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Histogenetic Characterization of Giant Cell Tumor of Bone

机译:骨巨细胞瘤的组织学表征

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摘要

The unpredictable behavior of giant cell tumor (GCT) parallels its controversial histogenesis. Multinucleated giant cells, stromal cells, and CD68+ monocytes/macrophages are the three elements that interact in GCT. We compared the ability of stromal cells and normal mesenchymal stromal cells to differentiate into osteoblasts. Stromal cells and mesenchymal cells had similar proliferation rates and lifespans. Although stromal cells expressed early osteogenic markers, they were unable to differentiate into osteoblasts but they did express intracellular adhesion molecule-1, a marker of bone-lining cells. They were unable to form clones in a semisolid medium and unable to promote osteoclast differentiation, although they exerted a strong chemotactic effect on osteoclast precursors. Stromal cells may be either immature proliferating osteogenic elements or specialized osteoblast-like cells that fail to show neoplastic features but can induce the differentiation of osteoclast precursors. They might be secondarily induced to proliferate by a paracrine effect induced by monocyte-macrophages and/or giant cells. The increased number of giant cells in GCT may be secondary to an autocrine circuit mediated by the receptor activator of nuclear factor kB.
机译:巨细胞瘤(GCT)的不可预测的行为与其有争议的组织发生相平行。多核巨细胞,基质细胞和CD68 + 单核细胞/巨噬细胞是在GCT中相互作用的三个要素。我们比较了基质细胞和正常间充质基质细胞分化为成骨细胞的能力。基质细胞和间质细胞具有相似的增殖率和寿命。尽管基质细胞表达了早期的成骨标志物,但它们无法分化为成骨细胞,但它们确实表达了细胞内粘附分子-1(骨衬细胞的标志物)。尽管它们对破骨细胞前体具有强大的趋化作用,但它们无法在半固体培养基中形成克隆,也无法促进破骨细胞分化。基质细胞可能是未成熟的成骨细胞,也可能是特化的成骨细胞样细胞,不能表现出肿瘤特征,但可以诱导破骨细胞前体的分化。单核巨噬细胞和/或巨细胞诱导的旁分泌作用可能继而诱导它们增殖。 GCT中巨细胞数量的增加可能是继发于核因子kB受体激活剂介导的自分泌回路的继发作用。

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