Chemical compounds that suppress hypoxia-induced stress granule formation enhance cancer drug sensitivity of human cervical cancer HeLa cells

Chemical compounds that suppress hypoxia-induced stress granule formation enhance cancer drug sensitivity of human cervical cancer HeLa cells

Abstract In eukaryotic cells, when exposed to certain types of stress including hypoxia, eIF2α is phosphorylated by several kinases including protein kinase R (PKR) and PKR-like endoplasmic reticulum kinase (PERK). Subsequently, protein translation is stopped and stress granules (SGs) are formed. Ca...

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Veröffentlicht in:Journal of biochemistry (Tokyo) 2018-11, Vol.164 (5), p.381-391
Hauptverfasser: Timalsina, Shikshya, Arimoto-Matsuzaki, Kyoko, Kitamura, Masami, Xu, Xiaoyin, Wenzhe, Qiu, Ishigami-Yuasa, Mari, Kagechika, Hiroyuki, Hata, Yutaka
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container_end_page 391
container_issue 5
container_start_page 381
container_title Journal of biochemistry (Tokyo)
container_volume 164
creator Timalsina, Shikshya
Arimoto-Matsuzaki, Kyoko
Kitamura, Masami
Xu, Xiaoyin
Wenzhe, Qiu
Ishigami-Yuasa, Mari
Kagechika, Hiroyuki
Hata, Yutaka
description Abstract In eukaryotic cells, when exposed to certain types of stress including hypoxia, eIF2α is phosphorylated by several kinases including protein kinase R (PKR) and PKR-like endoplasmic reticulum kinase (PERK). Subsequently, protein translation is stopped and stress granules (SGs) are formed. Cancer cells form SGs under hypoxia. SGs accumulate apoptosis-related molecules and play anti-apoptotic roles. Thus, hypoxia-induced SG formation contributes to drug resistance in cancer cells. For this reason, inhibition of SG formation is expected to be beneficial in cancer therapy. To prove this concept, chemical reagents that inhibit SG formation are required as experimental tools. We searched for chemical compounds that suppress SG formation and identified that β-estradiol, progesterone, and stanolone (hereafter described as EPS) inhibit SG formation in human cervical cancer HeLa cells. As it turned out, EPS block PKR but not PERK, thus fail to suppress SG formation in most cancer cells, where SGs are formed via PERK. Nevertheless, in this study, we used HeLa cells as a model and demonstrated that EPS block hypoxia-induced SG formation in HeLa cells and consequently reduce drug resistance that HeLa cells acquire under hypoxia. Our findings support that inhibition of SG formation is a useful method to control cancers.
doi_str_mv 10.1093/jb/mvy062
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title Chemical compounds that suppress hypoxia-induced stress granule formation enhance cancer drug sensitivity of human cervical cancer HeLa cells
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