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The peptide-HLA class I tetramer is a valuable tool for rapid and detailed characterization of epitope specific CD8+T cells.

Products

CLGGLLTMV-A0201

Catalog no.
1002-04
Group
HLA-A
Alpha chain
HLA-A0201
Beta chain
b2m
Peptide
CLGGLLTMV
Peptide source
LMP2, EBV
Format
monomer,tetramer
Storage
Monomers (-20°C), Tetramers (4°C)
Buffer
TRIS/MALEATE pH 7
Shelf life
18 Months
Application
FCM
For Research Use Only (RUO)
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Published Research using immunAware reagents and services

08/03/2024

Science advances

Coxsackievirus infection induces direct pancreatic _ cell killing but poor antiviral CD8+ T cell responses
Coxsackievirus B (CVB) infection of pancreatic _ cells is associated with _ cell autoimmunity and type 1 diabetes. We investigated how CVB affects human _ cells and anti-CVB T cell responses. _ cells were efficiently infected by CVB in vitro, down-regulated human leukocyte antigen (HLA) class I, and presented few, selected HLA-bound viral peptides. Circulating CD8+ T cells from CVB-seropositive individuals recognized a fraction of these peptides; only another subfraction was targeted by effector/memory T cells that expressed exhaustion marker PD-1. T cells recognizing a CVB epitope cross-reacted with _ cell antigen GAD. Infected _ cells, which formed filopodia to propagate infection, were more efficiently killed by CVB than by CVB-reactive T cells. Our in vitro and ex vivo data highlight limited CD8+ T cell responses to CVB, supporting the rationale for CVB vaccination trials for type 1 diabetes prevention. CD8+ T cells recognizing structural and nonstructural CVB epitopes provide biomarkers to differentially follow response to infection and vaccination.

08/03/2024

Science advances

Coxsackievirus infection induces direct pancreatic β cell killing but poor antiviral CD8+ T cell responses
Coxsackievirus B (CVB) infection of pancreatic β cells is associated with β cell autoimmunity and type 1 diabetes. We investigated how CVB affects human β cells and anti-CVB T cell responses. β cells were efficiently infected by CVB in vitro, down-regulated human leukocyte antigen (HLA) class I, and presented few, selected HLA-bound viral peptides. Circulating CD8+ T cells from CVB-seropositive individuals recognized a fraction of these peptides; only another subfraction was targeted by effector/memory T cells that expressed exhaustion marker PD-1. T cells recognizing a CVB epitope cross-reacted with β cell antigen GAD. Infected β cells, which formed filopodia to propagate infection, were more efficiently killed by CVB than by CVB-reactive T cells. Our in vitro and ex vivo data highlight limited CD8+ T cell responses to CVB, supporting the rationale for CVB vaccination trials for type 1 diabetes prevention. CD8+ T cells recognizing structural and nonstructural CVB epitopes provide biomarkers to differentially follow response to infection and vaccination.