Einzeltreffer — DigiBib

4-Hydroxy-2-nonenal (HNE) is one of the most reactive products of lipid peroxidation and has both cytotoxic and genotoxic effects in cells. Several enzymatic pathways have been reported to detoxify HNE, including conjugation by glutathione-S-transferases (GSTs). Removal of the resulting HNE-glutathione conjugate (HNE-SG) by an efflux transporter may be required for complete detoxification. We investigated the effect of expression of GSTM1 and/or the ABC efflux transporter protein, multidrug-resistance protein-1 (MRP1), on HNE-induced cellular toxicity. Stably transfected MCF7 cell lines were used to examine the effect of GSTM1 and/or MRP1 expression on HNE-induced cytotoxicity, GSH depletion, and HNE-protein adduct formation. Co-expression in the MCF7 cell line of GSTM1 with MRP1 resulted in a 2.3-fold sensitization to HNE cytotoxicity (0.44-fold IC(50) value relative to control) rather than the expected protection. Expression of either GSTM1 or MRP1 alone also resulted in slight sensitization to HNE cytotoxicity (0.79-fold and 0.71-fold decreases in IC(50) values, respectively). Co-expression of GSTM1 and MRP1 strongly enhanced the formation of HNE-protein adducts relative to the non-expressing control cell line, whereas expression of either MRP1 alone or GSTM1 alone yielded similarly low levels of HNE-protein adducts to that of the control cell line. Glutathione (GSH) levels were reduced by 10-20% in either the control cell line or the MCF7/GSTM1 cell line with the same HNE exposure for 60min. However, HNE induced >80% depletion of GSH in cells expressing MRP1 alone. Co-expression of both MRP1 and GSTM1 caused slightly greater GSH depletion, consistent with the greater protein adduct formation and cytotoxicity in this cell line. Since expression of GSTM1 or MRP1 alone did not strongly sensitize cells to HNE, or result in greater HNE-protein adducts than in the control cell line, these results indicate that MRP1 and GSTM1 collaborate to enhance HNE-protein adduct formation and HNE cytotoxicity, facilitated by GSH depletion mediated by both MRP1 and GSTM1.

Titel:	Enhanced glutathione depletion, protein adduct formation, and cytotoxicity following exposure to 4-hydroxy-2-nonenal (HNE) in cells expressing human multidrug resistance protein-1 (MRP1) together with human glutathione S-transferase-M1 (GSTM1).
Autor/in / Beteiligte Person:	Rudd, LP ; Kabler, SL ; Morrow, CS ; Townsend, AJ
Zeitschrift:	Chemico-biological interactions, Jg. 194 (2011-11-15), Heft 2-3, S. 113-9
Veröffentlichung:	Limerick : Elsevier ; <i>Original Publication</i>: Amsterdam, Elsevier., 2011
Medientyp:	academicJournal
ISSN:	1872-7786 (electronic)
DOI:	10.1016/j.cbi.2011.08.012
Schlagwort:	Cell Line, Tumor Electrophoresis, Polyacrylamide Gel Humans Inhibitory Concentration 50 ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism Aldehydes pharmacology Glutathione metabolism Glutathione Transferase metabolism
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, N.I.H., Extramural Language: English [Chem Biol Interact] 2011 Nov 15; Vol. 194 (2-3), pp. 113-9. <i>Date of Electronic Publication: </i>2011 Sep 08. MeSH Terms: ATP Binding Cassette Transporter, Subfamily B, Member 1 / metabolism ; Aldehydes / pharmacology ; Glutathione / metabolism ; Glutathione Transferase / metabolism ; Cell Line, Tumor ; Electrophoresis, Polyacrylamide Gel ; Humans ; Inhibitory Concentration 50 References: Chem Res Toxicol. 2004 Feb;17(2):158-64. (PMID: 14967003) ; Chem Biol Interact. 2001 Jan 30;130-132(1-3):261-73. (PMID: 11306050) ; J Biol Chem. 1989 Dec 25;264(36):21582-90. (PMID: 2689439) ; Toxicol Lett. 2006 Oct 25;166(3):212-21. (PMID: 16919899) ; Biochim Biophys Acta. 1980 Nov 7;620(2):281-96. (PMID: 6254573) ; Physiol Rev. 2006 Jul;86(3):849-99. (PMID: 16816140) ; J Pharmacol Exp Ther. 2004 Jan;308(1):260-7. (PMID: 14569069) ; Cancer Res. 1997 Dec 1;57(23):5238-42. (PMID: 9393741) ; Pharmacol Rev. 2010 Mar;62(1):1-96. (PMID: 20103563) ; Free Radic Res. 1999 Oct;31(4):273-300. (PMID: 10517533) ; J Neurochem. 2001 Jan;76(2):627-36. (PMID: 11208926) ; Mol Carcinog. 2000 Nov;29(3):170-8. (PMID: 11108662) ; J Biol Chem. 1998 Aug 7;273(32):20114-20. (PMID: 9685354) ; Free Radic Biol Med. 1991;11(1):81-128. (PMID: 1937131) ; J Biol Chem. 1999 Jan 22;274(4):2234-42. (PMID: 9890986) ; Semin Liver Dis. 1998;18(4):359-76. (PMID: 9875554) ; Biochem J. 1998 Feb 15;330 ( Pt 1):175-9. (PMID: 9461507) ; Proc Natl Acad Sci U S A. 1994 Feb 15;91(4):1480-4. (PMID: 8108434) ; Free Radic Biol Med. 2004 Dec 1;37(11):1694-702. (PMID: 15528028) ; Eur J Pharmacol. 2001 Jun 1;421(1):1-9. (PMID: 11408043) ; Mol Cancer Ther. 2006 Nov;5(11):2851-60. (PMID: 17121932) ; Toxicol Sci. 2007 Sep;99(1):51-7. (PMID: 17525473) ; Prog Lipid Res. 2003 Jul;42(4):318-43. (PMID: 12689622) ; Biochem J. 2000 Sep 1;350 Pt 2:555-61. (PMID: 10947971) ; Proc Natl Acad Sci U S A. 1995 Aug 15;92(17):7690-4. (PMID: 7644478) ; FEBS Lett. 1985 Jan 7;179(2):267-70. (PMID: 3838159) ; Mol Aspects Med. 2003 Aug-Oct;24(4-5):149-59. (PMID: 12892992) ; Mol Pharmacol. 1990 Feb;37(2):192-7. (PMID: 1968221) ; Cancer Res. 1998 Nov 15;58(22):5130-6. (PMID: 9823323) ; Biochem J. 1987 Nov 1;247(3):707-13. (PMID: 3426557) ; Proc Natl Acad Sci U S A. 1988 Oct;85(19):7293-7. (PMID: 3174634) ; Toxicol Sci. 2007 Dec;100(2):513-24. (PMID: 17890767) ; Carcinogenesis. 1994 Jun;15(6):1155-60. (PMID: 8020149) ; Toxicol Appl Pharmacol. 1999 Jun 1;157(2):85-93. (PMID: 10366541) ; Toxicol In Vitro. 2007 Dec;21(8):1365-72. (PMID: 17553661) ; Cancer Res. 1990 May 1;50(9):2747-52. (PMID: 2328501) ; Free Radic Biol Med. 2002 Aug 1;33(3):370-8. (PMID: 12126759) ; Biochem J. 1995 Mar 1;306 ( Pt 2):565-9. (PMID: 7887912) ; Free Radic Biol Med. 2004 Oct 1;37(7):937-45. (PMID: 15336309) ; Biochem Pharmacol. 1997 Apr 25;53(8):1133-40. (PMID: 9175718) ; Carcinogenesis. 1998 Jan;19(1):109-15. (PMID: 9472701) ; Xenobiotica. 1993 Aug;23(8):823-34. (PMID: 8284939) ; Arch Biochem Biophys. 1995 Jan 10;316(1):197-205. (PMID: 7840616) ; J Natl Cancer Inst. 1993 Jul 21;85(14):1159-64. (PMID: 8320745) ; Methods Enzymol. 1984;105:273-82. (PMID: 6727666) ; Biochemistry. 2004 Mar 2;43(8):2345-52. (PMID: 14979731) ; J Biol Chem. 2001 Mar 16;276(11):7952-6. (PMID: 11115505) ; J Biol Chem. 1974 Nov 25;249(22):7130-9. (PMID: 4436300) ; Mol Pharmacol. 1998 Aug;54(2):298-304. (PMID: 9687571) ; Biol Chem. 1997 Aug;378(8):787-91. (PMID: 9377473) ; Biochem J. 1996 Mar 1;314 ( Pt 2):433-7. (PMID: 8670053) ; Mol Pharmacol. 1992 Feb;41(2):230-6. (PMID: 1538704) ; Clin Chim Acta. 1998 Jul 28;275(2):175-84. (PMID: 9721075) ; Free Radic Biol Med. 1989;7(3):333-49. (PMID: 2673948) Grant Information: R01 ES010175-07 United States ES NIEHS NIH HHS; R01 ES010175-06S1 United States ES NIEHS NIH HHS; R01 CA070338 United States CA NCI NIH HHS; R01 ES010175-08 United States ES NIEHS NIH HHS; 3 RO1-CA-70338 United States CA NCI NIH HHS; R01 ES010175 United States ES NIEHS NIH HHS; R01 ES010175-05A1 United States ES NIEHS NIH HHS; R01 ES010175-06 United States ES NIEHS NIH HHS; R01 ES010175-08S1 United States ES NIEHS NIH HHS; R01-ES-10175 United States ES NIEHS NIH HHS Substance Nomenclature: 0 (ATP Binding Cassette Transporter, Subfamily B, Member 1) ; 0 (Aldehydes) ; EC 2.5.1.18 (Glutathione Transferase) ; EC 2.5.1.18 (glutathione S-transferase M1) ; GAN16C9B8O (Glutathione) ; K1CVM13F96 (4-hydroxy-2-nonenal) Entry Date(s): Date Created: 20110920 Date Completed: 20120109 Latest Revision: 20240317 Update Code: 20240317 PubMed Central ID: PMC3221485

Klicken Sie ein Format an und speichern Sie dann die Daten oder geben Sie eine Empfänger-Adresse ein und lassen Sie sich per Email zusenden.

BibTeX Citavi, JabRef, u.a.
(Literaturverwaltung)

PDF kein Volltext!
(Merkzettel, Notizen)

RIS Endnote, Citavi u.a.
(Literaturverwaltung)

MODS
(XML zur Weiterverarbeitung)

oder

Wählen Sie das für Sie passende Zitationsformat und kopieren Sie es dann in die Zwischenablage, lassen es sich per Mail zusenden oder speichern es als PDF-Datei.

Gewünschter Zitations-Stil:

oder

Bitte prüfen Sie, ob die Zitation formal korrekt ist, bevor Sie sie in einer Arbeit verwenden. Benutzen Sie gegebenenfalls den "Exportieren"-Dialog, wenn Sie ein Literaturverwaltungsprogramm verwenden und die Zitat-Angaben selbst formatieren wollen.

Enhanced glutathione depletion, protein adduct formation, and cytotoxicity following exposure to 4-hydroxy-2-nonenal (HNE) in cells expressing human multidrug resistance protein-1 (MRP1) together with human glutathione S-transferase-M1 (GSTM1).