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首页> 外文期刊>Clinical and experimental metastasis >Tumor-stromal interactions of the bone microenvironment: in vitro findings and potential in vivo relevance in metastatic lung cancer models.
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Tumor-stromal interactions of the bone microenvironment: in vitro findings and potential in vivo relevance in metastatic lung cancer models.

机译:骨微环境的肿瘤基质相互作用:转移性肺癌模型的体外发现和潜在的体内相关性。

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摘要

Lung cancer comprises a large variety of histological subtypes with a frequent proclivity to form bone metastasis; a condition associated with dismal prognosis. To identify common mechanisms in the development of osteolytic metastasis, we systematically screened a battery of lung cancer cell lines and developed three models of non-small cell lung cancer (NSCLC) with a common proclivity to form osseous lesions, which represented different histological subtypes. Comparative analysis revealed different incidences and latency times. These differences were correlated with cell-type-specific secretion of osteoclastogenic factors, including macrophage inflammatory protein-1alpha, interleukin-8 and parathyroid hormone-related protein, some of which were exacerbated in conditions that mimicked tumor-stroma interactions. In addition, a distinct signature of matrix metalloproteinase (MMP) activity derived from reciprocal tumor-stroma interactions was detected for each tumor cell line. Thus, these results suggest subtle differences in the mechanisms of bone colonization for each lung cancer subtype, but share, although each to a different degree, dual MMP and osteoclastogenic activities that are differentially enhanced upon tumor-stromal interactions.
机译:肺癌包括多种组织学亚型,经常倾向于形成骨转移。与预后不良有关的疾病。为了确定溶骨性转移发展的常见机制,我们系统地筛选了一系列肺癌细胞系,并开发了三种常见的非小细胞肺癌(NSCLC)模型,它们倾向于形成骨性病变,代表了不同的组织学亚型。比较分析显示了不同的发生率和等待时间。这些差异与破骨细胞形成因子的细胞类型特异性分泌有关,包括巨噬细胞炎性蛋白-1α,白介素8和甲状旁腺激素相关蛋白,其中一些在模仿肿瘤-基质相互作用的情况下会加剧。另外,对于每种肿瘤细胞系,检测到源自相互的肿瘤-基质相互作用的基质金属蛋白酶(MMP)活性的独特特征。因此,这些结果表明每种肺癌亚型的骨定植机制存在细微差异,但是尽管每种都具有不同程度,但它们都共享双重MMP和破骨细胞生成活性,这些活性在肿瘤-基质相互作用后会有所不同。

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