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预防性香叶基香叶酸(GGA)诱导人肝癌细胞系发生不完全自噬反应。

Induction of an incomplete autophagic response by cancer-preventive geranylgeranoic acid (GGA) in a human hepatoma-derived cell line.

机构信息

Molecular and Cellular Biology, Graduate School of Human Health Sciences, Siebold University of Nagasaki, Nagasaki, Japan.

出版信息

Biochem J. 2011 Nov 15;440(1):63-71. doi: 10.1042/BJ20110610.

DOI:10.1042/BJ20110610
PMID:21787360
Abstract

GGA (geranylgeranoic acid) is a natural polyprenoic acid, derivatives of which has been shown to prevent second primary hepatoma. GGA induces mitochondria-mediated PCD (programmed cell death), which may be relevant to cancer prevention. To gain further insights into GGA-induced PCD, autophagy processes were examined in human hepatoma-derived HuH-7 cells. Treatment of HuH-7/GFP (green fluorescent protein)-LC3 cells with GGA induced green fluorescent puncta in the cytoplasm within 30 min and their massive accumulation at 24 h. After 15 min of GGA treatment, a burst of mitochondrial superoxide production occurred and LC3β-I was appreciably converted into LC3β-II. GGA-induced early stages of autophagy were unequivocally confirmed by electron-microscopic observation of early/initial autophagic vacuoles. On the other hand, LC3β-II as well as p62/SQSTM1 (sequestosome 1) continuously accumulated and co-localized in the cytoplasmic puncta after GGA treatment. Furthermore, GGA treatment of HuH-7/mRFP (monomeric red fluorescent protein)-GFP-LC3 cells showed yellow fluorescent puncta, whereas glucose deprivation of the cells gave red fluorescent puncta. These results strongly suggest that GGA induces the initial phase of autophagy, but blocks the maturation process of autolysosomes or late stages of autophagy, insomuch that GGA provides substantial accumulation of autophagosomes under serum-starvation conditions in human hepatoma cells.

摘要

香叶基香叶酸(GGA)是一种天然的多萜烯酸,其衍生物已被证明可预防第二原发性肝癌。GGA 诱导线粒体介导的细胞程序性死亡(PCD),这可能与癌症预防有关。为了更深入地了解 GGA 诱导的 PCD,在人肝癌衍生的 HuH-7 细胞中检查了自噬过程。用 GGA 处理 HuH-7/GFP(绿色荧光蛋白)-LC3 细胞在 30 分钟内诱导细胞质中出现绿色荧光斑点,并在 24 小时时大量积累。在用 GGA 处理 15 分钟后,线粒体中超氧阴离子的产生爆发,LC3β-I 明显转化为 LC3β-II。用电子显微镜观察早期/初始自噬小泡,明确证实了 GGA 诱导的自噬早期阶段。另一方面,在用 GGA 处理后,LC3β-II 以及 p62/SQSTM1(自噬体 1)不断积累并在细胞质斑点中共定位。此外,在用 GGA 处理 HuH-7/mRFP(单体红色荧光蛋白)-GFP-LC3 细胞后显示黄色荧光斑点,而细胞的葡萄糖剥夺则给出红色荧光斑点。这些结果强烈表明 GGA 诱导自噬的初始阶段,但阻止自噬溶酶体的成熟过程或自噬的晚期阶段,以至于 GGA 在人肝癌细胞的血清饥饿条件下提供大量自噬体的积累。

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