The sphingosine kinase 2 inhibitors ABC294640 and K145 elevate (dihydro)sphingosine 1-phosphate levels in various cells.

IF 5 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of Lipid Research Pub Date : 2024-10-01 Epub Date: 2024-08-23 DOI:10.1016/j.jlr.2024.100631
Agata Prell, Dominik Wigger, Andrea Huwiler, Fabian Schumacher, Burkhard Kleuser
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Abstract

Sphingosine kinases (SphKs), enzymes that produce the bioactive lipids dihydrosphingosine 1-phosphate (dhS1P) and sphingosine 1-phosphate (S1P), are associated with various diseases, including cancer and infections. For this reason, a number of SphK inhibitors have been developed. Although off-target effects have been described for selected agents, SphK inhibitors are mostly used in research without monitoring the effects on the sphingolipidome. We have now investigated the effects of seven commonly used SphK inhibitors (5c, ABC294640 (opaganib), N,N-dimethylsphingosine, K145, PF-543, SLM6031434, and SKI-II) on profiles of selected sphingolipids in Chang, HepG2, and human umbilical vein endothelial cells. While we observed the expected (dh)S1P reduction for N,N-dimethylsphingosine, PF-543, SKI-II, and SLM6031434, 5c showed hardly any effect. Remarkably, for K145 and ABC294640, both reported to be specific for SphK2, we observed dose-dependent strong increases in dhS1P and S1P across cell lines. Compensatory effects of SphK1 could be excluded, as this observation was also made in SphK1-deficient HK-2 cells. Furthermore, we observed effects on dihydroceramide desaturase activity for all inhibitors tested, as has been previously noted for ABC294640 and SKI-II. In additional mechanistic studies, we investigated the massive increase of dhS1P and S1P after short-term cell treatment with ABC294640 and K145 in more detail. We found that both compounds affect sphingolipid de novo synthesis, with 3-ketodihydrosphingosine reductase and dihydroceramide desaturase as their targets. Our study indicates that none of the seven SphK inhibitors tested was free of unexpected on-target and/or off-target effects. Therefore, it is important to monitor cellular sphingolipid profiles when SphK inhibitors are used in mechanistic studies.

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鞘氨醇激酶 2 抑制剂 ABC294640 和 K145 可提高各种细胞中的 1-磷酸(二氢)鞘氨醇水平。
鞘氨醇激酶(SphKs)是产生生物活性脂质二氢鞘氨醇 1-磷酸酯(dhS1P)和鞘氨醇 1-磷酸酯(S1P)的酶,与癌症和感染等多种疾病有关。因此,人们开发了许多 SphK 抑制剂。虽然对某些药物的脱靶效应已有描述,但 SphK 抑制剂大多用于研究,而没有监测对鞘脂群的影响。我们现在研究了七种常用的 SphK 抑制剂(5c、ABC294640(opaganib)、DMS、K145、PF-543、SLM6031434 和 SKI-II)对 Chang、HepG2 和 HUVEC 细胞中特定鞘脂的影响。虽然我们观察到 DMS、PF-543、SKI-II 和 SLM6031434 的 (dh)S1P 减少,但 5c 几乎没有任何影响。值得注意的是,对于 K145 和 ABC294640(据报道两者对 SphK2 都有特异性),我们观察到不同细胞系的 dhS1P 和 S1P 都出现了剂量依赖性的强烈升高。可以排除 SphK1 的补偿效应,因为在 SphK1 缺失的 HK-2 细胞中也观察到了这种效应。此外,我们还观察到所有测试的抑制剂都对二氢甘油酰胺去饱和酶(DEGS)的活性有影响,这与之前对 ABC294640 和 SKI-II 的观察结果相同。在其他机理研究中,我们更详细地调查了用 ABC294640 和 K145 对细胞进行短期处理后 dhS1P 和 S1P 的大量增加。我们发现,这两种化合物都会影响鞘脂的从头合成,3-酮二氢鞘氨醇还原酶和 DEGS 是它们的靶点。我们的研究强调了在机理研究中使用 SphK 抑制剂时监测细胞鞘脂特征的紧迫性,因为所测试的七种 SphK 抑制剂中没有一种不会产生意想不到的靶上和/或脱靶效应。
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来源期刊
Journal of Lipid Research
Journal of Lipid Research 生物-生化与分子生物学
CiteScore
11.10
自引率
4.60%
发文量
146
审稿时长
41 days
期刊介绍: The Journal of Lipid Research (JLR) publishes original articles and reviews in the broadly defined area of biological lipids. We encourage the submission of manuscripts relating to lipids, including those addressing problems in biochemistry, molecular biology, structural biology, cell biology, genetics, molecular medicine, clinical medicine and metabolism. Major criteria for acceptance of articles are new insights into mechanisms of lipid function and metabolism and/or genes regulating lipid metabolism along with sound primary experimental data. Interpretation of the data is the authors’ responsibility, and speculation should be labeled as such. Manuscripts that provide new ways of purifying, identifying and quantifying lipids are invited for the Methods section of the Journal. JLR encourages contributions from investigators in all countries, but articles must be submitted in clear and concise English.
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