛细血管腔结构的能力有限有关。成血管细胞瘤应重新分类,并与中枢神经系统的其他血管肿瘤归为一类。

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