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New insights into hypoxia-related mechanisms involved in different microvascular patterns of bronchopulmonary carcinoids and poorly differentiated neuroendocrine carcinomas. Role of ribonuclease T2 (RNASET2) and HIF-1α

机译:新洞察缺氧相关机制,涉及不同微血管毒细胞癌和差异差异化神经内分泌癌的不同微血管模式。 核糖核酸酶T2(RNASET2)和HIF-1α的作用

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Ribonuclease T2 (RNASET2) is a pleiotropic and polyfunctional protein, which exerts several different activities in neoplastic cells since the early steps of tumor development. Besides having an antitumorigenic activity, RNASET2 inhibits both bFGF-induced and VEGF-induced angiogenesis and has a role as a stress-response, alarmin-like, protein. In this study, we investigated RNASET2 expression in well-differentiated and poorly differentiated neuroendocrine neoplasms of the lung (Lu-NENs), which are known to show clear-cut differences in morphology, biology and clinical behavior. In addition, we explored possible relationships between RNASET2 expression and a series of immunohistochemical markers related to hypoxic stress, apoptosis, proliferation and angiogenesis. Our results showed a significantly higher expression of RNASET2, HIF-1α, and its target CA IX in poorly differentiated than in well-differentiated Lu-NENs, the former also showing higher proliferation and apoptotic rates, as well as a lower microvessel density (MVD) than the latter. Moreover, we were able to demonstrate in vitro an overexpression of RNASET2 in consequence of the activation of HIF-1α. In conclusion, we suggest that in poorly differentiated Lu-NENs, RNASET2 expression may be induced by HIF-1α, behaving as an alarmin-like molecule. In this aggressive group of cancers, which have highly deregulated proliferation pathways, RNASET2 fails to exert the growth-inhibiting effects described in other types of neoplasms. Its increased expression, however, may contribute to the typical phenotypic alterations seen in poorly differentiated Lu-NENs, such as the high apoptotic rate and the extensive necrosis, and may also enhance the low MVD observed in these neoplasms.
机译:Ribonuclease T2(RNASet2)是一种磷酸和多官能蛋白,其自肿瘤发育早期步骤以来施加几种不同的活性。除了具有抗肿瘤活性之外,RNASET2抑制了BFGF诱导和VEGF诱导的血管生成,并且具有应激响应,呈蛋白质的蛋白质的作用。在这项研究中,我们研究了肺(Lu-nens)的良好分化和差异差异化的神经内分泌肿瘤中的RNASET2表达,该表达众所周知,众所周知,表现出形态,生物学和临床行为的透明差异。此外,我们探讨了RNASET2表达与一系列与缺氧应激,细胞凋亡,增殖和血管生成相关的一系列免疫组织化学标志物之间的可能关系。我们的结果表明,RNASET2,HIF-1α的表达显着高于差异化的鲁汶良好,前者也显示出更高的增殖和凋亡率,以及较低的微血管密度(MVD )比后者。此外,由于HIF-1α的激活,我们能够在体外证明RNASET2的过表达。总之,我们建议在差异化的Lu-nens中,HIF-1α可以诱导RNASET2表达,表现为像呈辐射的分子。在这种具有高度失调增殖途径的侵略性癌症中,RNASET2不能施加其他类型的肿瘤中描述的生长抑制效果。然而,其增加的表达可能有助于典型的表型改变在差异化的Lu-nens中,例如高凋亡率和广泛的坏死,并且还可以增强这些肿瘤中观察到的低MVD。

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