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HERV-K Modulates the Immune Response in ALS Patients

Giannina Arru, Grazia Galleri, Giovanni Deiana, Ignazio Roberto Zarbo, Elia Sechi, Marco Bo, Maria Piera L. Cadoni, Davide Corda, Claudia Frau, Elena Rita Simula, Maria Antonietta Manca, Franca Galistu, Paolo Solla, Roberto Manetti, GianPietro Sechi, Leonardo A. Sechi

2021Microorganisms49 citationsDOIOpen Access PDF

Abstract

Human endogenous retrovirus (HERV)-K env-su glycoprotein has been documented in amyotrophic lateral sclerosis (ALS), where HERV-K env-su 19–37 antibody levels significantly correlated with clinical measures of disease severity. Herein, we investigated further the humoral and cell-mediated immune response against specific antigenic peptides derived from HERV-K in ALS. HERV-K env glycoprotein expression on peripheral blood mononuclear cells (PBMCs) membrane and cytokines and chemokines after stimulation with HERV-K env 19–37 and HERV-K env 109–126 were quantified in patients and healthy controls (HCs). HERV-K env glycoprotein was more expressed in B cells and NK cells of ALS patients compared to HCs, whereas HERV-K env transcripts were similar in ALS and HCs. In ALS patients, specific stimulation with HERV-K env 109–126 peptide showed a higher expression of IL-6 by CD19/B cells. Both peptides, however, were able to induce a great production of IFN-γ by stimulation CD19/B cells, and yielded a higher expression of MIP-1α and a lower expression of MCP-1. HERV-K env 19–37 peptide induced a great production of TNF-α in CD8/T cells. In conclusion, we observed the ability of HERV-K to modulate the immune system, generating mediators mainly involved in proinflammatory response.

Topics & Concepts

Immune systemCD19Peripheral blood mononuclear cellCD8Proinflammatory cytokineImmunologyChemokineGlycoproteinBiologyAntibodyT cellStimulationVirologyAntigenMolecular biologyInflammationIn vitroEndocrinologyBiochemistryAmyotrophic Lateral Sclerosis ResearchNeurogenetic and Muscular Disorders ResearchRNA Research and Splicing
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