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在哺乳动物细胞中,明确的证据表明香叶基香叶酸是由甲羟戊酸生物合成的。

Unequivocal evidence for endogenous geranylgeranoic acid biosynthesized from mevalonate in mammalian cells.

机构信息

Molecular and Cellular Biology, Graduate School of Human Health Science, University of Nagasaki, Nagayo, Nagasaki, Japan

Molecular and Cellular Biology, Graduate School of Human Health Science, University of Nagasaki, Nagayo, Nagasaki, Japan.

出版信息

J Lipid Res. 2019 Mar;60(3):579-593. doi: 10.1194/jlr.M090548. Epub 2019 Jan 8.

Abstract

Geranylgeranoic acid (GGA) has been reported to induce autophagic cell death via upregulation of lipid-induced unfolded protein response in several human hepatoma-derived cell lines, and its 4,5-didehydro derivative has been developed as a preventive agent against second primary hepatoma in clinical trials. We have previously reported that GGA is a natural diterpenoid synthesized in several medicinal herbs. Here, we provide unequivocal evidence for de novo GGA biosynthesis in mammals. First, with normal male Wistar rats, the levels of GGA in liver were found to be far greater than those in other organs analyzed. Second, we demonstrated the metabolic GGA labeling from the C-labeled mevalonolactone in the human hepatoma-derived cell line, HuH-7. Isotopomer spectral analysis revealed that approximately 80% of the cellular GGA was newly synthesized from mevalonate (MVA) in 12 h and the acid picked up preexisting farnesyl diphosphate (FPP) and geranylgeranyl diphosphate (GGPP), suggesting that GGA is derived from FPP and GGPP through the MVA pathway. Third, zaragozic acid A, a squalene synthase inhibitor, induced dose-dependent upregulation of endogenous GGA content in HuH-7 cells and their concomitant cell death. These results strongly suggest that a cancer-preventive GGA is biosynthesized via the MVA pathway in mammals.

摘要

香叶基香叶酸(GGA)已被报道可通过上调几种人肝癌衍生细胞系中的脂诱导未折叠蛋白反应诱导自噬性细胞死亡,其 4,5-二脱氢衍生物已被开发为临床试验中预防第二原发性肝癌的药物。我们之前曾报道过,GGA 是几种药用植物中合成的天然二萜。在这里,我们提供了哺乳动物中 GGA 从头生物合成的明确证据。首先,在正常雄性 Wistar 大鼠中,肝脏中的 GGA 水平远远高于分析的其他器官中的水平。其次,我们在人肝癌衍生细胞系 HuH-7 中证明了代谢 GGA 对 C 标记的甲羟戊酸内酯的标记。同位素峰谱分析表明,大约 80%的细胞 GGA 在 12 小时内是从头从甲羟戊酸(MVA)合成的,酸提取了预先存在的法呢基二磷酸(FPP)和香叶基二磷酸(GGPP),表明 GGA 是通过 MVA 途径从 FPP 和 GGPP 衍生而来的。第三,角鲨烯合酶抑制剂扎拉格酸 A 诱导 HuH-7 细胞中内源性 GGA 含量的剂量依赖性上调及其伴随的细胞死亡。这些结果强烈表明,通过哺乳动物的 MVA 途径生物合成了一种具有抗癌作用的 GGA。

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