The Mitochondrial Permeability Transition Augments Fas-induced Apoptosis in Mouse Hepatocytes

Anton; Bossy-Wetzel; Bradham; Bradham; Cai; Chinnaiyan; Clement; Cohen; De Maria; de Moissac; DiDonato; Dimmeler; Fladmark; Galle; Green; Green; Gross; Haskill; Heiskanen; Iimuro; Imai; Jobin; Jones; Jurgensmeier; Kim; Kim; Kim; Kluck; Kristal; Kroemer; Leist; Leist; Li; Liu; Luo; Malinin; Malisan; Melino; Mercurio; Moldeus; Nagata; Natoli; Ni; Nieminen; Obeid; Ogasawara; Pastorino; Perry; Ponton; Qian; Qian; Ray; Reed; Rothwarf; Rouquet; Scaffidi; Scorrano; Susin; Susin; Takehara; Van Antwerp; Verheij; Wang; Wang; Westwick; Woronicz; Xu; Yang; Yin; Yoshida; Zamzami; Zamzami; Zandi; Zhao; Zhou

The Mitochondrial Permeability Transition Augments Fas-induced Apoptosis in Mouse Hepatocytes

Authors: Anton
Bossy-Wetzel
Bradham
Bradham
Cai
Chinnaiyan
Clement
Cohen
De Maria
de Moissac
DiDonato
Dimmeler
Fladmark
Galle
Green
Green
Gross
Haskill
Heiskanen
Iimuro
Imai
Jobin
Jones
Jurgensmeier
Kim
Kim
Kim
Kluck
Kristal
Kroemer
Leist
Leist
Li
Liu
Luo
Malinin
Malisan
Melino
Mercurio
Moldeus
Nagata
Natoli
Ni
Nieminen
Obeid
Ogasawara
Pastorino
Perry
Ponton
Qian
Qian
Ray
Reed
Rothwarf
Rouquet
Scaffidi
Scorrano
Susin
Susin
Takehara
Van Antwerp
Verheij
Wang
Wang
Westwick
Woronicz
Xu
Yang
Yin
Yoshida
Zamzami
Zamzami
Zandi
Zhao
Zhou
Publication date: 1 January 2000
Publisher
Doi

Abstract

Tumor necrosis factor-alpha receptor 1 and Fas recruit overlapping signaling pathways. To clarify the differences between tumor necrosis factor alpha (TNFalpha) and Fas pathways in hepatocyte apoptosis, primary mouse hepatocytes were treated with TNFalpha or an agonist anti-Fas antibody after infection with an adenovirus expressing an IkappaB superrepressor (Ad5IkappaB). Treatment with TNFalpha induced apoptosis in Ad5IkappaB-infected mouse hepatocytes, as we previously reported for rat hepatocytes. Ad5IkappaB plus anti-Fas antibody or actinomycin D plus anti-Fas antibody rapidly induced apoptosis, whereas anti-Fas antibody alone produced little cytotoxicity. The proteasome inhibitor (MG-132) and a dominant-negative mutant of nuclear factor-kappaB-inducing kinase also promoted TNFalpha- and Fas-mediated apoptosis. Expression of either crmA or a dominant-negative mutant of the Fas-associated death domain protein prevented TNFalpha- and Fas-mediated apoptosis. In addition, the caspase inhibitors, DEVD-cho and IETD-fmk, inhibited TNFalpha- and Fas-mediated apoptosis. In Ad5IkappaB-infected hepatocytes, caspases-3 and -8 were activated within 2 h after treatment with anti-Fas antibody or within 6 h after TNFalpha treatment. Confocal microscopy demonstrated onset of the mitochondrial permeability transition (MPT) and mitochondrial depolarization by 2-3 h after anti-Fas antibody treatment and 8-10 h after TNFalpha treatment, followed by cytochrome c release. The combination of the MPT inhibitors, cyclosporin A, and trifluoperazine, protected Ad5IkappaB-infected hepatocytes from TNFalpha-mediated apoptosis. After anti-Fas antibody, cyclosporin A and trifluoperazine decreased cytochrome c release but did not prevent caspase-3 activation and cell-death. In conclusion, nuclear factor-kappaB activation protects mouse hepatocytes against both TNFalpha- and Fas-mediated apoptosis. TNFalpha and Fas recruit similar but nonidentical, pathways signaling apoptosis. The MPT is obligatory for TNFalpha-induced apoptosis. In Fas-mediated apoptosis, the MPT accelerates the apoptogenic events but is not obligatory for them

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