The C-terminal region of hepatitis C core protein is required for Fas-ligand independent apoptosis in Jurkat cells by facilitating Fas oligomerization

Moorman, Jonathan P.; Prayther, Deborah; McVay, Derek P.; Hahn, Young S.; Hahn, Chang S.

doi:10.1016/s0042-6822(03)00208-3

Cited by 40 publications

(34 citation statements)

References 40 publications

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“…The apoptotic property of the genotype 1a core protein has yet to be studied using the JFH-1-based infectious clone system, although previous studies have attributed both prosurvival and proapoptotic properties to it (25,30,46,57). Similar observations also have been described in overexpression studies using the genotype 1b core protein and appear to be dependent on the death stimuli and types of cells used (3,9,10,36,49,53,56,60,76).…”

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confidence: 66%

“…In addition, other domains in the core protein have been shown to bind host proteins and may contribute to apoptosis regulation by interfering with different cellular pathways (see reviews in references 33, 42, and 52). For example, the Nterminal domain (aa 1 to 75) of the core protein interacts with Hsp60, leading to the production of reactive oxygen species and enhancement of tumor necrosis factor alpha-mediated apoptosis (30), while a C-terminal domain (aa 153 to 192) facilitates Fas oligomerization and is required for apoptosis induction in Jurkat cells (46). However, the relative contribution of these various factors to apoptosis induction during HCV infection remains to be determined.…”

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confidence: 99%

“…Several studies have identified domains or regions within the core protein that interfere with specific apoptosis pathways. For instance, the interaction of the N-terminal domain (residues 1 to 75) of the genotype 1a core protein with Hsp60 enhanced tumor necrosis factor alphamediated apoptosis, while its C-terminal region (residues 153 to 192) is required for Fas ligand-independent apoptosis (30,46). The genotype 1b core protein (residues 1 to 153) binds to the death domain of FADD, resulting in enhanced apoptosis (76).…”

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confidence: 99%

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The Hepatitis C Virus Core Protein Contains a BH3 Domain That Regulates Apoptosis through Specific Interaction with Human Mcl-1

Mohd-Ismail

Deng

Sukumaran

et al. 2009

J Virol

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The hepatitis C virus (HCV) core protein is known to modulate apoptosis and contribute to viral replication and pathogenesis. In this study, we have identified a Bcl-2 homology 3 (BH3) domain in the core protein that is essential for its proapoptotic property. Coimmunoprecipitation experiments showed that the core protein interacts specifically with the human myeloid cell factor 1 (Mcl-1), a prosurvival member of the Bcl-2 family, but not with other prosurvival members (Bcl-X L and Bcl-w). Moreover, the overexpression of Mcl-1 protects against core-induced apoptosis. By using peptide mimetics, core was found to release cytochrome c from isolated mitochondria when complemented with Bad. Thus, core is a bona fide BH3-only protein having properties similar to those of Noxa, a BH3-only member of the Bcl-2 family that binds preferentially to Mcl-1. There are three critical hydrophobic residues in the BH3 domain of the core protein, and they are essential for the proapoptotic property of the core protein. Furthermore, the genotype 1b core protein is more effective than the genotype 2a core protein in inducing apoptosis due to a single-amino-acid difference at one of these hydrophobic residues (residue 119). Replacing this residue in the J6/JFH-1 infectious clone (genotype 2a) with the corresponding amino acid in the genotype 1b core protein produced a mutant virus, J6/JFH-1(V119L), which induced significantly higher levels of apoptosis in the infected cells than the parental J6/JFH-1 virus. Furthermore, the core protein of J6/JFH-1(V119L), but not that of J6/JFH-1, interacted with Mcl-1 in virus-infected cells. Taken together, the core protein is a novel BH3-only viral homologue that contributes to the induction of apoptosis during HCV infection.

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confidence: 66%

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confidence: 99%

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confidence: 99%

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The Hepatitis C Virus Core Protein Contains a BH3 Domain That Regulates Apoptosis through Specific Interaction with Human Mcl-1

Mohd-Ismail

Deng

Sukumaran

et al. 2009

J Virol

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“…There are several well characterized cases in which expression or modification of intracellular proteins inhibits or promotes apoptotic events downstream of Fas (3,6). In contrast, few examples exist in which Fas activity is modulated in either a positive or negative fashion by membrane proteins expressed in cis (7).…”

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confidence: 99%

CD47 Augments Fas/CD95-mediated Apoptosis

Manna

Dimitry

Oldenborg

et al. 2005

Journal of Biological Chemistry

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“…Interaction of the HCV core protein with a wide variety of cellular proteins has been reported to influence host cell functions (26,34). The HCV core protein is also able to suppress host immunity through several mechanisms, such as impairment of the function of dendritic cells in vitro, promotion of apoptosis of immune cells, or suppression of type I interferon (IFN) signaling, among other mechanisms (7,14,22,28,31,32,52). In the case of DNA vaccination, a high level of expression of the HCV core protein is desired for the priming of specific immune responses.…”

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confidence: 99%

The Wild-Type Hepatitis C Virus Core Inhibits Initiation of Antigen-Specific T- and B-Cell Immune Responses in BALB/c Mice

Zhu

Chang

et al. 2010

Clin Vaccine Immunol

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In this study, the effects of wild-type and deletion mutant hepatitis C virus (HCV) core proteins on the induction of immune responses in BALB/c mice were assessed. p2HA-C145-S23, encoding a core protein with the C-terminal 46 amino acids truncated, significantly produced stronger antibody and cellular responses than p2HA-C191-S23. The induction of immune responses by p2HA-C145-S23 was dose dependent. However, increasing the doses or repeated administration did not enhance immune responses by the wild-type core protein. In addition, p2HA-C191-S23 was apparently able to interfere with the priming of specific immune responses by p2HA-C145-S23 when the two were coadministered. These results demonstrated that the wild-type HCV core protein itself could inhibit the priming of immune responses in the course of a DNA vaccination, whereas the truncated HCV core protein could provide potential applications for the development of DNA-and peptide-based HCV vaccines.

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The C-terminal region of hepatitis C core protein is required for Fas-ligand independent apoptosis in Jurkat cells by facilitating Fas oligomerization

Cited by 40 publications

References 40 publications

The Hepatitis C Virus Core Protein Contains a BH3 Domain That Regulates Apoptosis through Specific Interaction with Human Mcl-1

The Hepatitis C Virus Core Protein Contains a BH3 Domain That Regulates Apoptosis through Specific Interaction with Human Mcl-1

CD47 Augments Fas/CD95-mediated Apoptosis

The Wild-Type Hepatitis C Virus Core Inhibits Initiation of Antigen-Specific T- and B-Cell Immune Responses in BALB/c Mice

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