Temporal Proteome and Lipidome Profiles Reveal Hepatitis C Virus-Associated Reprogramming of Hepatocellular Metabolism and Bioenergetics

Diamond, Deborah L.; Syder, Andrew J.; Jacobs, Jon; Sørensen, Christina; Walters, Kathie–Anne; Proll, Sean; McDermott, Jason; Gritsenko, Marina; Zhang, Qibin; Zhao, Rui; Metz, Thomas O.; Camp, David G.; Waters, Katrina M.; Smith, Richard D.; Rice, Charles M.; Katze, Michael G.

doi:10.1371/journal.ppat.1000719

Cited by 372 publications

(446 citation statements)

References 67 publications

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“…Although DENV and polioviruses stimulate PC synthesis (17,20), it is not clear whether HCV infection increases total PC levels. Nevertheless, certain PC species, such as PC 30:0, increased significantly, whereas some decreased (e.g., PC 35:1) upon HCV infection (35). To determine if the enhanced synthesis/accumulation of PC at the site of viral replication is a common feature associated with (+)RNA virus infections, we checked distribution and signal intensity of PC and PE in cells infected with DENV, HCV, or poliovirus.…”

Section: Virus-stimulated and Viral Replication Site-localized Pc Accmentioning

confidence: 99%

Positive-strand RNA viruses stimulate host phosphatidylcholine synthesis at viral replication sites

Zhang

Chukkapalli

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

112

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All positive-strand RNA viruses reorganize host intracellular membranes to assemble their viral replication complexes (VRCs); however, how these viruses modulate host lipid metabolism to accommodate such membrane proliferation and rearrangements is not well defined. We show that a significantly increased phosphatidylcholine (PC) content is associated with brome mosaic virus (BMV) replication in both natural host barley and alternate host yeast based on a lipidomic analysis. Enhanced PC levels are primarily associated with the perinuclear ER membrane, where BMV replication takes place. More specifically, BMV replication protein 1a interacts with and recruits Cho2p (choline requiring 2), a host enzyme involved in PC synthesis, to the site of viral replication. These results suggest that PC synthesized at the site of VRC assembly, not the transport of existing PC, is responsible for the enhanced accumulation. Blocking PC synthesis by deleting the CHO2 gene resulted in VRCs with wider diameters than those in wild-type cells; however, BMV replication was significantly inhibited, highlighting the critical role of PC in VRC formation and viral replication. We further show that enhanced PC levels also accumulate at the replication sites of hepatitis C virus and poliovirus, revealing a conserved feature among a group of positive-strand RNA viruses. Our work also highlights a potential broad-spectrum antiviral strategy that would disrupt PC synthesis at the sites of viral replication but would not alter cellular processes.positive-strand RNA viruses | viral replication complexes | virus-host interactions | virus control | phospholipids A ll positive-strand RNA viruses [(+)RNA viruses], which include numerous important human, animal, and plant pathogens, share similar strategies for genomic replication. A highly conserved and indispensable feature of their replication is the proliferation and reorganization of host cellular membranes to assemble viral replication complexes (VRCs). Despite this central importance, it is largely unknown how cellular membranes are rearranged by the viral replication proteins and how cellular lipid metabolism is modulated to accommodate membrane proliferation and remodeling.Brome mosaic virus (BMV) serves as a model for understanding VRC formation of (+)RNA viruses (1). BMV is the type member of the plant virus family Bromoviridae and a representative member of the alphavirus-like superfamily, which includes many human, animal, and plant-infecting viruses (2). BMV encodes two replication proteins, 1a and 2a pol . 2a pol serves as the replicase, whereas 1a has an N-terminal methyltransferase domain (3, 4) and a C-terminal ATPase/helicase-like domain (5). Together, 1a and 2a pol are necessary and sufficient for BMV replication. BMV induces vesicular structures in its surrogate host, the yeast Saccharomyces cerevisiae, and its natural host, barley (6, 7). These structures, termed spherules, have been shown to be the VRCs in yeast as 1a, 2a pol , and nascent viral RNAs reside in the interior of th...

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Section: Virus-stimulated and Viral Replication Site-localized Pc Accmentioning

confidence: 99%

Positive-strand RNA viruses stimulate host phosphatidylcholine synthesis at viral replication sites

Zhang

Chukkapalli

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

112

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“…Indeed, recent studies based on transcriptome and proteomic analyses have demonstrated that expression of host genes involved in the biosynthesis, degradation and transport of intracellular lipids is profoundly altered upon infection. [86][87][88][89] The expression of SREBPs, which control transcription of genes required for cholesterol biosynthesis, 90 is stimulated both by HCV infection and It was demonstrated that NS proteins associate with cholesterol-rich lipid rafts and that depletion of cholesterol with statins selectively reduces HCV RNA replication. 104 However, statins are inhibitors of the mevalonate pathway, 99 which produces not only cholesterol, but also non-sterol isoprenoids, including geranylgeranyl and farnesyl.…”

Section: Role Of Lipid Metabolism In Hcv Rna Replicationmentioning

confidence: 99%

“…Although the significance of this simultaneous induction in lipid anabolism and catabolism remains unclear, the authors argue that β-oxidation may help to maintain elevated ATP levels to support energy-dependent biosynthetic processes as well as to limit the accumulation and toxic effect of ceramide overload. 86 In the last years, the role of cholesterol in HCV infection has gained much attention. In mammalian cells, cholesterol can be either synthesized via the mevalonate pathway, 99 or generated by internalization and degradation of LDL particles.…”

Section: Role Of Lipid Metabolism In Hcv Rna Replicationmentioning

confidence: 99%

Hepatitis c virus and host cell lipids: An intimate connection

Alvisi¹,

Madan²,

2011

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“…sterol biosynthesis, fatty acid metabolism and synthesis of specific phosphoinositides [15]. For instance, a marked alteration of cellular metabolism and an increase in fatty acid biosynthetic pathway have been described upon human cytomegalovirus (HCMV), DENV or HCV infection [1, 5,6,11]. The association of viral multiplication with modulation of host cell factors involved in lipid metabolism is not an exclusive feature of animal viruses, thus, replication and recombination of the plant pathogens tombusviruses has been revealed to rely on host genes involved in lipid metabolism [96][97][98][99].…”

Section: Cellular Lipids Involved In Viral Replication Complex Assemblymentioning

confidence: 99%

“…The involvement of lipids in the infectious cycle is shared by enveloped viruses (those viruses whose infectious particle is wrapped by one or more lipid membranes) and non-enveloped viruses [1][2][3][4]. Apart from taking advantage on cellular lipids that are usually located inside cells, viruses induce global metabolic changes on infected cells, leading to the rearrangement of the lipid metabolism to facilitate viral multiplication [1, [5][6][7][8][9][10][11]. In some cases, these alterations produce the reorganization of intracellular membranes of the host cell, building the adequate microenvironment for viral replication [12,13].…”

Section: Introductionmentioning

confidence: 99%

Lipid Involvement in Viral Infections: Present and Future Perspectives for the Design of Antiviral Strategies

Martín-Acebes¹,

Vázquez-Calvo²,

Caridi³

et al. 2013

Lipid Metabolism

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Temporal Proteome and Lipidome Profiles Reveal Hepatitis C Virus-Associated Reprogramming of Hepatocellular Metabolism and Bioenergetics

Cited by 372 publications

References 67 publications

Positive-strand RNA viruses stimulate host phosphatidylcholine synthesis at viral replication sites

Positive-strand RNA viruses stimulate host phosphatidylcholine synthesis at viral replication sites

Hepatitis c virus and host cell lipids: An intimate connection

Lipid Involvement in Viral Infections: Present and Future Perspectives for the Design of Antiviral Strategies

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