CD4+ binding proteins as immunosuppression factors
CD4结合蛋白作为免疫抑制因子
基本信息
- 批准号:6432010
- 负责人:
- 金额:--
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:
- 资助国家:美国
- 起止时间:至
- 项目状态:未结题
- 来源:
- 关键词:CD4 molecule CD40 molecule HIV envelope protein gp120 HIV infections T cell receptor apoptosis athymic mouse gel electrophoresis helper T lymphocyte human tissue immunologic assay /test immunosuppression neoplasm /cancer immunology neoplasm /cancer transplantation receptor binding recombinant proteins xenotransplantation
项目摘要
It appears that there is a conformation change in the C4 domain of HIV gp120 that allows gp120 to evade a neutralizing immune response and which may contribute to the toxicity of gp120. We synthesized peptides from the C4 domain of gp120 in 2 forms; helical and cyclic. We learned that both forms, although having the same amino acid sequence and ability to bind recombinant soluble CD4, have very different immunological properties. When the C4 peptomer having an alpha helical conformation is used as the immunogen in monkeys, antibodies are formed that react with the parent gp120 but the antibodies do not block gp120 binding to CD4 and they do not inhibit HIV infection in vitro. Monkeys that were immunized with the peptomer had a very pronounced T helper cell response but, surprisingly, showed increased viremia following intrarectal challenge with live SIV. It thus appears that in monkeys C4 is contributing to SIV disease progression. 9 out of 10 human sera that were HIV+ contain antibodies that react with the C4 peptomer in the helical conformation but 3 out of 10 had antibodies that reacted with C4 in the cyclic conformation. In addition, this year we learned that, when the cyclic C4 peptide is used as an immunogen in rabbits, antibodies are formed that react with the parent gp120 but they do not block gp120 binding to CD4. In addition, these antibodies magnify the toxic effects of gp120 on T cell production of IL-2, probably by crosslinking CD4 on the T cell surface. Affinity purified human anti cyclic C4 antibodies also augmented IL-2 attenuation by gp120. In summary, natural HIV infection causes the production of antibodies against the linear, helical and/or cyclic C4 peptide but, the antibodies appear to be harmful to the HIV+ host. Thus, even though the C4 domain of gp120 is highly conserved, it contributes to HIV pathogenesis by avoiding neutralizing immune responses The end result represents another way HIV protects itself from destruction by the immune system. The work clearly signals immune responses against C4 as being harmful and studies of future vaccine formulations should carefully focus in part on the harmful roles played by C4 if the C4 domain is a component of the vaccine.
似乎HIV gp 120的C4结构域中存在构象变化,其允许gp 120逃避中和免疫应答,并且这可能有助于gp 120的毒性。 我们从gp 120的C4结构域合成了两种形式的肽:螺旋和环状。 我们了解到,这两种形式虽然具有相同的氨基酸序列和结合重组可溶性CD 4的能力,但具有非常不同的免疫学特性。 当将具有α螺旋构象的C4肽异构体用作猴的免疫原时,形成与亲本gp 120反应的抗体,但该抗体不阻断gp 120与CD 4的结合,并且它们在体外不抑制HIV感染。 用肽异构体免疫的猴子有非常明显的T辅助细胞应答,但令人惊讶的是,在用活SIV直肠内攻击后显示出增加的病毒血症。 因此,在猴子中,C4似乎有助于SIV疾病的进展。 10份HIV+人血清中有9份含有与螺旋构象的C4肽异构体反应的抗体,但10份中有3份含有与环状构象的C4反应的抗体。此外,今年我们了解到,当环C4肽用作兔的免疫原时,会形成与亲本gp 120反应的抗体,但它们不会阻止gp 120与CD 4结合。 此外,这些抗体放大了gp 120对T细胞产生IL-2的毒性作用,可能是通过交联T细胞表面上的CD 4。 亲和纯化的人抗环C4抗体也增强了gp 120对IL-2的衰减。 总之,天然HIV感染引起针对线性、螺旋和/或环状C4肽的抗体的产生,但是抗体似乎对HIV+宿主有害。 因此,尽管gp 120的C4结构域是高度保守的,但它通过避免中和免疫反应而有助于HIV发病。最终结果代表了HIV保护自身免受免疫系统破坏的另一种方式。这项工作清楚地表明,针对C4的免疫反应是有害的,如果C4结构域是疫苗的一个组成部分,未来疫苗制剂的研究应谨慎地部分关注C4所起的有害作用。
项目成果
期刊论文数量(0)
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会议论文数量(0)
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Frank A. Robey其他文献
Frank A. Robey的其他文献
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{{ truncateString('Frank A. Robey', 18)}}的其他基金
An AIDS Vaccine Cocktail Composed of 2 Conserved Conformational Immunogens
由 2 种保守构象免疫原组成的艾滋病疫苗混合物
- 批准号:
7164476 - 财政年份:2006
- 资助金额:
-- - 项目类别:
Thioether cross-linked 4E10 peptide epitope from gp41
来自 gp41 的硫醚交联 4E10 肽表位
- 批准号:
6947131 - 财政年份:2005
- 资助金额:
-- - 项目类别: