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HSPB1 as a novel regulator of ferroptotic cancer cell death.

Oncogene (2015-03-03)
X Sun, Z Ou, M Xie, R Kang, Y Fan, X Niu, H Wang, L Cao, D Tang
要旨

Ferroptosis is an iron-dependent form of non-apoptotic cell death, but its molecular mechanism remains largely unknown. Here, we demonstrate that heat shock protein beta-1 (HSPB1) is a negative regulator of ferroptotic cancer cell death. Erastin, a specific ferroptosis-inducing compound, stimulates heat shock factor 1 (HSF1)-dependent HSPB1 expression in cancer cells. Knockdown of HSF1 and HSPB1 enhances erastin-induced ferroptosis, whereas heat shock pretreatment and overexpression of HSPB1 inhibits erastin-induced ferroptosis. Protein kinase C-mediated HSPB1 phosphorylation confers protection against ferroptosis by reducing iron-mediated production of lipid reactive oxygen species. Moreover, inhibition of the HSF1-HSPB1 pathway and HSPB1 phosphorylation increases the anticancer activity of erastin in human xenograft mouse tumor models. Our findings reveal an essential role for HSPB1 in iron metabolism with important effects on ferroptosis-mediated cancer therapy.

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過酸化水素 溶液, contains ~200 ppm acetanilide as stabilizer, 3 wt. % in H2O
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抗GAPDH抗体、マウスモノクローナル, clone GAPDH-71.1, purified from hybridoma cell culture
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スタウロスポリン 放線菌由来, Molecular Biology, ≥95% (HPLC)
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過酸化水素 溶液, purum p.a., ≥35% (RT)
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サイトカラシンD, Ready Made Solution, from Zygosporium mansonii, 5 mg/mL in DMSO
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シクロスポリンA, from Tolypocladium inflatum, ≥95% (HPLC), solid
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Z-VAD-FMK, solid
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シクロスポリンA, BioReagent, from Tolypocladium inflatum, Molecular Biology, ≥95%
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Gö 6983, ≥97%
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カルホスチンC Cladosporium cladosporioides由来, ≥90% (HPLC), powder
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1-デカンチオール, 99%