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树突状细胞在 HIV-1 的天然免疫和适应性免疫的界面

Dendritic cells at the interface of innate and adaptive immunity to HIV-1.

机构信息

Department of Microbiology, Tumor and Cell Biology bCenter for Infectious Medicine, Department of Medicine, Karolinska Institutet, Stockholm, Sweden.

出版信息

Curr Opin HIV AIDS. 2011 Sep;6(5):405-10. doi: 10.1097/COH.0b013e328349b06b.

Abstract

PURPOSE OF REVIEW

This review summarizes recent findings on how HIV-1 infection affects dendritic cells in their ability to elicit innate and adaptive immune responses.

RECENT FINDINGS

The phenomenon describing a reduction of dendritic cell numbers in the blood of HIV-1-infected individuals has been expanded on in recent studies demonstrating that dendritic cells decline very early in primary infection and that there is a mobilization of semi-mature dendritic cells to lymph nodes. Recent data suggest that dendritic cells in lymph nodes are more prone to apoptosis, which correlates with disease progression. In addition, plasmacytoid dendritic cells isolated from blood showed a semi-mature phenotype after HIV-1 exposure, which coincided with persistent IFN-α secretion. Emerging data show that semi-mature dendritic cells induce regulatory T cells and suppress effector function. There may therefore be mechanisms by which HIV-1 affects dendritic cell immune stimulation and, in doing so, interferes with the elicitation of anti-HIV-1 responses.

SUMMARY

Understanding how dendritic cells are functionally altered during HIV-1 infection is crucial for the development of new immune-therapy strategies including approaches to target dendritic cells with antigen in vivo or ex vivo to induce efficient adaptive anti-HIV immunity.

摘要

目的综述

本文总结了 HIV-1 感染如何影响树突状细胞(DC),从而影响固有和适应性免疫反应的最新发现。

最近的发现

描述 HIV-1 感染个体血液中 DC 数量减少的现象,在最近的研究中得到了扩展,这些研究表明,在原发性感染中,DC 数量很早就会下降,并且半成熟 DC 会向淋巴结动员。最近的数据表明,淋巴结中的 DC 更容易发生凋亡,这与疾病进展相关。此外,从血液中分离出的浆细胞样树突状细胞在接触 HIV-1 后表现出半成熟表型,同时持续分泌 IFN-α。新出现的数据表明,半成熟 DC 可诱导调节性 T 细胞并抑制效应功能。因此,HIV-1 可能通过影响 DC 的免疫刺激来影响其功能,从而干扰抗 HIV-1 反应的产生。

总结

了解 HIV-1 感染期间 DC 如何发生功能改变,对于开发新的免疫治疗策略至关重要,包括用抗原靶向体内或体外 DC 以诱导有效的适应性抗 HIV 免疫的方法。

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