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Melatonin affects the dynamic steady-state equilibrium of estrogen sulfates in human umbilical vein endothelial cells by regulating the balance between estrogen sulfatase and sulfotransferase

机译:褪黑素通过调节雌激素硫酸酯酶和磺基转移酶之间的平衡来影响人脐静脉内皮细胞中硫酸雌激素的动态稳态平衡

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摘要

Melatonin is known to reduce the growth of endocrine-responsive breast cancers by interacting with estrogen signaling pathways. Estrogens play an important role in breast cancer, but also in various types of tissues, including vascular tissue. Estrogen sulfatase (STS) converts inactive estrogen sulfates into active estrogens, whereas estrogen sulfotransferase (EST) sulfonates estrogens to estrogen sulfates. Therefore, STS and EST are considered to be involved in the regulation of local estrogen levels in hormone‑dependent tumors and in non-pathologic tissues, such as those of the vascular system. Estrogens have a major impact on the vasculature, influencing vascular function, the expression of adhesion proteins, angiogenesis and the inflammatory state. In this study, we investigated the status of STS and EST in human umbilical vein endothelial cells (HUVECs) and the modulatory effects of melatonin. Both STS and EST were highly expressed in the HUVECs. The enzymatic activity correlated with the expression levels in these cells. Our findings also demonstrated that melatonin, at physiological concentrations, modulated the synthesis and transformation of biologically active estrogens in HUVECs through the inhibition of STS activity and expression, and the stimulation of EST activity and expression. Since melatonin decreased the STS levels and increased the EST levels, it modified the dynamic steady‑state equilibrium of estrogen sulfates by increasing the inactive estrogen levels and decreasing the active estrogen levels. Therefore, melatonin may modulate the known different biological actions of estrogens in endothelial cells, as well as in estrogen‑dependent tumors and non-pathologic tissues.
机译:众所周知,褪黑激素可通过与雌激素信号传导途径相互作用来减少内分泌反应性乳腺癌的生长。雌激素在乳腺癌中也起着重要作用,而且在包括血管组织在内的各种类型的组织中也起着重要的作用。雌激素硫酸酯酶(STS)将无活性的雌激素硫酸盐转化为活性雌激素,而雌激素磺基转移酶(EST)将雌激素磺化为雌激素硫酸盐。因此,STS和EST被认为参与激素依赖性肿瘤和非病理组织(如血管系统组织)中局部雌激素水平的调节。雌激素对脉管系统有重大影响,影响血管功能,粘附蛋白的表达,血管生成和炎症状态。在这项研究中,我们调查了人脐静脉内皮细胞(HUVECs)中STS和EST的状态以及褪黑激素的调节作用。 STS和EST在HUVEC中都高度表达。酶活性与这些细胞中的表达水平相关。我们的研究结果还表明,褪黑素在生理浓度下可通过抑制STS活性和表达以及刺激EST活性和表达来调节HUVEC中生物活性雌激素的合成和转化。由于褪黑激素降低了STS水平并提高了EST水平,因此它通过增加非活性雌激素水平和降低活性雌激素水平来改变硫酸雌激素的动态稳态平衡。因此,褪黑激素可以调节内皮细胞以及雌激素依赖性肿瘤和非病理组织中雌激素的已知不同生物学作用。

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