Chair of Pharmacology, Faculty of Science and Medicine, University of Fribourg, Fribourg, Switzerland.
Pharmacol Res. 2021 Mar;165:105393. doi: 10.1016/j.phrs.2020.105393. Epub 2021 Jan 20.
Hydrogen sulfide (HS) is an important endogenous gaseous transmitter mediator, which regulates a variety of cellular functions in autocrine and paracrine manner. The enzymes responsible for the biological generation of HS include cystathionine-β-synthase (CBS), cystathionine-γ-lyase (CSE) and 3-mercaptopyruvate sulfurtransferase (3-MST). Increased expression of these enzymes and overproduction of HS has been implicated in essential processes of various cancer cells, including the stimulation of metabolism, maintenance of cell proliferation and cytoprotection. Cancer cell identity is characterized by so-called "transition states". The progression from normal (epithelial) to transformed (mesenchymal) state is termed epithelial-to-mesenchymal transition (EMT) whereby epithelial cells lose their cell-to-cell adhesion capacity and gain mesenchymal characteristics. The transition process can also proceed in the opposite direction, and this process is termed mesenchymal-to-epithelial transition (MET). The current project was designed to determine whether inhibition of endogenous HS production in colon cancer cells affects the EMT/MET balance in vitro. Inhibition of HS biosynthesis in HCT116 human colon cancer cells was achieved either with aminooxyacetic acid (AOAA) or 2-[(4-hydroxy-6-methylpyrimidin-2-yl)sulfanyl]-1-(naphthalen-1-yl)ethan-1-one (HMPSNE). These inhibitors induced an upregulation of E-cadherin and Zonula occludens-1 (ZO-1) expression and downregulation of fibronectin expression, demonstrating that HS biosynthesis inhibitors can produce a pharmacological induction of MET in colon cancer cells. These actions were functionally reflected in an inhibition of cell migration, as demonstrated in an in vitro "scratch wound" assay. The mechanisms involved in the action of endogenously produced HS in cancer cells in promoting (or maintaining) EMT (or tonically inhibiting MET) relate, at least in part, in the induction of ATP citrate lyase (ACLY) protein expression, which occurs via upregulation of ACLY mRNA (via activation of the ACLY promoter). ACLY in turn, regulates the Wnt-β-catenin pathway, an essential regulator of the EMT/MET balance. Taken together, pharmacological inhibition of endogenous HS biosynthesis in cancer cells induces MET. We hypothesize that this may contribute to anti-cancer / anti-metastatic effects of HS biosynthesis inhibitors.
硫化氢 (HS) 是一种重要的内源性气体递质介质,以自分泌和旁分泌方式调节多种细胞功能。负责 HS 生物生成的酶包括胱硫醚-β-合酶 (CBS)、胱硫醚-γ-裂合酶 (CSE) 和 3-巯基丙酮酸硫转移酶 (3-MST)。这些酶的表达增加和 HS 的过度产生与各种癌细胞的重要过程有关,包括代谢的刺激、细胞增殖的维持和细胞保护。癌细胞的特性是所谓的“过渡状态”。从正常 (上皮) 到转化 (间充质) 的进展称为上皮-间充质转化 (EMT),其中上皮细胞丧失细胞间粘附能力并获得间充质特征。该转化过程也可以向相反方向进行,这个过程称为间充质-上皮转化 (MET)。本项目旨在确定抑制结肠癌细胞内源性 HS 产生是否会影响体外 EMT/MET 平衡。通过使用氨基氧乙酸 (AOAA) 或 2-[(4-羟基-6-甲基嘧啶-2-基)硫基]-1-(萘-1-基)乙酮 (HMPSNE) 抑制 HCT116 人结肠癌细胞中的 HS 生物合成。这些抑制剂诱导 E-钙粘蛋白和封闭蛋白-1 (ZO-1) 表达上调,纤连蛋白表达下调,表明 HS 生物合成抑制剂可在结肠癌细胞中产生 MET 的药理学诱导。这些作用在体外“划痕伤口”测定中抑制细胞迁移的功能上得到了反映。内源性 HS 在促进 (或维持) EMT 方面在癌细胞中的作用机制 (或通过抑制 MET 来维持) 至少部分涉及诱导三磷酸腺苷柠檬酸裂解酶 (ACLY) 蛋白表达,这是通过 ACLY mRNA 的上调 (通过激活 ACLY 启动子) 发生的。ACLY 反过来又调节 Wnt-β-连环蛋白途径,这是 EMT/MET 平衡的关键调节剂。综上所述,癌细胞内源性 HS 生物合成的药理学抑制诱导 MET。我们假设这可能有助于 HS 生物合成抑制剂的抗癌/抗转移作用。
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