DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer

Abstract. Ferroptosis is a oxidative damage-dependent form of regulated cell death that has become an emerging target for disease prevention and treatment. Here, we show that dual-specificity phosphatase 1 (DUSP1), a phosphatase playing multiple roles in stress-signaling pathways, is a new repressor...

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Main Authors: Yangchun Xie, Feimei Kuang, Jiao Liu, Daolin Tang, MD, Rui Kang
Format: Article
Language:English
Published: Wolters Kluwer Health/LWW 2020-09-01
Series:Journal of Pancreatology
Online Access:http://journals.lww.com/10.1097/JP9.0000000000000054
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spelling doaj-692a4ef90e154584b3efeda4824a04662021-09-22T02:59:04ZengWolters Kluwer Health/LWWJournal of Pancreatology2096-56642577-35772020-09-013315416010.1097/JP9.0000000000000054202009000-00006DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancerYangchun XieFeimei KuangJiao LiuDaolin Tang, MDRui KangAbstract. Ferroptosis is a oxidative damage-dependent form of regulated cell death that has become an emerging target for disease prevention and treatment. Here, we show that dual-specificity phosphatase 1 (DUSP1), a phosphatase playing multiple roles in stress-signaling pathways, is a new repressor of ferroptosis in human pancreatic cancer cells. Several classical ferroptosis activators (eg, erastin and RSL3) induce the expression of DUSP1, but not other members of DUSP, which depends on extracellular signal-regulated protein kinases 1 and 2 (ERK1/2). Moreover, shRNA-mediated DUSP1 knockdown increases the anticancer activity of ferroptosis activators in pancreatic cancer cells through activating lipid peroxidation in vitro and in vivo. Importantly, DUSP1-mediated autophagy is responsible for lipid peroxidation-mediated ferroptotic cell death. Thus, the DUSP1-related ferroptotic pathway may represent a potential target for therapeutic intervention in pancreatic cancer.http://journals.lww.com/10.1097/JP9.0000000000000054
collection DOAJ
language English
format Article
sources DOAJ
author Yangchun Xie
Feimei Kuang
Jiao Liu
Daolin Tang, MD
Rui Kang
spellingShingle Yangchun Xie
Feimei Kuang
Jiao Liu
Daolin Tang, MD
Rui Kang
DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer
Journal of Pancreatology
author_facet Yangchun Xie
Feimei Kuang
Jiao Liu
Daolin Tang, MD
Rui Kang
author_sort Yangchun Xie
title DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer
title_short DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer
title_full DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer
title_fullStr DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer
title_full_unstemmed DUSP1 Blocks autophagy-dependent ferroptosis in pancreatic cancer
title_sort dusp1 blocks autophagy-dependent ferroptosis in pancreatic cancer
publisher Wolters Kluwer Health/LWW
series Journal of Pancreatology
issn 2096-5664
2577-3577
publishDate 2020-09-01
description Abstract. Ferroptosis is a oxidative damage-dependent form of regulated cell death that has become an emerging target for disease prevention and treatment. Here, we show that dual-specificity phosphatase 1 (DUSP1), a phosphatase playing multiple roles in stress-signaling pathways, is a new repressor of ferroptosis in human pancreatic cancer cells. Several classical ferroptosis activators (eg, erastin and RSL3) induce the expression of DUSP1, but not other members of DUSP, which depends on extracellular signal-regulated protein kinases 1 and 2 (ERK1/2). Moreover, shRNA-mediated DUSP1 knockdown increases the anticancer activity of ferroptosis activators in pancreatic cancer cells through activating lipid peroxidation in vitro and in vivo. Importantly, DUSP1-mediated autophagy is responsible for lipid peroxidation-mediated ferroptotic cell death. Thus, the DUSP1-related ferroptotic pathway may represent a potential target for therapeutic intervention in pancreatic cancer.
url http://journals.lww.com/10.1097/JP9.0000000000000054
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