The direct STAT3 inhibitor 6-ethoxydihydrosanguinarine exhibits anticancer activity in gastric cancer

Xue-wen Liu, Xin Jin, Hongling Ou, Chen Qian, Hui Wu, C. Zuo, Yuliang Ren, Miaoxin Fu, Te Zhang, Liang Zhang, Y. Si, Ying Liu
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引用次数: 6

Abstract

Signal transducer and activator of transcription 3 (STAT3) plays a key role in promoting tumor malignant progression. Suppression of hyperactivated STAT3 signaling has emerged as a potential therapeutic strategy for many cancer types. In this study, the effect of 6-ethoxydihydrosanguinarine (6-EDS), a secondary transformation product formed from dihydrosanguinarine, isolated from Macleaya (Papaveraceae), was evaluated in gastric cancer (GC). We demonstrated that 6-EDS inhibited the survival, migration, and invasiveness of GC cells in vitro. Moreover, 6-EDS inhibited STAT3 phosphorylation and transcriptional activity, thus suppressing the mRNA expression of downstream target genes associated with the malignant survival, migration, and invasiveness of GC cells. Molecular docking indicated that 6-EDS directly bound the SH2 domain of STAT3. Molecular dynamics simulations suggested that 6-EDS inhibited the binding of phosphorylated and non-phosphorylated STAT3 to target DNA. Cellular thermal-shift assays and microscale thermophoresis further confirmed the direct binding of 6-EDS to STAT3. Site-directed mutagenesis indicated that the S611 residue in the SH2 domain of STAT3 is critical for 6-EDS binding. In vivo, 6-EDS decreased tumor growth in xenografted nude mice by blocking STAT3 signaling. These findings indicated that 6-EDS, a direct STAT3 inhibitor, may be a potent anticancer candidate for GC therapy.
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STAT3直接抑制剂6-乙氧基二氢血根碱对癌症具有抗癌活性
信号换能器和转录激活因子3 (STAT3)在促进肿瘤恶性进展中起关键作用。抑制过度激活的STAT3信号已成为许多癌症类型的潜在治疗策略。本研究评价了从木瓜科植物中分离得到的二氢血碱二级转化产物6-乙氧基二氢血碱(6-EDS)对胃癌(GC)的作用。我们证明了6-EDS在体外抑制GC细胞的存活、迁移和侵袭性。此外,6-EDS抑制STAT3的磷酸化和转录活性,从而抑制与胃癌细胞恶性存活、迁移和侵袭性相关的下游靶基因mRNA的表达。分子对接表明,6-EDS直接结合STAT3的SH2结构域。分子动力学模拟表明,6-EDS抑制磷酸化和非磷酸化STAT3与靶DNA的结合。细胞热移实验和微尺度热电泳进一步证实了6-EDS与STAT3的直接结合。定点突变表明,STAT3 SH2结构域的S611残基对6-EDS结合至关重要。在体内,6-EDS通过阻断STAT3信号传导抑制异种移植裸鼠的肿瘤生长。这些发现表明,6-EDS是一种直接的STAT3抑制剂,可能是一种有效的胃癌治疗候选药物。
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