E2 of Hepatitis C Virus Inhibits Apoptosis

Lee, Song Hee; Kim, Yoon Ki; Kim, Chon Saeng; Seol, Su Kyoung; Kim, Joonhyun; Cho, Sungchan; Song, Young Lan; Bartenschlager, Ralf; Jang, Sung Key

doi:10.4049/jimmunol.175.12.8226

Cited by 66 publications

(58 citation statements)

References 67 publications

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“…XIAP could influence this event in two ways, directly by ubiquitinating the cleaved form of caspase-8 and causing its degradation, or indirectly by blocking caspase-3, which was previously shown to cleave caspase-8 (Wieder et al, 2001;Lee et al, 2005;Hayakawa et al, 2008). As XIAP was shown to interact with caspases 3, 7 and 9, but not 8 , it is unlikely that the accumulation of the p43/41 forms of caspase-8 is caused directly by XIAP.…”

Section: Discussionmentioning

confidence: 99%

“…As XIAP was shown to interact with caspases 3, 7 and 9, but not 8 , it is unlikely that the accumulation of the p43/41 forms of caspase-8 is caused directly by XIAP. More likely, XIAP, by inhibiting caspase-3, prevents its positive feedback loop, by which caspase-8 is further cleaved (Wieder et al, 2001;Lee et al, 2005;Hayakawa et al, 2008). Thus, lower levels of XIAP allow the accumulation of the cleaved form of caspase-8.…”

Section: Discussionmentioning

confidence: 99%

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Novel SMAC-mimetics synergistically stimulate melanoma cell death in combination with TRAIL and Bortezomib

et al. 2010

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BACKGROUND: XIAP (X-linked inhibitor of apoptosis protein) is an anti-apoptotic protein exerting its activity by binding and suppressing caspases. As XIAP is overexpressed in several tumours, in which it apparently contributes to chemoresistance, and because its activity in vivo is antagonised by second mitochondria-derived activator of caspase (SMAC)/direct inhibitor of apoptosisbinding protein with low pI, small molecules mimicking SMAC (so called SMAC-mimetics) can potentially overcome tumour resistance by promoting apoptosis. METHODS: Three homodimeric compounds were synthesised tethering a monomeric SMAC-mimetic with different linkers and their affinity binding for the baculoviral inhibitor repeats domains of XIAP measured by fluorescent polarisation assay. The apoptotic activity of these molecules, alone or in combination with tumour necrosis factor-related apoptosis-inducing ligand (TRAIL) and/or Bortezomib, was tested in melanoma cell lines by MTT viability assays and western blot analysis of activated caspases. RESULTS: We show that in melanoma cell lines, which are typically resistant to chemotherapeutic agents, XIAP knock-down sensitises cells to TRAIL treatment in vitro, also favouring the accumulation of cleaved caspase-8. We also describe a new series of 4-substituted azabicyclo[5.3.0]alkane monomeric and dimeric SMAC-mimetics that target various members of the IAP family and powerfully synergise at submicromolar concentrations with TRAIL in inducing cell death. Finally, we show that the simultaneous administration of newly developed SMAC-mimetics with Bortezomib potently triggers apoptosis in a melanoma cell line resistant to the combined effect of SMAC-mimetics and TRAIL. CONCLUSION: Hence, the newly developed SMAC-mimetics effectively synergise with TRAIL and Bortezomib in inducing cell death. These findings warrant further preclinical studies in vivo to verify the anticancer effectiveness of the combination of these agents.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Novel SMAC-mimetics synergistically stimulate melanoma cell death in combination with TRAIL and Bortezomib

et al. 2010

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“…In this respect, HCV core protein has been shown to inhibit TNFα-or FAS-mediated activation of caspase 8, p21 and p53 expression, or to enhance Bcl-XL, Bcl2 and cyclin D1 expression or the Raf1/MAPK signaling pathways (Hassan et al, 2004;Saito et al, 2006). E2 was reported to inhibit apoptosis by negatively regulating the cytochrome c release from mitochondria after TRAIL activation (Lee et al, 2005). NS3/NS4A protects liver damage in animals treated with lethal doses of TNFα combined with D-galactosamine, while NS3 interacts with and affects p53 activity (Frelin et al, 2006;Tanaka et al, 2006).…”

Section: Interferon Signaling Pathway and Viral Resistancementioning

confidence: 99%

Cellular models for the screening and development of anti-hepatitis C virus agents

Gondeau

Pichard-Garcia

Maurel

2009

Pharmacology & Therapeutics

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Investigations on the biology of hepatitis C virus (HCV) have been hampered by the lack of small animal models. Efforts have therefore been directed to designing practical and robust cellular models of human origin able to support HCV replication and production in a reproducible, reliable and consistent manner. Many different models based on different forms of virions and hepatoma or other cell types have been described including virus-like particles, pseudotyped particles, subgenomic and full length replicons, virion productive replicons, immortalised hepatocytes, fetal and adult primary human hepatocytes. This review focuses on these different cellular models, their advantages and disadvantages at the biological and experimental levels, and their respective use for evaluating the effect of antiviral molecules on different steps of HCV biology including virus entry, replication, particles generation and excretion, as well as on the modulation by the virus of the host cell response to infection.

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“…24 This suggests that replicon RNA replicates in a structure surrounded by lipid membrane, i.e. lipid raft.…”

Section: Structure Of the Replication Complexmentioning

confidence: 99%

“…18,19 In the full-length HCV RNA replication system, the presence of double strand RNA (dsRNA), consisting of the HCV RNA plus strand and the minus strand, an intermediate replication product, enables easier evaluation of the influence of HCV, including the effect of dsRNA, on host factors, compared with a replicon system with nonstructural regions using a variety of promoters. Since structural proteins are required for the production of viral particles, full-length HCV RNA replication systems have advanced research on in vivo properties of the virus, including packaging, budding, and infection [20][21][22][23][24] (Fig.3).…”

Section: Full-length Hcv Rna Replication Systemmentioning

confidence: 99%

Advances in Genomic Research on Hepatitis C Virus with a Useful Tool, Replicon System

2008

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E2 of Hepatitis C Virus Inhibits Apoptosis

Cited by 66 publications

References 67 publications

Novel SMAC-mimetics synergistically stimulate melanoma cell death in combination with TRAIL and Bortezomib

Novel SMAC-mimetics synergistically stimulate melanoma cell death in combination with TRAIL and Bortezomib

Cellular models for the screening and development of anti-hepatitis C virus agents

Advances in Genomic Research on Hepatitis C Virus with a Useful Tool, Replicon System

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