Dendritic cells (DCs) are essential antigen-presenting cells for the induction of immunity against pathogens. However, HIV-1 spread is strongly enhanced in clusters of DCs and CD4(+) T cells. Uninfected DCs capture HIV-1 and mediate viral transfer to bystander CD4(+) T cells through a process termed trans-infection. Initial studies identified the C-type lectin DC-SIGN as the HIV-1 binding factor on DCs, which interacts with the viral envelope glycoproteins. Upon DC maturation, however, DC-SIGN is down-regulated, while HIV-1 capture and trans-infection is strongly enhanced via a glycoprotein-independent capture pathway that recognizes sialyllactose-containing membrane gangliosides. Here we show that the sialic acid-binding Ig-like lectin 1 (Siglec-1, CD169), which is highly expressed on mature DCs, specifically binds HIV-1 and vesicles carrying sialyllactose. Furthermore, Siglec-1 is essential for trans-infection by mature DCs. These findings identify Siglec-1 as a key factor for HIV-1 spread via infectious DC/T-cell synapses, highlighting a novel mechanism that mediates HIV-1 dissemination in activated tissues

A Granelli-Piperno

A Hartnell

A Hodges

AC van der Kuyl

Amalio Telenti

B Février

Bonaventura Clotet

Bärbel Glass

C Goujon

C Théry

D McDonald

E Garcia

Elina Erikson

H Rempel

Hans-Georg Kräusslich

Itziar Erkizia

J Munday

Javier Martinez-Picado

JM Brenchley

K Hrecka

KJ Livak

L Gautier

L Kalvodova

M Iannacone

M Lampe

M Li

MA Barron

Maier Lorizate

Maria C. Puertas

Maria Pino

Maria T. Rodriguez-Plata

MT Rodriguez-Plata

N Izquierdo-Useros

N Laguette

N Manel

Nadine Zangger

Nuria Izquierdo-Useros

Oliver T. Keppler

P Zhu

PR Crocker

PU Cameron

R Chan

RW Sanders

S Kirchberger

SG Turville

T Junt

TB Geijtenbeek

TK van den Berg

V Piguet

Walther Mothes

WB Puryear

Y Benjamini

Y van Kooyk

Z Zou

PLoS Biology

PubMed

Izquierdo-Useros Nuria

Lorizate Maier

Puertas Maria C.

Rodriguez-Plata Maria T.

Zangger Nadine

Erikson Elina

Pino Maria

Erkizia Itziar

Glass Bärbel

Clotet Bonaventura

Keppler Oliver T.

Telenti Amalio

Kräusslich Hans-Georg

Martinez-Picado Javier

Public Library of Science (PLOS)

-Infection Through Recognition of Viral Membrane Gangliosides

Altres ajuts: This work was supported by the Spanish Ministry of Science and Innovation, the Spanish AIDS network "Red Temática Cooperativa de Investigació3n en SIDA" (RD06/0006), the Catalan HIV Vaccine Development Program (HIVACAT), Gala contra la sida: Barcelona 2011, and by a grant from the Deutsche Forschungsgemeinschaft to H.-G.K. (TRR83; project 14). N.I-U. was supported by the program "José Castillejo" from the Spanish Ministry of Education. M.T.R.-P. is supported by grant from the Spanish Ministry of Science and Innovation H.-G.K. is investigator of the Cell Networks Cluster of Excellence (EXC81). A.T. is supported by the Swiss National Science Foundation (31003A_132863). The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.'The novel dendritic cell receptor Siglec-1 binds sialyllactose moieties on HIV-1 membrane gangliosides, thereby enhancing HIV-1 transinfection. Dendritic cells (DCs) are essential antigen-presenting cells for the induction of immunity against pathogens. However, HIV-1 spread is strongly enhanced in clusters of DCs and CD4 + T cells. Uninfected DCs capture HIV-1 and mediate viral transfer to bystander CD4 + T cells through a process termed trans -infection. Initial studies identified the C-type lectin DC-SIGN as the HIV-1 binding factor on DCs, which interacts with the viral envelope glycoproteins. Upon DC maturation, however, DC-SIGN is down-regulated, while HIV-1 capture and trans -infection is strongly enhanced via a glycoprotein-independent capture pathway that recognizes sialyllactose-containing membrane gangliosides. Here we show that the sialic acid-binding Ig-like lectin 1 (Siglec-1, CD169), which is highly expressed on mature DCs, specifically binds HIV-1 and vesicles carrying sialyllactose. Furthermore, Siglec-1 is essential for trans -infection by mature DCs. These findings identify Siglec-1 as a key factor for HIV-1 spread via infectious DC/T-cell synapses, highlighting a novel mechanism that mediates HIV-1 dissemination in activated tissues. Mature dendritic cells (mDCs) capture and store infectious HIV-1 and subsequently infect neighboring CD4 + T cells in lymphoid organs. This process, known as trans -infection, is a key contributor to HIV pathogenesis, but the precise mechanism and the identity of the receptor on the mDC surface that recognizes viral particles remain controversial. Although the interaction of HIV-1 envelope glycoproteins with the C-type lectin DC-SIGN has been suggested to mediate HIV-1 capture and trans -infection, later studies revealed an envelope glycoprotein-independent virus capture mechanism in mDCs. Here, we identify Siglec-1 as the surface receptor on mDCs that boosts their uptake of HIV-1 and their capacity to trans -infect CD4 + cells, leading in turn to HIV-1 disease progression. Siglec-1 captures the virus by interacting with sialyllactose-containing gangliosides exposed on viral membranes. This indicates that Siglec-1 functions as a general binding molecule for any vesicle carrying sialyllactose in its membrane, including exosomes and other viruses. We suggest that this natural pathway through mDC, which would normally lead to antigen processing and presentation, has been subverted by HIV-1 for its own storage and transmission

Izquierdo Useros, Nuria

Lorizate, Maier

Puertas, Maria C..

Rodriguez-Plata, Maria T.

Zangger, Nadine

Erikson, Elina

Pino, Maria

Erkizia, Itziar

Glass, Bärbel

Clotet Sala, Bonaventura

Keppler, Oliver T.

Telenti, Amalio

Kräusslich, Hans-Georg

Martinez-Picado, Javier

Universitat Autònoma de Barcelona

Diposit Digital de Documents de la UAB

English

Siglec-1 Is a Novel Dendritic Cell Receptor That Mediates HIV-1 Trans -Infection Through Recognition of Viral Membrane Gangliosides

Maria C Puertas

Maria T Rodriguez-Plata

Oliver T Keppler

Directory of Open Access Journals

Siglec-1 is a novel dendritic cell receptor that mediates HIV-1 trans-infection through recognition of viral membrane gangliosides.

Crossref

Siglec-1 Is a Novel Dendritic Cell Receptor That Mediates HIV-1 Trans-Infection Through Recognition of Viral Membrane Gangliosides

Izquierdo-Useros, N.

Lorizate, M.

Puertas, M.C.

Rodriguez-Plata, M.T.

Zangger, N.

Erikson, E.

Pino, M.

Erkizia, I.

Glass, B.

Clotet, B.

Keppler, O.T.

Telenti, A.

Kräusslich, H.G.

Martinez-Picado, J.

Serveur académique lausannois

<div>Dendritic cells (DCs) are essential antigen-presenting cells for the induction of immunity against pathogens. However, HIV-1 spread is strongly enhanced in clusters of DCs and CD4+ T cells. Uninfected DCs capture HIV-1 and mediate viral transfer to bystander CD4+ T cells through a process termed trans-infection. Initial studies identified the C-type lectin DC-SIGN as the HIV-1 binding factor on DCs, which interacts with the viral envelope glycoproteins. Upon DC maturation, however, DC-SIGN is down-regulated, while HIV-1 capture and trans-infection is strongly enhanced via a glycoprotein-independent capture pathway that recognizes sialyllactose-containing membrane gangliosides. Here we show that the sialic acid-binding Ig-like lectin 1 (Siglec-1, CD169), which is highly expressed on mature DCs, specifically binds HIV-1 and vesicles carrying sialyllactose. Furthermore, Siglec-1 is essential for trans-infection by mature DCs. These findings identify Siglec-1 as a key factor for HIV-1 spread via infectious DC/T-cell synapses, highlighting a novel mechanism that mediates HIV-1 dissemination in activated tissues. </div

Nuria Izquierdo-Useros (91232)

Maier Lorizate (108435)

Maria C. Puertas (109964)

Maria T. Rodriguez-Plata (109967)

Nadine Zangger (109972)

Elina Erikson (109976)

Maria Pino (109981)

Itziar Erkizia (109986)

Bärbel Glass (81638)

Bonaventura Clotet (91238)

Oliver T. Keppler (109989)

Amalio Telenti (25361)

Hans-Georg Kräusslich (7273)

Javier Martinez-Picado (91236)

FigShare

Siglec-1 Is a Novel Dendritic Cell Receptor That Mediates HIV-1 Trans-Infection Through Recognition of Viral Membrane Gangliosides

A cryptic sensor for HIV-1 activates antiviral innate immunity in dendritic cells.

Activation of the lectin DC-SIGN induces an immature dendritic cell phenotype triggering Rho-GTPase activity required for HIV-1 replication.

affy—analysis of Affymetrix GeneChip data at the probe level.

Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method.

Capture and transfer of HIV-1 particles by mature dendritic cells converges with the exosome-dissemination pathway.

Characterization of human sialoadhesin, a sialic acid binding receptor expressed by resident and inflammatory macrophage populations.

Cimarelli A

Controlling the false discovery rate: a practical and powerful approach to multiple testing.

Cutting edge: CD43 functions as a T cell counterreceptor for the macrophage adhesion receptor sialoadhesin (Siglec-1).

DC-SIGN, a dendritic cell-specific HIV-1-binding protein that enhances trans-infection of T cells.

DC-SIGN: escape mechanism for pathogens.

Dendritic cells exposed to human immunodeficiency virus type-1 transmit a vigorous cytopathic infection to CD4+ T cells.

Differential transmission of human Immunodeficiency virus type 1 by distinct subsets of effector dendritic cells.

Distribution and threedimensional structure of AIDS virus envelope spikes.

Double-labelled HIV-1 particles for study of virus-cell interaction.

Exosomes: endosomal-derived vesicles shipping extracellular messages.

HIV-1 capture and antigen presentation by dendritic cells: enhanced viral capture does not correlate with better T cell activation.

HIV-1 incorporation of host-cell-derived glycosphingolipid GM3 allows for capture by mature dendritic cells.

HIV-1 trafficking to the dendritic cell-T-cell infectious synapse uses a pathway of tetraspanin sorting to the immunological synapse.

HIV-1-infected monocyte-derived dendritic cells do not undergo maturation but can elicit IL-10 production and T cell regulation.

Human immunodeficiency virus type 1 env clones from acute and early subtype B infections for standardized assessments of vaccine-elicited neutralizing antibodies.

Human rhinoviruses inhibit the accessory function of dendritic cells by inducing sialoadhesin and B7-H1 expression.

Immunodeficiency virus uptake, turnover, and 2-phase transfer in human dendritic cells. Blood 103: 2170–2179.

Indirect activation of naı ¨ve CD4+ T cells by dendritic cell-derived exosomes.

Influence of plasma viremia on defects in number and immunophenotype of blood dendritic cell subsets in human immunodeficiency virus 1-infected individuals.

Limma: linear models for microarray data. In:

Microbial translocation is a cause of systemic immune activation in chronic HIV infection.

Recruitment of HIV and its receptors to dendritic cell-T cell junctions.

Retroviruses human immunodeficiency virus and murine leukemia virus are enriched in phosphoinositides.

SAMHD1 is the dendritic- and myeloid-cell-specific HIV-1 restriction factor counteracted by Vpx.

Sialic acid binding receptors (siglecs) expressed by macrophages.

Sialoadhesin (CD169) expression in CD14+ cells is upregulated early after HIV-1 infection and increases during disease progression.

Sialoadhesin expressed on IFNinduced monocytes binds HIV-1 and enhances infectivity.

Sialyllactose in viral membrane gangliosides is a novel molecular recognition pattern for mature dendritic cell capture of HIV-1. PLoS

Siglecs as positive and negative regulators of the immune system.

Siglecs facilitate HIV-1 infection of macrophages through adhesion with viral sialic acids.

Subcapsular sinus macrophages in lymph nodes clear lymph-borne viruses and present them to antiviral B cells.

Subcapsular sinus macrophages prevent CNS invasion on peripheral infection with a neurotropic virus.

The interaction of HIV with dendritic cells: outcomes and pathways.

The lipidomes of vesicular stomatitis virus, semliki forest virus, and the host plasma membrane analyzed by quantitative shotgun mass spectrometry.

Varki A

Vpx relieves inhibition of HIV-1 infection of macrophages mediated by the SAMHD1 protein.

https://figshare.com/articles/Siglec_1_Is_a_Novel_Dendritic_Cell_Receptor_That_Mediates_HIV_1_Trans_Infection_Through_Recognition_of_Viral_Membrane_Gangliosides__/115954

Siglec-1 is a novel dendritic cell receptor that mediates HIV-1 trans-infection through recognition of viral membrane gangliosides.

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