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本文引用的文献

1
Inclusion of the bovine neutrophil beta-defensin 3 with glycoprotein D of bovine herpesvirus 1 in a DNA vaccine modulates immune responses of mice and cattle.将牛嗜中性粒细胞β-防御素3与牛疱疹病毒1的糖蛋白D一起包含在DNA疫苗中可调节小鼠和牛的免疫反应。
Clin Vaccine Immunol. 2014 Apr;21(4):463-77. doi: 10.1128/CVI.00696-13. Epub 2014 Jan 22.
2
Biologic activities of recombinant human-beta-defensin-4 toward cultured human cancer cells.重组人β-防御素-4对培养的人癌细胞的生物学活性。
Exp Oncol. 2013 Jun;35(2):76-82.
3
The mouse dendritic cell marker CD11c is down-regulated upon cell activation through Toll-like receptor triggering.小鼠树突状细胞标志物 CD11c 在通过 Toll 样受体触发的细胞激活时下调。
Immunobiology. 2013 Jan;218(1):28-39. doi: 10.1016/j.imbio.2012.01.021. Epub 2012 Feb 21.
4
The synthetic peptides bovine enteric β-defensin (EBD), bovine neutrophil β-defensin (BNBD) 9 and BNBD 3 are chemotactic for immature bovine dendritic cells.合成肽牛肠道β-防御素(EBD)、牛中性粒细胞β-防御素(BNBD)9和BNBD 3对未成熟牛树突状细胞具有趋化作用。
Vet Immunol Immunopathol. 2011 Sep 15;143(1-2):87-107. doi: 10.1016/j.vetimm.2011.06.028. Epub 2011 Jun 24.
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Effects on antigen-presenting cells of short-term interaction with the human host defence peptide β-defensin 2.与人类防御肽 β-防御素 2 短期相互作用对抗原呈递细胞的影响。
Biochem J. 2011 Jun 15;436(3):537-46. doi: 10.1042/BJ20101977.
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A peptide-based vector for efficient gene transfer in vitro and in vivo.一种基于肽的载体,可在体外和体内高效进行基因转移。
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N-terminal glutamate to pyroglutamate conversion in vivo for human IgG2 antibodies.人源 IgG2 抗体体内 N 端谷氨酸至焦谷氨酸的转化。
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Liposomal delivery of p-ialB and p-omp25 DNA vaccines improves immunogenicity but fails to provide full protection against B. melitensis challenge.脂质体递送的p-ialB和p-omp25 DNA疫苗可提高免疫原性,但未能完全保护机体免受布鲁氏菌的攻击。
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Human beta-defensin 2 and 3 and their mouse orthologs induce chemotaxis through interaction with CCR2.人β-防御素 2 和 3 及其鼠同源物通过与 CCR2 的相互作用诱导趋化作用。
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Specific binding and chemotactic activity of mBD4 and its functional orthologue hBD2 to CCR6-expressing cells.mBD4 及其功能同源物 hBD2 对 CCR6 表达细胞的特异性结合和趋化活性。
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与牛中性粒细胞β-防御素3复合的牛疱疹病毒1糖蛋白D DNA疫苗的免疫原性

Immunogenicity of a bovine herpesvirus 1 glycoprotein D DNA vaccine complexed with bovine neutrophil beta-defensin 3.

作者信息

Mackenzie-Dyck Sarah, Latimer Laura, Atanley Ethel, Kovacs-Nolan Jennifer, Attah-Poku Sam, Babiuk Lorne A, van Drunen Littel-van den Hurk Sylvia

机构信息

VIDO-InterVac, University of Saskatchewan, Saskatoon, Canada Veterinary Microbiology, University of Saskatchewan, Saskatoon, Canada.

VIDO-InterVac, University of Saskatchewan, Saskatoon, Canada.

出版信息

Clin Vaccine Immunol. 2015 Jan;22(1):79-90. doi: 10.1128/CVI.00476-14. Epub 2014 Nov 5.

DOI:10.1128/CVI.00476-14
PMID:25378352
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4278921/
Abstract

Protective efficacy against bovine herpesvirus 1 (BoHV-1) has been demonstrated to be induced by a plasmid encoding bovine neutrophil beta-defensin 3 (BNBD3) as a fusion construct with truncated glycoprotein D (tgD). However, in spite of the increased cell-mediated immune responses induced by this DNA vaccine, the clinical responses of BoHV-1-challenged cattle were not reduced over those observed in animals vaccinated with the plasmid encoding tgD alone; this might have been because the vaccine failed to improve humoral responses. We hypothesized that an alternative vaccine design strategy that utilized the DNA vaccine pMASIA-tgD as a complex with BNBD3 might improve humoral responses while maintaining robust Th1-type cell-mediated responses. C57BL/6 mice were vaccinated with pMASIA-tgD complexed with 0, 0.01875, 0.1875, or 1.875 nmol of a stable synthesized analog of BNBD3 (aBNBD3). The best results were seen in mice immunized with the vaccine composed of pMASIA-tgD complexed to 0.1875 nmol aBNBD3. In this group, humoral responses were improved, as evidenced by increased virus neutralization, tgD-specific early IgG1, and later IgG2a titers, while the strong cell-mediated immune responses, measured based on specific gamma interferon (IFN-γ)-secreting cells, were maintained relative to pMASIA-tgD. Modulation of the immune response might have been due in part to the effect of BNBD3 on dendritic cells (DCs). In vitro studies showed that murine bone marrow-derived DCs (BMDCs) pretreated with aBNBD3 were activated, as evidenced by CD11c downregulation, and were functionally mature, as shown by increased allostimulatory ability. Native, synthetic, and analog forms of BNBD3 were equally capable of inducing functional maturation of BMDCs.

摘要

编码牛中性粒细胞β-防御素3(BNBD3)与截短的糖蛋白D(tgD)融合构建体的质粒已被证明可诱导对牛疱疹病毒1型(BoHV-1)的保护效力。然而,尽管这种DNA疫苗诱导的细胞介导免疫反应有所增强,但与仅接种编码tgD的质粒的动物相比,BoHV-1攻击的牛的临床反应并未降低;这可能是因为该疫苗未能改善体液反应。我们推测,一种利用DNA疫苗pMASIA-tgD与BNBD3形成复合物的替代疫苗设计策略,可能在维持强大的Th1型细胞介导反应的同时改善体液反应。用与0、0.01875、0.1875或1.875 nmol稳定合成的BNBD3类似物(aBNBD3)复合的pMASIA-tgD对C57BL/6小鼠进行免疫接种。在用与0.1875 nmol aBNBD3复合的pMASIA-tgD组成的疫苗免疫的小鼠中观察到了最佳结果。在该组中,体液反应得到改善,病毒中和、tgD特异性早期IgG1和后期IgG2a滴度增加证明了这一点,同时相对于pMASIA-tgD,基于分泌特异性γ干扰素(IFN-γ)的细胞测量的强大细胞介导免疫反应得以维持。免疫反应的调节可能部分归因于BNBD3对树突状细胞(DCs)的作用。体外研究表明,用aBNBD3预处理的小鼠骨髓来源DCs(BMDCs)被激活,CD11c下调证明了这一点,并且其功能成熟,同种异体刺激能力增强表明了这一点。BNBD3的天然、合成和类似物形式同样能够诱导BMDCs的功能成熟。