Nathalie Koch scite author profile

Cellular glycosphingolipids mediate the fusion between some viruses and the plasma membrane of target cells. In the present study, we have analyzed the interaction of human immunodeficiency virus (HIV)-1 and HIV-2 surface envelope glycoproteins from distinct viral isolates with monolayers of various glycosphingolipids at the air-water interface. The penetration of the viral glycoproteins into glycosphingolipid monolayers was detected as an increase in the surface pressure. We found that HIV-1 recombinant gp120 (IIIB isolate) could penetrate into a monomolecular film of ␣-hydroxylated galactosylceramide (GalCer-HFA), while ceramides, GluCer, and nonhydroxylated GalCer were totally inactive. The glycoproteins isolated from HIV-1 isolates LAI and NDK and from HIV-2(ROD) could also interact with a GalCer-HFA monolayer, whereas gp120 from HIV-1(SEN) and HIV-1(89.6) did not react. These data correlated with the ability of the corresponding viruses to gain entry into the CD4 ؊ /GalCer ؉ cell line HT-29, demonstrating the determinant role of GalCer-HFA in this CD4-independent pathway of HIV-1 and HIV-2 infection. In contrast, all HIV-1 and HIV-2 glycoproteins tested were found to interact with a monolayer of GM3, a ganglioside abundantly expressed in the plasma membrane of CD4 ؉ lymphocytes and macrophages. A V3 loop-derived synthetic peptide inhibitor of HIV-1 and HIV-2 infection in both CD4؊ and CD4 ؉ cells could penetrate into various glycosphingolipid monolayers, including GalCer-HFA and GM3. Taken together, these data suggest that the adsorption of human immunodeficiency viruses to the surface of target cells involves an interaction between the V3 domain of the surface envelope glycoprotein and specific glycosphingolipids, i.e. GalCer-HFA for CD4 ؊ cells and GM3 for CD4 ؉ cells.

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Co-expression of CXCR4/fusin and galactosylceramide in the human intestinal epithelial cell line HT-29

Delézay

Koch²,

Yahi³

et al. 1997

AIDS

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Early tailored assertive community case management for hard‐to‐engage adolescents suffering from psychiatric disorders: an exploratory pilot study

Baier¹,

Favrod²,

Ferrari³

et al. 2012

Early Intervention Psych

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Impact of a pain protocol including hypnosis in major burns

Berger

Davadant

Marin

et al. 2010

Burns

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Use of Drug Resistance Sequence Data for the Systematic Detection of Non‐B Human Immunodeficiency Virus Type 1 (HIV‐1) Subtypes: How to Create a Sentinel Site for Monitoring the Genetic Diversity of HIV‐1 at a Country Scale

Yahi¹,

Fantini

Tourres

et al. 2001

J INFECT DIS

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To assess the molecular epidemiology of human immunodeficiency virus type 1 (HIV-1), a screening method was developed for identification of non-B subtypes from sequence data obtained for resistance testing. The method is based on the evaluation of the percentage of divergence of a given sequence from the reference B subtype HXB2. Analysis of 1720 reverse-transcriptase (RT) and 1824 protease sequences stored in a database allowed for the determination of a threshold level of divergence from HXB2 above which a non-B subtype could be unambiguously characterized regardless of the pattern of resistance mutations (>8.6% for RT; >10.8% for protease). This conclusion was validated by phylogenetic analysis of RT, protease, and env genes. Overall, 72 (4.2%) and 73 (4.0%) non-B sequences were identified in the RT and protease coding regions, respectively. This method allows for the rapid detection of non-B subtypes among retrospective, recent, and future RT and/or protease sequence databases.

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Nathalie Koch

Specific Interaction of HIV-1 and HIV-2 Surface Envelope Glycoproteins with Monolayers of Galactosylceramide and Ganglioside GM3

Co-expression of CXCR4/fusin and galactosylceramide in the human intestinal epithelial cell line HT-29

Early tailored assertive community case management for hard‐to‐engage adolescents suffering from psychiatric disorders: an exploratory pilot study

Impact of a pain protocol including hypnosis in major burns

Use of Drug Resistance Sequence Data for the Systematic Detection of Non‐B Human Immunodeficiency Virus Type 1 (HIV‐1) Subtypes: How to Create a Sentinel Site for Monitoring the Genetic Diversity of HIV‐1 at a Country Scale

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