Gerald Eder scite author profile

There is now abundant evidence to substantiate an important role of hepatitis C virus (HCV) core protein in cellular gene expression as well as in the viral cycle. Thus the subcellular localization of this protein has important implications. However, several studies have shown controversial results: the HCV core has been, indeed, described as cytoplasmic or nuclear depending on the size of the protein or on the genotype analyzed. We have studied the localization of the HCV core protein in two different cell lines, one nonhepatic (CHO) and the other hepatic (HepG2). Double immunof luorescence staining using a nuclear membrane marker and confocal analysis showed the core protein pattern to be cytoplasmic and globular. This pattern is not cell cycleregulated. Electron microscopy analysis revealed the nature of the globular staining observed in immunof luorescence. The HCV core protein accumulated at the surface of lipid droplets that were also the unique morphological feature of nonhepatic core transfected cells. The lipid droplets were isolated by sequential ultracentrifugation on the basis of their density; biochemical analysis revealed a prevalence of triglycerides. In addition the core protein colocalized with apolipoprotein AII at the surface of the lipid droplets as revealed by confocal microscopy. Moreover analysis of liver biopsies from chronically HCV-infected chimpanzees revealed that HCV core is cytoplasmic and localized on the endoplasmic reticulum and on lipid droplets. These results clearly define the subcellular localization of the HCV core protein and suggest a relationship between the expression of the HCV core protein and cellular lipid metabolism.The hepatitis C virus (HCV), the major causative agent of non-A͞non-B hepatitis (1), is a positive-stranded RNA virus of about 10 kb evolutionary related to pestivirus and flavivirus (2, 3). The HCV ORF is flanked by a 341-bp long 5Ј untranslated region and a 3Ј untranslated region with a poly(U) or a poly(A) tail (3, 4) and encodes for a precursor polyprotein of about 3000 aa that is then cleaved into structural and nonstructural proteins (5, 6).A major characteristic of HCV infection is the extremely high (up to 80%) risk of chronicity; in addition, chronic infection can lead to liver cirrhosis and liver cancer (7,8). An important issue regarding the pathogenesis of HCV-associated liver lesions is to determine whether or not HCV proteins might have a direct effect on cellular phenotype as suggested by some recent works (9, 10). In this view, a regulative effect by HCV core protein, one of the structural proteins of the virus, has been shown by transfection both on hepatitis B viral genome expression and replication (11) and on expression of different cellular genes such as c-myc oncogene (12) or genes encoding for interferon ␤ in a human cell line (13).The observations reported above would suggest that the HCV core protein could have not only a packaging function in the cytoplasm, but also a regulatory role on cell functions. Precise informatio...

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A randomized, controlled trial to study the efficacy and safety of C1 inhibitor concentrate in treating hereditary angioedema

Kunschak¹,

Engl

Maritsch³

et al. 1998

Transfusion

137

106

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Markers of Foamy Virus Infections in Monkeys, Apes, and Accidentally Infected Humans: Appropriate Testing Fails to Confirm Suspected Foamy Virus Prevalence in Humans

Schweizer¹,

Turek²,

Hahn³

et al. 1995

AIDS Research and Human Retroviruses

163

104

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Foamy viruses (FVs) persist in healthy individuals of various mammalian species, including nonhuman primates. Laboratory markers of FV infection are (1) virus in throat epithelium or peripheral blood lymphocytes (PBLs), (2) proviral DNA sequences in PBLs and various solid organs, and (3) antibodies reactive to viral antigens on Western blots, in radioimmunoprecipitation tests, and in immunofluorescence assays. Using PCR and serological tests, we readily detected FV markers in naturally infected African green monkeys, rhesus monkeys, and chimpanzees, as well as in accidentally infected humans. Transmission of simian foamy viruses to humans (by bite or inadvertent laboratory infection) leads to viral markers, without affecting the recipient. Reports on FV-associated clinical disorders (e.g., thyroid or neurological) have remained controversial. In this study we failed to detect, by PCR, viral sequences in the samples from 223 patients, including 16 HIV-infected Africans, 46 Graves' disease patients, and 28 patients with the de Quervain's thyroiditis. Evaluation of 2688 sera from suspected high-risk areas (e.g., Central and East Africa, or high-risk groups such as HIV-infected individuals and patients with AIDS, thyroid, and neurological disorders) did not reveal FV-specific antibodies in a single case. Previously reported FV seroprevalence in various populations has never been verified by appropriate confirmatory tests. The strain of "human foamy virus" has remained a unique isolate. In conclusion, FVs are unlikely--at present--to circulate in human populations.

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Gerald Eder

Hepatitis C virus core protein shows a cytoplasmic localization and associates to cellular lipid storage droplets

A randomized, controlled trial to study the efficacy and safety of C1 inhibitor concentrate in treating hereditary angioedema

Markers of Foamy Virus Infections in Monkeys, Apes, and Accidentally Infected Humans: Appropriate Testing Fails to Confirm Suspected Foamy Virus Prevalence in Humans

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