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腺苷脱氨酶-1 增强了 HIV-1 包膜 DNA 和蛋白疫苗的生发中心形成和功能性抗体反应。

Adenosine deaminase-1 enhances germinal center formation and functional antibody responses to HIV-1 Envelope DNA and protein vaccines.

机构信息

The Department of Microbiology and Immunology, Drexel University College of Medicine, Philadelphia, PA, United States.

Department of Medicine, Division of Infectious Diseases & HIV Medicine, Drexel University College of Medicine, Philadelphia, PA, United States; The Department of Biochemistry and Cell Biology, Drexel University College of Medicine, Philadelphia, PA, United States.

出版信息

Vaccine. 2020 May 8;38(22):3821-3831. doi: 10.1016/j.vaccine.2020.03.047. Epub 2020 Apr 10.

Abstract

Adenosine deaminase-1 (ADA-1) plays both enzymatic and non-enzymatic roles in regulating immune cell function. Mutations in the ADA1 gene account for 15% of heritable severe-combined immunodeficiencies. We determined previously that ADA1 expression defines and is instrumental for the germinal center follicular helper T cell (T) phenotype using in vitro human assays. Herein, we tested whether ADA-1 can be used as an adjuvant to improve vaccine efficacy in vivo. In vitro, ADA-1 induced myeloid dendritic cell (mDC) maturation as measured by increased frequencies of CD40-, CD83-, CD86-, and HLA-DR-positive mDCs. ADA-1 treatment also promoted the secretion of the T-polarizing cytokine IL-6 from mDCs. In the context of an HIV-1 envelope (env) DNA vaccine, co-immunization with plasmid-encoded ADA-1 (pADA) enhanced humoral immunity. Animals co-immunized with env DNA and pADA had significantly increased frequencies of T cells in their draining lymph nodes and increased HIV-binding IgG in serum. Next, mice were co-immunized with subtype C env gp160 DNA and pADA along with simultaneous immunization with matched gp140 trimeric protein. Mice that received env gp160 DNA, pADA, and gp140 glycoprotein had significantly more heterologous HIV-specific binding IgG in their serum. Furthermore, only these mice had detectable neutralizing antibody responses. These studies support the use of ADA-1 as a vaccine adjuvant to qualitatively enhance germinal center responses and represent a novel application of an existing therapeutic agent that can be quickly translated for clinical use.

摘要

腺苷脱氨酶-1(ADA-1)在调节免疫细胞功能方面具有酶和非酶两种作用。ADA1 基因的突变占遗传性严重联合免疫缺陷的 15%。我们之前已经确定,ADA1 表达定义了生发中心滤泡辅助 T 细胞(T 细胞)表型,并对其具有重要作用,这是通过体外人类检测来实现的。在此,我们测试了 ADA-1 是否可以用作佐剂来提高体内疫苗的功效。体外,ADA-1 通过增加 CD40+、CD83+、CD86+和 HLA-DR+的 mDC 频率来诱导髓样树突状细胞(mDC)成熟。ADA-1 处理还促进了 mDC 中 T 极化细胞因子 IL-6 的分泌。在 HIV-1 包膜(env)DNA 疫苗的背景下,与质粒编码的 ADA-1(pADA)共免疫增强了体液免疫。用 env DNA 和 pADA 共免疫的动物在引流淋巴结中的 T 细胞频率显著增加,血清中 HIV 结合 IgG 也显著增加。接下来,用 C 型 env gp160 DNA 和 pADA 同时对小鼠进行共免疫,并同时免疫匹配的 gp140 三聚体蛋白。接受 env gp160 DNA、pADA 和 gp140 糖蛋白的小鼠血清中具有明显更多的异源 HIV 特异性结合 IgG。此外,只有这些小鼠具有可检测的中和抗体反应。这些研究支持将 ADA-1 用作疫苗佐剂,以定性增强生发中心反应,并代表了一种现有治疗剂的新应用,可快速转化为临床应用。

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