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SHP2, SOCS3 and PIAS3 Expression Patterns in Medulloblastomas: Relevance to STAT3 Activation and Resveratrol-Suppressed STAT3 Signaling

机译:SHP2,SOCS3和PIAS3在髓母细胞瘤中的表达模式:与STAT3激活和白藜芦醇抑制STAT3信号传导的相关性

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Background: Activated STAT3 signaling is critical for human medulloblastoma cells. SHP2, SOCS3 and PIAS3 are known as the negative regulators of STAT3 signaling, while their relevance to frequent STAT3 activation in medulloblastomas remains unknown. Methods: Tissue microarrays were constructed with 17 tumor-surrounding noncancerous brain tissues and 61 cases of the classic medulloblastomas, 44 the large-cell medulloblastomas, and 15 nodular medulloblastomas, which were used for immunohistochemical profiling of STAT3, SHP2, SOCS3 and PIAS3 expression patterns and the frequencies of STAT3 nuclear translocation. Three human medulloblastoma cell lines (Daoy, UW228-2 and UW228-3) were cultured with and without 100 μM resveratrol supplementation. The influences of resveratrol in SHP2, SOCS3 and PIAS3 expression and SOCS3 knockdown in STAT3 activation were analyzed using multiple experimental approaches. Results: SHP2, SOCS3 and PIAS3 levels are reduced in medulloblastomas in vivo and in vitro, of which PIAS3 downregulation is more reversely correlated with STAT3 activation. In resveratrol-suppressed medulloblastoma cells with STAT3 downregulation and decreased incidence of STAT3 nuclear translocation, PIAS3 is upregulated, the SHP2 level remains unchanged and SOCS3 is downregulated. SOCS3 proteins are accumulated in the distal ends of axon-like processes of resveratrol-differentiated medulloblastoma cells. Knockdown of SOCS3 expression by siRNA neither influences cell proliferation nor STAT3 activation or resveratrol sensitivity but inhibits resveratrol-induced axon-like process formation. Conclusion: Our results suggest that (1) the overall reduction of SHP2, SOCS3 and PIAS3 in medulloblastoma tissues and cell lines; (2) the more inverse relevance of PIAS3 expression with STAT3 activation; (3) the favorable prognostic values of PIAS3 for medulloblastomas and (4) the involvement of SOCS3 in resveratrol-promoted axon regeneration of medulloblastoma cells.
机译:背景:激活的STAT3信号对于人类髓母细胞瘤细胞至关重要。 SHP2,SOCS3和PIAS3被称为STAT3信号的负调节剂,但它们与髓母细胞瘤中频繁STAT3激活的相关性仍未知。方法:用17个肿瘤周围非癌性脑组织,61例经典髓母细胞瘤,44例大细胞髓母细胞瘤和15个结节性髓母细胞瘤构建组织芯片,​​用于免疫组化分析STAT3,SHP2,SOCS3和PIAS3表达模式STAT3核易位的频率。在添加和不添加100μM白藜芦醇的情况下,培养了三种人类髓母细胞瘤细胞系(Daoy,UW228-2和UW228-3)。使用多种实验方法分析了白藜芦醇对SHP2,SOCS3和PIAS3表达的影响以及SOCS3敲低对STAT3激活的影响。结果:体内和体外髓母细胞瘤中SHP2,SOCS3和PIAS3的水平降低,其中PIAS3的下调与STAT3激活的反向相关性更高。在具有STAT3下调和STAT3核易位发生率降低的白藜芦醇抑制的髓母细胞瘤细胞中,PIAS3被上调,SHP2水平保持不变,SOCS3被下调。 SOCS3蛋白积聚在白藜芦醇分化的髓母细胞瘤细胞的轴突样过程的远端。 siRNA抑制SOCS3表达既不影响细胞增殖也不影响STAT3激活或白藜芦醇敏感性,但抑制白藜芦醇诱导的轴突样过程形成。结论:我们的结果表明:(1)髓母细胞瘤组织和细胞系中SHP2,SOCS3和PIAS3总体减少; (2)PIAS3表达与STAT3激活的反相关性更高; (3)PIAS3对髓母细胞瘤具有良好的预后价值;(4)SOCS3参与白藜芦醇促进的髓母细胞瘤细胞轴突再生。

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