Einzeltreffer — DigiBib

Necroptosis is a regulated necrotic cell death pathway involved in development and disease. Its signaling cascade results in the formation of disulfide bond-dependent amyloid-like polymers of mixed lineage kinase domain-like protein (MLKL), which mediate proinflammatory cell membrane disruption. We screened compound libraries provided by the National Cancer Institute and identified a small-molecule inhibitor of necroptosis named necroptosis-blocking compound 1 (NBC1). Biotin-labeled NBC1 specifically conjugates to heat shock protein Hsp70. NBC1 and PES-Cl, a known Hsp70 substrate-binding inhibitor, block the formation of MLKL polymers, but not MLKL tetramers in necroptosis-induced cells. In vitro , recombinant Hsp70 interacts with the N-terminal domain (NTD) of MLKL and promotes NTD polymerization, which has been shown to mediate the cell killing activity. Furthermore, the substrate-binding domain (SBD) of Hsp70 is sufficient to promote MLKL polymerization. NBC1 covalently conjugates cysteine 574 and cysteine 603 of the SBD to block its function. In addition, an SBD mutant with both cysteines mutated to serines loses its ability to promote MLKL polymerization. Interestingly, knockdown of Hsp70 in cells leads to MLKL destabilization, suggesting that MLKL might also be a client protein of Hsp70. In summary, using NBC1, an inhibitor of necroptosis, we identified Hsp70 as a molecular chaperone performing dual functions in necroptosis. It stabilizes MLKL protein under normal condition and promotes MLKL polymerization through its substrate-binding domain during necroptosis.

Competing Interests: The authors declare no competing interest.

Titel:	Necroptosis-blocking compound NBC1 targets heat shock protein 70 to inhibit MLKL polymerization and necroptosis.
Autor/in / Beteiligte Person:	Johnston, AN ; Ma, Y ; Liu, H ; Liu, S ; Hanna-Addams, S ; Chen, S ; Chen, C ; Wang, Z
Link:	Full Text Finder (Volltext)
Zeitschrift:	Proceedings of the National Academy of Sciences of the United States of America, Jg. 117 (2020-03-24), Heft 12, S. 6521-6530
Veröffentlichung:	Washington, DC : National Academy of Sciences, 2020
Medientyp:	academicJournal
ISSN:	1091-6490 (electronic)
DOI:	10.1073/pnas.1916503117
Schlagwort:	Animals Binding Sites Cell Line Gene Knockdown Techniques HSP70 Heat-Shock Proteins chemistry HSP70 Heat-Shock Proteins genetics HT29 Cells Humans Molecular Structure Mutation Piperidines chemistry Protein Binding Protein Domains Protein Kinases chemistry Protein Kinases genetics Protein Multimerization drug effects Small Molecule Libraries chemistry Small Molecule Libraries pharmacology HSP70 Heat-Shock Proteins antagonists & inhibitors HSP70 Heat-Shock Proteins metabolism Necroptosis drug effects Piperidines pharmacology Protein Kinases metabolism
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, N.I.H., Extramural; Research Support, Non-U.S. Gov't Language: English [Proc Natl Acad Sci U S A] 2020 Mar 24; Vol. 117 (12), pp. 6521-6530. <i>Date of Electronic Publication: </i>2020 Mar 10. MeSH Terms: HSP70 Heat-Shock Proteins / antagonists & inhibitors ; HSP70 Heat-Shock Proteins / metabolism ; Necroptosis / drug effects ; Piperidines / pharmacology ; Protein Kinases / *metabolism ; Animals ; Binding Sites ; Cell Line ; Gene Knockdown Techniques ; HSP70 Heat-Shock Proteins / chemistry ; HSP70 Heat-Shock Proteins / genetics ; HT29 Cells ; Humans ; Molecular Structure ; Mutation ; Piperidines / chemistry ; Protein Binding ; Protein Domains ; Protein Kinases / chemistry ; Protein Kinases / genetics ; Protein Multimerization / drug effects ; Small Molecule Libraries / chemistry ; Small Molecule Libraries / pharmacology References: J Biol Chem. 2017 Oct 20;292(42):17514-17524. (PMID: 28878015) ; J Nat Sci. 2018 Jul;4(7):. (PMID: 30294675) ; Carcinogenesis. 2013 Jun;34(6):1181-8. (PMID: 23563090) ; Proc Natl Acad Sci U S A. 2015 Apr 21;112(16):5017-22. (PMID: 25852146) ; J Med Chem. 2017 Feb 9;60(3):839-885. (PMID: 27996267) ; Cell Death Differ. 2018 Mar;25(3):486-541. (PMID: 29362479) ; Cell Death Dis. 2016 Mar 03;7:e2126. (PMID: 26938299) ; Cell. 2012 Jan 20;148(1-2):228-43. (PMID: 22265414) ; Nat Rev Mol Cell Biol. 2017 Feb;18(2):127-136. (PMID: 27999438) ; Mol Cell. 2014 Apr 10;54(1):133-146. (PMID: 24703947) ; Trends Biochem Sci. 2014 Dec;39(12):587-93. (PMID: 25455759) ; Cancer Chemother Pharmacol. 2010 Aug;66(3):535-45. (PMID: 20012863) ; Proc Natl Acad Sci U S A. 2012 Jul 31;109(31):12479-84. (PMID: 22802614) ; PLoS Biol. 2017 Jun 26;15(6):e2002711. (PMID: 28650960) ; J Cell Sci. 2018 Apr 13;131(8):. (PMID: 29654159) ; Nature. 2011 Jul 20;475(7356):324-32. (PMID: 21776078) ; Genes Dev. 2018 Mar 1;32(5-6):327-340. (PMID: 29593066) ; Nature. 2015 Aug 13;524(7564):247-51. (PMID: 26245380) ; Annu Rev Immunol. 2015;33:79-106. (PMID: 25493335) ; Methods Mol Biol. 2018;1709:371-396. (PMID: 29177673) ; Cell Mol Life Sci. 2005 Mar;62(6):670-84. (PMID: 15770419) ; Nature. 2015 Jan 15;517(7534):311-20. (PMID: 25592536) ; Mol Cell. 2016 Oct 20;64(2):236-250. (PMID: 27746017) ; Mol Cancer Res. 2018 Jan;16(1):58-68. (PMID: 28970360) ; Nat Struct Mol Biol. 2011 Mar;18(3):345-51. (PMID: 21278757) ; J Vis Exp. 2018 Apr 26;(134):. (PMID: 29757289) ; Mol Cell. 2015 Sep 3;59(5):781-93. (PMID: 26300264) ; Mol Cancer Res. 2013 Mar;11(3):219-29. (PMID: 23303345) ; Cell. 2009 Jun 12;137(6):1100-11. (PMID: 19524512) ; Nat Immunol. 2000 Dec;1(6):489-95. (PMID: 11101870) ; Cell Rep. 2014 May 22;7(4):971-81. (PMID: 24813885) ; PLoS One. 2013 Nov 12;8(11):e78443. (PMID: 24265689) ; Cell Death Dis. 2016 Feb 11;7:e2089. (PMID: 26866270) ; Cell Chem Biol. 2016 Feb 18;23(2):257-266. (PMID: 27028885) ; Structure. 2014 Oct 7;22(10):1489-500. (PMID: 25220470) ; Virology. 2015 May;479-480:160-6. (PMID: 25819165) ; Cell. 2012 Jul 20;150(2):339-50. (PMID: 22817896) ; Cell Death Dis. 2016 Jan 14;7:e2051. (PMID: 26775703) ; Proc Natl Acad Sci U S A. 2017 Sep 5;114(36):E7450-E7459. (PMID: 28827318) ; Cell. 2012 Jan 20;148(1-2):213-27. (PMID: 22265413) ; Cell. 2009 Jun 12;137(6):1112-23. (PMID: 19524513) ; Nat Chem Biol. 2005 Jul;1(2):112-9. (PMID: 16408008) ; Science. 2009 Jul 17;325(5938):332-6. (PMID: 19498109) ; Proc Natl Acad Sci U S A. 2014 Oct 21;111(42):15072-7. (PMID: 25288762) ; Proc Natl Acad Sci U S A. 2012 Apr 3;109(14):5322-7. (PMID: 22421439) ; Cell Res. 2014 Jan;24(1):105-21. (PMID: 24366341) ; Nat Cell Biol. 2014 Jan;16(1):55-65. (PMID: 24316671) Grant Information: R01 GM120502 United States GM NIGMS NIH HHS; T32 GM008203 United States GM NIGMS NIH HHS; TL1 TR001104 United States TR NCATS NIH HHS Contributed Indexing: Keywords: Hsp70; MLKL; NBC1; necroptosis; polymerization Substance Nomenclature: 0 (HSP70 Heat-Shock Proteins) ; 0 (Piperidines) ; 0 (Small Molecule Libraries) ; 0 (necroptosis-blocking compound NBC1) ; EC 2.7.- (MLKL protein, human) ; EC 2.7.- (Protein Kinases) Entry Date(s): Date Created: 20200312 Date Completed: 20200810 Latest Revision: 20210709 Update Code: 20231215 PubMed Central ID: PMC7104336

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Necroptosis-blocking compound NBC1 targets heat shock protein 70 to inhibit MLKL polymerization and necroptosis.