Differential induction of C6 glioma apoptosis and autophagy by 3β-hydroxysteroid-indolamine conjugates

IF 2.1 4区医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Steroids Pub Date : 2023-10-10 DOI:10.1016/j.steroids.2023.109326

Jan Panada , Valeriya Klopava , Tatsiana Kulahava , Siarhei Koran , Yaroslav Faletrov , Nina Frolova , Elena Fomina , Vladimir Shkumatov

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Abstract

In a previous work, we reported the synthesis of four novel indole steroids and their effect on rat C6 glioma proliferation in vitro. The steroid derived from dehydroepiandrosterone and tryptamine (IS-1) was the most active (52 % inhibition at 10 µM), followed by one of the epimers derived from pregnenolone and tryptamine (IS-3, 36 % inhibition at 10 µM). By contrast, the steroid derived from estrone and tryptamine (IS-2) showed negligible activity at 10 µM. No necrosis, increase in intracellular calcium or ROS levels was observed. In this work, the effect of compounds on C6 glioma apoptosis and autophagy is examined by fluorimetry and fluorescent microscopy. The IS-3 epimers disrupt the mitochondrial membrane potential and induce apoptosis in vitro moderately whereas IS-1 and IS-2 do not. However, IS-1 produces a large increase in monodansylcadaverine-positive autophagic vesicles over 24 h. The antiproliferative effect of indole steroids is ameliorated by autophagy inhibitor hydroxychloroquine, suggesting an autophagy-dependent mechanism of cell death.

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3β-羟基类固醇吲哚胺偶联物对C6胶质瘤细胞凋亡和自噬的差异诱导。

在先前的工作中，我们报道了四种新型吲哚类固醇的合成及其对大鼠C6神经胶质瘤体外增殖的影响。脱氢表雄酮和色胺衍生的类固醇（IS-1）最具活性（52 % 10时的抑制 µM），然后是一种衍生自孕烯醇酮和色胺的差向异构体（IS-3，36 % 10时的抑制 µM）。相反，从雌酮和色胺衍生的类固醇（IS-2）在10 µM。未观察到坏死、细胞内钙或ROS水平增加。在这项工作中，化合物对C6神经胶质瘤细胞凋亡和自噬的影响是通过荧光法和荧光显微镜检查的。IS-3差向异构体在体外适度破坏线粒体膜电位并诱导细胞凋亡，而IS-1和IS-2则不然。然而，IS-1在24小时内产生单丹酰尸胺阳性自噬小泡的大量增加 h.自噬抑制剂羟氯喹改善了吲哚类固醇的抗增殖作用，这表明细胞死亡的自噬依赖性机制。

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来源期刊

Steroids 医学-内分泌学与代谢

CiteScore

5.10

自引率

3.70%

发文量

120

审稿时长

73 days

期刊介绍： STEROIDS is an international research journal devoted to studies on all chemical and biological aspects of steroidal moieties. The journal focuses on both experimental and theoretical studies on the biology, chemistry, biosynthesis, metabolism, molecular biology, physiology and pharmacology of steroids and other molecules that target or regulate steroid receptors. Manuscripts presenting clinical research related to steroids, steroid drug development, comparative endocrinology of steroid hormones, investigations on the mechanism of steroid action and steroid chemistry are all appropriate for submission for peer review. STEROIDS publishes both original research and timely reviews. For details concerning the preparation of manuscripts see Instructions to Authors, which is published in each issue of the journal.