Evento

A lectin from Heliantus Annus recongizes GP120 from HIV-1 and promotes an inflammatory phenotype in dendritic cells

Chop, MaiaIcon ; Radicioni, Melisa BelénIcon ; del Rio, Marianela VictoriaIcon ; Sabatte, Juan AtilioIcon ; Regente, Mariana CleliaIcon ; Rodríguez Rodrígues, Christian Fernando ArielIcon
Tipo del evento: Congreso
Nombre del evento: Reunión de Sociedades de Biociencias 2023; LXVIII Annual Meeting of Sociedad Argentina de Investigación Clínica (Saic); Xxv Annual Conferences of Sociedad Argentina de Biología (Sab); Lv Annual Meeting of Asociación Argentina de Farmacología Experimental (Aafe); Viii Regional Scientific Meeting of Asociación Argentina de Ciencia y Tecnología de Animales de Laboratorio (Aacytal)
Fecha del evento: 15/11/2023
Institución Organizadora: Sociedad Argentina de Investigación Clínica; Sociedad Argentina de Biología; Asociación Argentina de Farmacología Experimental; Asociación Argentina de Ciencia y Tecnología de Animales de Laboratorio;
Título de la revista: Medicina
Editorial: Fundación Revista Medicina
ISSN: 1669-9106
Idioma: Español
Clasificación temática:

Resumen

Background: Helja is a mannose-binding lectin that is isolated fromsunflower seeds. HIV-1 envelope glycoprotein (gp120) containshigh-mannose and complex N-glycans. The aim of this study wasto analyze whether Helja recognizes gp120 and induces maturationand pro-inflammatory cytokine transcription in dendritic cells (BMDCs).Methods: Helja was purified from Helianthus annuus seedsusing D-mannose-agarose affinity chromatography. Molecular interactionsbetween Helja and recombinant gp120 were evaluatedby dot and ligand blot approaches using anti-Helja antibodies. BMDCswere cultured in complete RPMI medium supplemented withFLT3-L. Cell phenotype was evaluated in Helja-treated BMDCs bymeasuring membrane proteins (CD86, CD40, MHCII, CD11c, CD80,Clec9a, Ly6G, SIPRα, CD103 and SiglecH) by FACS. BMDCs cytokineprofiles were analyzed using RT-qPCR (il-6, tnf-α, il-12, inf-αtgf-b, and il-10). Results: Helja-gp120 interactions were measuredby immunodetection and confirmed by ligand blot assays. A signaldot was observed at a MW of 95 kDa. Next, BMDCs were stimulatedwith Helja (10 μg/ml) to evaluate cell activation. The lectin induced amarked upregulation of MHCII, MHCI, CD80, CD40 and CD86 (n=3,**p<0.01 Helja-treated BMDCs vs control, *p<0.05 Helja+LPS-treatedBMDCs vs LPS control). No changes in Clec9a, Ly6G, SIRPα,CD103 and SiglecH were detected. Finally, Helja also induced thetranscriptional activity of pro-inflammatory and antiviral cytokines(il-6, tnf-α, il-12 and inf-α (n=3, *p<0,05, **p<0,01, ***p<0,001 vscontrol) resulting in an additive effect with LPS. No increase in anti-inflammatory cytokines (tgf-b, il-10) was observed. Conclusions:Helja recognizes specific glycosidic residues and arrangements ofgp120 in HIV-1, which induces dendritic cell maturation. This promotesimmune activation, leading to the release of proinflammatorycytokines by BMDCs. These results suggest that this lectin has potentialbiomedical applications as an antiviral agent.
Palabras clave: MANNOSE-BINDING LECTIN , JACALIN , HIV , ANTIVIRAL
 
Archivos asociados
Thumbnail
 
Tamaño: 2.435Mb
Formato: PDF
.
Licencia
info:eu-repo/semantics/openAccess Excepto donde se diga explícitamente, este item se publica bajo la siguiente descripción: Creative Commons Attribution-NonCommercial-ShareAlike 2.5 Unported (CC BY-NC-SA 2.5)
Identificadores
URI: http://hdl.handle.net/11336/262011
URL: https://www.saic.org.ar/revista-medicina
Colecciones
Eventos(IIB)
Eventos de INSTITUTO DE INVESTIGACIONES BIOLOGICAS
Citación
A lectin from Heliantus Annus recongizes GP120 from HIV-1 and promotes an inflammatory phenotype in dendritic cells; Reunión de Sociedades de Biociencias 2023; LXVIII Annual Meeting of Sociedad Argentina de Investigación Clínica (Saic); Xxv Annual Conferences of Sociedad Argentina de Biología (Sab); Lv Annual Meeting of Asociación Argentina de Farmacología Experimental (Aafe); Viii Regional Scientific Meeting of Asociación Argentina de Ciencia y Tecnología de Animales de Laboratorio (Aacytal); Mar del Plata; Argentina; 2023; 207-208
Compartir