A search for inhibitors of the IL-6-mediated signal transduction in HepG2 cells using secreted alkaline phosphatase (SEAP) as reporter gene resulted in the isolation of galiellalactone (1) from fermentations of the ascomycete strain A111-95. Galiellalactone inhibits the IL-6-induced SEAP expression with IC(50) values of 250-500 nM by blocking the binding of the activated Stat3 dimers to their DNA binding sites without inhibiting the tyrosine and serine phosphorylation of the Stat3 transcription factor. Due to its selective activity, galiellalactone may serve as a lead compound for the development of new therapeutic agents for diseases originating from the inappropriate expression of IL-6 and as molecular tool to dissect the JAK/STAT pathways.

译文

:使用分泌的碱性磷酸酶(SEAP)作为报告基因寻找HepG2细胞中IL-6介导的信号转导抑制剂,从而从子囊菌菌株A111-95的发酵中分离了加利拉内酯(1)。 Galiellalactone通过阻止激活的Stat3二聚体与其DNA结合位点的结合,而不会抑制Stat3转录因子的酪氨酸和丝氨酸磷酸化,从而抑制IL-6诱导的SEAP表达,其IC(50)值为250-500 nM。由于加利拉内酯的选择性活性,它可以作为开发新型治疗剂的先导化合物,用于治疗因IL-6表达不当而引起的疾病,并可以作为解剖JAK / STAT途径的分子工具。

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