Cytosolic acetyl-CoA synthetase affected tumor cell survival under hypoxia: the possible function in tumor acetyl-CoA/acetate metabolism

被引:93
|
作者
Yoshii, Yukie [1 ]
Furukawa, Takako [2 ]
Yoshii, Hiroshi [3 ]
Mori, Tetsuya [1 ]
Kiyono, Yasushi [1 ]
Waki, Atsuo [1 ]
Kobayashi, Masato [1 ]
Tsujikawa, Tetsuya [1 ]
Kudo, Takashi [1 ]
Okazawa, Hidehiko [1 ]
Yonekura, Yoshiharu [2 ]
Fujibayashi, Yasuhisa [1 ,2 ]
机构
[1] Univ Fukui, Biomed Imaging Res Ctr, Fukui 9101193, Japan
[2] Natl Inst Radiol Sci, Chiba 2638555, Japan
[3] Univ Fukui, Fac Med Sci, Dept Biochem & Bioinformat Sci, Fukui 9101193, Japan
来源
CANCER SCIENCE | 2009年 / 100卷 / 05期
基金
日本学术振兴会; 日本科学技术振兴机构;
关键词
COENZYME-A SYNTHETASE; ATP-CITRATE LYASE; O2 TENSION MEASUREMENTS; SACCHAROMYCES-CEREVISIAE; UTERINE CERVIX; CANCER-CELLS; OXYGENATION; LOCALIZATION; ACTIVATION; ACETATE;
D O I
10.1111/j.1349-7006.2009.01099.x
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Understanding tumor-specific metabolism under hypoxia is important to find novel targets for antitumor drug design. Here we found that tumor cells expressed higher levels of cytosolic acetyl-CoA synthetase (ACSS2) under hypoxia than normoxia. Knockdown of ACSS2 by RNA interference (RNAi) in tumor cells enhanced tumor cell death under long-term hypoxia in vitro. Our data also demonstrated that the ACSS2 suppression slowed tumor growth in vivo. These findings showed that ACSS2 plays a significant role in tumor cell survival under hypoxia and that ACSS2 would be a potential target for tumor treatment. Furthermore, we found that tumor cells excreted acetate and the quantity increased under hypoxia: the pattern of acetate excretion followed the expression pattern of ACSS2. Additionally, the ACSS2 knockdown led to a corresponding reduction in the acetate excretion in tumor cells. These results mean that ACSS2 can conduct the reverse reaction from acetyl-CoA to acetate in tumor cells, which indicates that ACSS2 is a bi-directional enzyme in tumor cells and that ACSS2 might play a buffering role in tumor acetyl-CoA/acetate metabolism. (Cancer Sci 2009; 100: 821-827).
引用
收藏
页码:821 / 827
页数:7
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