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HIV-1 Tat-coated nanoparticles result in enhanced humoral immune responses and neutralizing antibodies compared to alum adjuvant

机译:与明矾佐剂相比,HIV-1 Tat涂层纳米颗粒可增强体液免疫反应并中和抗体

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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. It is well known that protein based vaccines produce poor immune responses by themselves and therefore require adjuvants to enhance immune responses. We have previously reported on the use of anionic nanoparticles (NPs) for enhancing cellular and humoral immune responses to Tat (1-72). The purpose of this study was to further evaluate the immune response of HIV-1 Tat (1-72) coated on anionic nanoparticles compared to alum using various doses of Tat (1-72). Nanoparticles were effective at generating comparable antibody titers at both 1 and 5 microg doses of Tat (1-72), whereas the antibody titers significantly decreased at the lower dose of Tat (1-72) using alum. Anti-sera from Tat (1-72) immunized mice reacted greatest to the N-terminal and basic regions of Tat, with the NP groups showing stronger reactivity to these regions compared to alum. Moreover, the anti-sera from all Tat (1-72) immunized groups contained Tat-neutralizing antibodies and were able to significantly inhibit Tat-mediated long terminal repeat (LTR) transactivation.
机译:HIV-1 Tat已被确定为疫苗开发的诱人靶标,目前正在作为HIV-1的治疗性和预防性疫苗进行临床试验研究。众所周知,基于蛋白质的疫苗本身会产生较差的免疫反应,因此需要佐剂来增强免疫反应。我们先前曾报道过使用阴离子纳米颗粒(NPs)增强对Tat(1-72)的细胞和体液免疫反应。这项研究的目的是与使用不同剂量的达(1-72)的明矾相比,进一步评估包覆在阴离子纳米颗粒上的HIV-1塔(1-72)的免疫反应。纳米颗粒可有效地在1和5微克剂量的Tat(1-72)上产生可比的抗体滴度,而使用明矾在较低剂量的Tat(1-72)上抗体滴度显着降低。来自Tat(1-72)免疫小鼠的抗血清对Tat的N末端和碱性区域反应最大,与明矾相比,NP基团对这些区域的反应性更强。此外,来自所有Tat(1-72)免疫组的抗血清均包含Tat中和抗体,并且能够显着抑制Tat介导的长末端重复(LTR)反式激活。

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