کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
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2402677 | 1102834 | 2012 | 9 صفحه PDF | دانلود رایگان |

HIV-1 Tat has been identified as an attractive target for vaccine development and is currently under investigation in clinical trials as both a therapeutic and preventative vaccine for HIV-1. The Tat C-terminal region is of significant importance for its extracellular activity. In this study, we designed two recombinant Tat immunogens, Tat(B41-100N) and Tat(B41-100C), with two extended Tat C-terminal regions (41–100 aa) and compared their humoral immune response with native Tat. Interestingly, our results showed that Tat(B41-100C) elicited a higher antibody titer than Tat and Tat(B41-100N) in both mice and rabbits. The recombinant fusion protein-based epitope analysis showed that Tat(B41-100C) induced a remarkably enhanced humoral immune response against extended Tat C-terminal regions containing residues 38–100, 49–100 and 60–100. Our study demonstrates that the designed Tat(B41-100C) presents a designed immunogenicity that elicits enhanced Tat-specific antibodies especially against extended Tat C-terminal regions.
► A designed Tat(B41-100C) elicits enhanced Tat-specific antibodies.
► Tat(B41-100C) elicits enhanced anti-Tat C-terminal antibodies.
► Recombinant Tat peptides were designed for determining Tat-specific epitopes.
► Our study contributes to the future improvement of Tat immunogens.
Journal: Vaccine - Volume 30, Issue 14, 23 March 2012, Pages 2453–2461