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非洲人群中的Tat突变不影响反式激活,但会改变其免疫原性。

Tat mutations in an African cohort that do not prevent transactivation but change its immunogenic properties.

作者信息

Campbell Grant R, Senkaali David, Watkins Jennifer, Esquieu Didier, Opi Sandrine, Yirrell David L, Kaleebu Pontiano, Loret Erwann P

机构信息

CNRS Formation de Recherche en Evolution 2737, Faculté de Pharmacie, Université de la Méditerranée, 27 Boulevard Jean Moulin, 13385 Marseille Cedex 5, France.

出版信息

Vaccine. 2007 Dec 5;25(50):8441-7. doi: 10.1016/j.vaccine.2007.09.070. Epub 2007 Oct 22.

Abstract

Humoral responses against extra-cellular HIV-1 Tat may be beneficial as Tat has been implicated in the viral pathogenesis associated with HIV-1 disease progression. We determined the levels of anti-Tat IgG in sera of HIV-1 seropositive individuals from the Rural Clinical Cohort in Uganda using nine different Tat proteins representative of the major subtypes presently accounting for 97% of infections worldwide. We observed the presence of anti-Tat IgG able to react against the various subtypes tested, although none cross-reacted against all nine variants. We show that 46.25% of seropositive patients were able to recognise at least one Tat variant with 1:1000 sera dilution. We also show that the C terminus of Tat is the most variable region and an important epitope that might explain the limitation of cross-recognition of Tat antibodies regarding Tat variants. This study shows in seropositive patients that Tat can tolerate mutations without modification of its primary function but with changes in its immunogenic properties. These findings should be considered when designing Tat-based HIV-1 vaccines.

摘要

针对细胞外HIV-1反式激活因子(Tat)的体液免疫反应可能有益,因为Tat与HIV-1疾病进展相关的病毒发病机制有关。我们使用代表目前占全球感染97%的主要亚型的九种不同Tat蛋白,测定了乌干达农村临床队列中HIV-1血清阳性个体血清中的抗Tat IgG水平。我们观察到存在能够与所测试的各种亚型发生反应的抗Tat IgG,尽管没有一种能与所有九种变体发生交叉反应。我们发现,46.25%的血清阳性患者在血清稀释度为1:1000时能够识别至少一种Tat变体。我们还表明,Tat的C末端是最可变的区域,也是一个重要的表位,这可能解释了Tat抗体对Tat变体交叉识别的局限性。这项研究表明,在血清阳性患者中,Tat可以耐受突变,而其主要功能不变,但免疫原性发生改变。在设计基于Tat的HIV-1疫苗时应考虑这些发现。

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