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Inhibition of human immunodeficiency virus type 1 replication in human cells by Debio-025, a novel cyclophilin binding agent.新型亲环素结合剂Debio-025对人细胞中1型人类免疫缺陷病毒复制的抑制作用
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Curr HIV Res. 2007 Nov;5(6):514-41. doi: 10.2174/157016207782418489.
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Broad HIV-1 neutralization mediated by CD4-binding site antibodies.由CD4结合位点抗体介导的广泛HIV-1中和作用。
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Extensively cross-reactive anti-HIV-1 neutralizing antibodies induced by gp140 immunization.由gp140免疫诱导产生的广泛交叉反应性抗HIV-1中和抗体。
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Cross-reactive HIV-1 neutralizing monoclonal antibodies selected by screening of an immune human phage library against an envelope glycoprotein (gp140) isolated from a patient (R2) with broadly HIV-1 neutralizing antibodies.通过筛选免疫人噬菌体文库以对抗从具有广泛HIV-1中和抗体的患者(R2)分离出的包膜糖蛋白(gp140)而选择的交叉反应性HIV-1中和单克隆抗体。
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10
FcRn mediates elongated serum half-life of human IgG in cattle.FcRn介导牛体内人IgG血清半衰期延长。
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用与IgG1 Fc融合的gp41免疫的兔子血清IgG的交叉反应性HIV-1中和活性:免疫原延长半衰期的可能作用。

Cross-reactive HIV-1-neutralizing activity of serum IgG from a rabbit immunized with gp41 fused to IgG1 Fc: possible role of the prolonged half-life of the immunogen.

作者信息

Zhang Mei-Yun, Wang Yanping, Mankowski Marie K, Ptak Roger G, Dimitrov Dimiter S

机构信息

Center for Cancer Research Nanobiology Program, CCR, NCI-Frederick, NIH, Frederick, MD 21702, USA.

出版信息

Vaccine. 2009 Feb 5;27(6):857-63. doi: 10.1016/j.vaccine.2008.11.083. Epub 2008 Dec 10.

DOI:10.1016/j.vaccine.2008.11.083
PMID:19084043
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3399430/
Abstract

The elicitation of broadly cross-reactive HIV-1 neutralizing antibodies in humans remains a major challenge in developing a viable AIDS vaccine. We hypothesized that prolonged exposure to candidate vaccine immunogens could enhance the elicitation of such antibodies. In an attempt to develop HIV-1 vaccine immunogens with prolonged half-lives and increased stability, we constructed a fusion protein, gp41Fc, in which a truncated HIV-1 gp41(89.6) was fused to a human IgG(1) Fc. Gp41Fc is stable in solution, retains its antigenic structure and is highly immunogenic in rabbits. The serum titers reached 1:102,400 for the gp41Fc and 1:5,120 for gp140(89.6). Rabbit IgG neutralized diverse HIV-1 isolates and HIV-2, and the neutralization activity was attributed to gp41-specific IgG. The concentration of the gp41Fc in the serum correlated with the neutralization activity of rabbit IgG which recognized mostly conformation-independent epitopes on gp41 and predominantly bound to peptides derived from the gp41 immunodominant loop region. These results suggest that the prolonged half-life of gp41Fc in the serum may enhance the generation of cross-reactive neutralizing antibodies. Further research is needed to confirm and extend these results which may have implications for the development of vaccine immunogens with enhanced capability to elicit cross-reactive HIV-1-neutralizing antibodies.

摘要

在人类中诱导产生广泛交叉反应的HIV-1中和抗体仍然是开发可行的艾滋病疫苗的一项重大挑战。我们假设长时间暴露于候选疫苗免疫原可以增强此类抗体的诱导。为了开发具有延长半衰期和更高稳定性的HIV-1疫苗免疫原,我们构建了一种融合蛋白gp41Fc,其中截短的HIV-1 gp41(89.6)与人类IgG(1) Fc融合。Gp41Fc在溶液中稳定,保留其抗原结构,并且在兔中具有高度免疫原性。gp41Fc的血清滴度达到1:102,400,gp140(89.6)的血清滴度达到1:5,120。兔IgG中和多种HIV-1分离株和HIV-2,并且中和活性归因于gp41特异性IgG。血清中gp41Fc的浓度与兔IgG的中和活性相关,兔IgG主要识别gp41上不依赖构象的表位,并主要结合来自gp41免疫显性环区域的肽。这些结果表明,gp41Fc在血清中的延长半衰期可能增强交叉反应性中和抗体的产生。需要进一步研究来证实和扩展这些结果,这可能对开发具有更强能力诱导交叉反应性HIV-1中和抗体的疫苗免疫原有影响。