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在非人灵长类动物中,与佐剂化蛋白加强免疫联合使用时,增强型合成多分支DNA初免可诱导产生更强的跨分支反应性功能性抗体。

An Enhanced Synthetic Multiclade DNA Prime Induces Improved Cross-Clade-Reactive Functional Antibodies when Combined with an Adjuvanted Protein Boost in Nonhuman Primates.

作者信息

Wise Megan C, Hutnick Natalie A, Pollara Justin, Myles Devin J F, Williams Constance, Yan Jian, LaBranche Celia C, Khan Amir S, Sardesai Niranjan Y, Montefiori David, Barnett Susan W, Zolla-Pazner Susan, Ferrari Guido, Weiner David B

机构信息

Department of Pathology, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania, USA.

Department of Surgery, Duke University, Durham, North Carolina, USA.

出版信息

J Virol. 2015 Sep;89(18):9154-66. doi: 10.1128/JVI.00652-15. Epub 2015 Jun 17.

Abstract

UNLABELLED

The search for an efficacious human immunodeficiency virus type 1 (HIV-1) vaccine remains a pressing need. The moderate success of the RV144 Thai clinical vaccine trial suggested that vaccine-induced HIV-1-specific antibodies can reduce the risk of HIV-1 infection. We have made several improvements to the DNA platform and have previously shown that improved DNA vaccines alone are capable of inducing both binding and neutralizing antibodies in small-animal models. In this study, we explored how an improved DNA prime and recombinant protein boost would impact HIV-specific vaccine immunogenicity in rhesus macaques (RhM). After DNA immunization with either a single HIV Env consensus sequence or multiple constructs expressing HIV subtype-specific Env consensus sequences, we detected both CD4(+) and CD8(+) T-cell responses to all vaccine immunogens. These T-cell responses were further increased after protein boosting to levels exceeding those of DNA-only or protein-only immunization. In addition, we observed antibodies that exhibited robust cross-clade binding and neutralizing and antibody-dependent cellular cytotoxicity (ADCC) activity after immunization with the DNA prime-protein boost regimen, with the multiple-Env formulation inducing a more robust and broader response than the single-Env formulation. The magnitude and functionality of these responses emphasize the strong priming effect improved DNA immunogens can induce, which are further expanded upon protein boost. These results support further study of an improved synthetic DNA prime together with a protein boost for enhancing anti-HIV immune responses.

IMPORTANCE

Even with effective antiretroviral drugs, HIV remains an enormous global health burden. Vaccine development has been problematic in part due to the high degree of diversity and poor immunogenicity of the HIV Env protein. Studies suggest that a relevant HIV vaccine will likely need to induce broad cellular and humoral responses from a simple vaccine regimen due to the resource-limited setting in which the HIV pandemic is most rampant. DNA vaccination lends itself well to increasing the amount of diversity included in a vaccine due to the ease of manufacturing multiple plasmids and formulating them as a single immunization. By increasing the number of Envs within a formulation, we were able to show an increased breadth of responses as well as improved functionality induced in a nonhuman primate model. This increased breadth could be built upon, leading to better coverage against circulating strains with broader vaccine-induced protection.

摘要

未标注

寻找一种有效的1型人类免疫缺陷病毒(HIV-1)疫苗仍然是一项紧迫需求。RV144泰国临床疫苗试验取得的一定成功表明,疫苗诱导产生的HIV-1特异性抗体可降低HIV-1感染风险。我们对DNA平台进行了多项改进,并且之前已经表明,改进后的DNA疫苗本身就能在小动物模型中诱导产生结合抗体和中和抗体。在本研究中,我们探究了改进的DNA初免和重组蛋白加强免疫对恒河猴(RhM)体内HIV特异性疫苗免疫原性的影响。在用单一HIV Env共有序列或表达HIV亚型特异性Env共有序列的多个构建体进行DNA免疫后,我们检测到了针对所有疫苗免疫原的CD4(+)和CD8(+) T细胞应答。蛋白加强免疫后,这些T细胞应答进一步增强,达到超过仅DNA免疫或仅蛋白免疫的水平。此外,在用DNA初免-蛋白加强免疫方案免疫后,我们观察到抗体表现出强大的跨亚型结合、中和及抗体依赖性细胞毒性(ADCC)活性,与单一Env制剂相比,多Env制剂诱导产生的应答更强且更广泛。这些应答的强度和功能强调了改进后的DNA免疫原可诱导的强大初免效应,这种效应在蛋白加强免疫后会进一步增强。这些结果支持进一步研究改进的合成DNA初免联合蛋白加强免疫以增强抗HIV免疫应答。

重要性

即使有了有效的抗逆转录病毒药物,HIV仍然是全球巨大的健康负担。疫苗研发一直存在问题,部分原因是HIV Env蛋白的高度多样性和较差的免疫原性。研究表明,鉴于HIV大流行最猖獗地区资源有限的情况,一种相关的HIV疫苗可能需要通过简单的疫苗方案诱导广泛的细胞和体液应答。由于易于生产多种质粒并将它们配制成单次免疫制剂,DNA疫苗非常适合增加疫苗中包含的多样性。通过增加制剂中Env的数量,我们能够在非人灵长类动物模型中展示出应答广度的增加以及诱导产生的功能改善。这种增加的广度可以在此基础上进一步拓展,从而通过更广泛的疫苗诱导保护更好地覆盖流行毒株。

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