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H-rev107 regulates prostaglandin D2 synthase-mediated suppression of cellular invasion in testicular cancer cells

机译:H-rev107调节前列腺素D2合酶介导的睾丸癌细胞侵袭抑制

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BackgroundH-rev107 is a member of the HREV107 type II tumor suppressor gene family which includes H-REV107, RIG1, and HRASLS. H-REV107 has been shown to express at high levels in differentiated tissues of post-meiotic testicular germ cells. Prostaglandin D2 (PGD2) is conjectured to induce SRY-related high-mobility group box 9 (SOX9) expression and subsequent Sertoli cell differentiation. To date, the function of H-rev107 in differentiated testicular cells has not been well defined.ResultsIn the study, we found that H-rev107 was co-localized with prostaglandin D2 synthase (PTGDS) and enhanced the activity of PTGDS, resulting in increase of PGD2 production in testis cells. Furthermore, when H-rev107 was expressed in human NT2/D1 testicular cancer cells, cell migration and invasion were inhibited. Also, silencing of PTGDS would reduce H-rev107-mediated increase in PGD2, cAMP, and SOX9. Silencing of PTGDS or SOX9 also alleviated H-rev107-mediated suppression of cell migration and invasion.ConclusionsThese results revealed that H-rev107, through PTGDS, suppressed cell migration and invasion. Our data suggest that the PGD2-cAMP-SOX9 signal pathway might play an important role in H-rev107-mediated cancer cell invasion in testes.
机译:背景H-rev107是HREV107 II型肿瘤抑制基因家族的成员,该家族包括H-REV107,RIG1和HRASLS。 H-REV107已显示在减数分裂后睾丸生殖细胞的分化组织中高水平表达。推测前列腺素D2(PGD2)诱导SRY相关的高迁移率族框9(SOX9)表达和随后的支持细胞分化。迄今为止,H-rev107在分化的睾丸细胞中的功能尚未得到很好的定义。结果在研究中,我们发现H-rev107与前列腺素D2合酶(PTGDS)共定位并增强了PTGDS的活性,从而导致睾丸细胞中PGD2的产生此外,当H-rev107在人NT2 / D1睾丸癌细胞中表达时,细胞迁移和侵袭被抑制。同样,沉默PTGDS可以减少H-rev107介导的PGD2,cAMP和SOX9的增加。 PTGDS或SOX9的沉默也减轻了H-rev107介导的细胞迁移和侵袭的抑制。结论这些结果表明H-rev107通过PTGDS抑制了细胞迁移和侵袭。我们的数据表明,PGD2-cAMP-SOX9信号通路可能在H-rev107介导的睾丸癌细胞入侵中发挥重要作用。

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