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Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death

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Veröffentlicht in: Scientific reports 7(2017) Artikel-Nummer 43168, 12 Seiten
Personen und Körperschaften: Schroeder, Anne (VerfasserIn), Nicolay, Jan Peter (VerfasserIn)
Titel: Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death/ Anne Schroeder, Uwe Warnken, Daniel Röth, Karel D. Klika, Diana Vobis, Andrea Barnert, Fatmire Bujupi, Tina Oberacker, Martina Schnölzer, Jan P. Nicolay, Peter H. Krammer and Karsten Gülow
Format: E-Book-Kapitel
Sprache: Englisch
veröffentlicht:
24 February 2017
Gesamtaufnahme: : Scientific reports, 7(2017) Artikel-Nummer 43168, 12 Seiten
, volume:7
Quelle: Verbunddaten SWB
Lizenzfreie Online-Ressourcen
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contents Constitutively active NFκB promotes survival of many cancers, especially T-cell lymphomas and leukemias by upregulating antiapoptotic proteins such as inhibitors of apoptosis (IAPs) and FLICE-like inhibitory proteins (cFLIPs). IAPs and cFLIPs negatively regulate the ripoptosome, which mediates cell death in an apoptotic or necroptotic manner. Here, we demonstrate for the first time, that DMF antagonizes NFκB by suppressing Thioredoxin-1 (Trx1), a major regulator of NFκB transcriptional activity. DMF-mediated inhibition of NFκB causes ripoptosome formation via downregulation of IAPs and cFLIPs. In addition, DMF promotes mitochondrial Smac release and subsequent degradation of IAPs, further enhancing cell death in tumor cells displaying constitutive NFκB activity. Significantly, CTCL patients treated with DMF display substantial ripoptosome formation and caspase-3 cleavage in T-cells. DMF induces cell death predominantly in malignant or activated T-cells. Further, we show that malignant T-cells can die by both apoptosis and necroptosis, in contrast to resting T-cells, which are restricted to apoptosis upon DMF administration. In summary, our data provide new mechanistic insight in the regulation of cell death by targeting NFκB via Trx1 in cancer. Thus, interference with Trx1 activity is a novel approach for treatment of NFκB-dependent tumors.
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spelling Schroeder, Anne VerfasserIn (DE-588)1155615883 (DE-627)1017886784 (DE-576)501777962 aut, Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death Anne Schroeder, Uwe Warnken, Daniel Röth, Karel D. Klika, Diana Vobis, Andrea Barnert, Fatmire Bujupi, Tina Oberacker, Martina Schnölzer, Jan P. Nicolay, Peter H. Krammer and Karsten Gülow, 24 February 2017, 12, Text txt rdacontent, Computermedien c rdamedia, Online-Ressource cr rdacarrier, Gesehen am 06.04.2018, Constitutively active NFκB promotes survival of many cancers, especially T-cell lymphomas and leukemias by upregulating antiapoptotic proteins such as inhibitors of apoptosis (IAPs) and FLICE-like inhibitory proteins (cFLIPs). IAPs and cFLIPs negatively regulate the ripoptosome, which mediates cell death in an apoptotic or necroptotic manner. Here, we demonstrate for the first time, that DMF antagonizes NFκB by suppressing Thioredoxin-1 (Trx1), a major regulator of NFκB transcriptional activity. DMF-mediated inhibition of NFκB causes ripoptosome formation via downregulation of IAPs and cFLIPs. In addition, DMF promotes mitochondrial Smac release and subsequent degradation of IAPs, further enhancing cell death in tumor cells displaying constitutive NFκB activity. Significantly, CTCL patients treated with DMF display substantial ripoptosome formation and caspase-3 cleavage in T-cells. DMF induces cell death predominantly in malignant or activated T-cells. Further, we show that malignant T-cells can die by both apoptosis and necroptosis, in contrast to resting T-cells, which are restricted to apoptosis upon DMF administration. In summary, our data provide new mechanistic insight in the regulation of cell death by targeting NFκB via Trx1 in cancer. Thus, interference with Trx1 activity is a novel approach for treatment of NFκB-dependent tumors., Nicolay, Jan Peter 1981- VerfasserIn (DE-588)138614474 (DE-627)604867352 (DE-576)308046188 aut, Enthalten in Scientific reports [London] : Macmillan Publishers Limited, part of Springer Nature, 2011 7(2017) Artikel-Nummer 43168, 12 Seiten Online-Ressource (DE-627)663366712 (DE-600)2615211-3 (DE-576)346641179 2045-2322 nnns, volume:7 year:2017 extent:12, http://dx.doi.org/10.1038/srep43168 Verlag Resolving-System kostenfrei Volltext, https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5324128/ Verlag kostenfrei Volltext, http://dx.doi.org/10.1038/srep43168 LFER, LFER 2018-05-17T00:00:00Z
spellingShingle Schroeder, Anne, Nicolay, Jan Peter, Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death, Constitutively active NFκB promotes survival of many cancers, especially T-cell lymphomas and leukemias by upregulating antiapoptotic proteins such as inhibitors of apoptosis (IAPs) and FLICE-like inhibitory proteins (cFLIPs). IAPs and cFLIPs negatively regulate the ripoptosome, which mediates cell death in an apoptotic or necroptotic manner. Here, we demonstrate for the first time, that DMF antagonizes NFκB by suppressing Thioredoxin-1 (Trx1), a major regulator of NFκB transcriptional activity. DMF-mediated inhibition of NFκB causes ripoptosome formation via downregulation of IAPs and cFLIPs. In addition, DMF promotes mitochondrial Smac release and subsequent degradation of IAPs, further enhancing cell death in tumor cells displaying constitutive NFκB activity. Significantly, CTCL patients treated with DMF display substantial ripoptosome formation and caspase-3 cleavage in T-cells. DMF induces cell death predominantly in malignant or activated T-cells. Further, we show that malignant T-cells can die by both apoptosis and necroptosis, in contrast to resting T-cells, which are restricted to apoptosis upon DMF administration. In summary, our data provide new mechanistic insight in the regulation of cell death by targeting NFκB via Trx1 in cancer. Thus, interference with Trx1 activity is a novel approach for treatment of NFκB-dependent tumors.
swb_id_str 501778306
title Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death
title_auth Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death
title_full Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death Anne Schroeder, Uwe Warnken, Daniel Röth, Karel D. Klika, Diana Vobis, Andrea Barnert, Fatmire Bujupi, Tina Oberacker, Martina Schnölzer, Jan P. Nicolay, Peter H. Krammer and Karsten Gülow
title_fullStr Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death Anne Schroeder, Uwe Warnken, Daniel Röth, Karel D. Klika, Diana Vobis, Andrea Barnert, Fatmire Bujupi, Tina Oberacker, Martina Schnölzer, Jan P. Nicolay, Peter H. Krammer and Karsten Gülow
title_full_unstemmed Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death Anne Schroeder, Uwe Warnken, Daniel Röth, Karel D. Klika, Diana Vobis, Andrea Barnert, Fatmire Bujupi, Tina Oberacker, Martina Schnölzer, Jan P. Nicolay, Peter H. Krammer and Karsten Gülow
title_in_hierarchy Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death / Anne Schroeder, Uwe Warnken, Daniel Röth, Karel D. Klika, Diana Vobis, Andrea Barnert, Fatmire Bujupi, Tina Oberacker, Martina Schnölzer, Jan P. Nicolay, Peter H. Krammer and Karsten Gülow,
title_short Targeting Thioredoxin-1 by dimethyl fumarate induces ripoptosome-mediated cell death
title_sort targeting thioredoxin 1 by dimethyl fumarate induces ripoptosome mediated cell death
url http://dx.doi.org/10.1038/srep43168, https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5324128/