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Literature DB >> 24739247

In vivo immunogenicity of Tax(11-19) epitope in HLA-A2/DTR transgenic mice: implication for dendritic cell-based anti-HTLV-1 vaccine.

Divya Sagar¹, Shet Masih¹, Todd Schell², Steven Jacobson³, Joseph D Comber⁴, Ramila Philip⁴, Brian Wigdahl⁵, Pooja Jain⁶, Zafar K Khan⁷.

Abstract

Viral oncoprotein Tax plays key roles in transformation of human T-cell leukemia virus (HTLV-1)-infected T cells leading to adult T-cell leukemia (ATL), and is the key antigen recognized during HTLV-associated myelopathy (HAM). In HLA-A2+ asymptomatic carriers as well as ATL and HAM patients, Tax(11-19) epitope exhibits immunodominance. Here, we evaluate CD8 T-cell immune response against this epitope in the presence and absence of dendritic cells (DCs) given the recent encouraging observations made with Phase 1 DC-based vaccine trial for ATL. To facilitate these studies, we first generated an HLA-A2/DTR hybrid mouse strain carrying the HLA-A2.1 and CD11c-DTR genes. We then studied CD8 T-cell immune response against Tax(11-19) epitope delivered in the absence or presence of Freund's adjuvant and/or DCs. Overall results demonstrate that naturally presented Tax epitope could initiate an antigen-specific CD8T cell response in vivo but failed to do so upon DC depletion. Presence of adjuvant potentiated Tax(11-19)-specific response. Elevated serum IL-6 levels coincided with depletion of DCs whereas decreased TGF-β was associated with adjuvant use. Thus, Tax(11-19) epitope is a potential candidate for the DC-based anti-HTLV-1 vaccine and the newly hybrid mouse strain could be used for investigating DC involvement in human class-I-restricted immune responses.

Entities: Chemical Disease Gene Species

Keywords: CD11c-DTR transgenic mice; Dendritic cells; HLA-A2.1 transgenic mice; HTLV-1; Tax

Mesh：

Substances：

Year: 2014 PMID： 24739247 PMCID： PMC4044917 DOI： 10.1016/j.vaccine.2014.03.087

Source DB: PubMed Journal: Vaccine ISSN： 0264-410X Impact factor: 3.641

65 in total

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4. Viral antigens detectable in CSF exosomes from patients with retrovirus associated neurologic disease: functional role of exosomes.

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