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在 HIV-1 暴露但未感染的静脉注射吸毒者中,浆细胞样树突状细胞成熟和自然杀伤细胞活化增加。

Increased plasmacytoid dendritic cell maturation and natural killer cell activation in HIV-1 exposed, uninfected intravenous drug users.

机构信息

The Wistar Institute, Philadelphia, Pennsylvania 19104, USA.

出版信息

AIDS. 2010 Sep 10;24(14):2151-60. doi: 10.1097/QAD.0b013e32833dfc20.

Abstract

BACKGROUND

Increased natural killer (NK) activation has been associated with resistance to HIV-1 infection in several cohorts of HIV-1 exposed, uninfected individuals. Inheritance of protective NK receptor alleles (KIR3DS1 and KIR3DL1) has also been observed in a subset of HIV-1 exposed, uninfected individuals. However, the exact mechanism contributing to NK activation in HIV-1 exposed, uninfected intravenous drug users (EU-IDU) remains to be elucidated.

OBJECTIVE

We investigated the role of both host genotype and pathogen-induced dendritic cell modulation of NK activation during high-risk activity in a cohort of 15 EU-IDU individuals and 15 control, uninfected donors from Philadelphia.

DESIGN

We assessed the activation status of NK cells and dendritic cells by flow cytometry and utilized functional assays of NK-DC cross-talk to characterize the innate immune compartment in EU-IDU individuals.

RESULTS

As previously reported, NK cell activation (CD69) and/or degranulation (CD107a) was significantly increased in EU-IDU individuals compared with control uninfected donors (P = 0.0056, n = 13). Genotypic analysis indicated that the frequency of protective KIR (KIR3DS1) and HLA-Bw4*80I ligands was not enriched in our cohort of EU-IDU individuals. Rather, plasmacytoid dendritic cells (PDC) from EU-IDU exhibited heightened maturation (CD83) compared with control uninfected donors (P = 0.0011, n = 12). When stimulated in vitro, both PDCs and NK cells from EU-IDU individuals maintained strong effector cell function and did not exhibit signs of exhaustion.

CONCLUSION

Increased maturation of PDCs is associated with heightened NK activation in EU-IDU individuals suggesting that both members of the innate compartment may contribute to resistance from HIV-1 infection in EU-IDU.

摘要

背景

在几个人群的 HIV-1 暴露未感染个体中,自然杀伤 (NK) 细胞的激活增加与对 HIV-1 感染的抵抗力有关。在一部分 HIV-1 暴露未感染个体中,也观察到保护性 NK 受体等位基因(KIR3DS1 和 KIR3DL1)的遗传。然而,导致 HIV-1 暴露未感染静脉吸毒者(EU-IDU)NK 细胞激活的确切机制仍有待阐明。

目的

我们研究了在费城的 15 名 EU-IDU 个体和 15 名对照未感染供体的高危活动期间,宿主基因型和病原体诱导的树突状细胞对 NK 激活的调节作用。

设计

我们通过流式细胞术评估 NK 细胞和树突状细胞的激活状态,并利用 NK-DC 相互作用的功能测定来描述 EU-IDU 个体的固有免疫成分。

结果

如前所述,与对照未感染供体相比,EU-IDU 个体的 NK 细胞激活(CD69)和/或脱颗粒(CD107a)明显增加(P=0.0056,n=13)。基因型分析表明,保护性 KIR(KIR3DS1)和 HLA-Bw4*80I 配体的频率在我们的 EU-IDU 个体队列中并未富集。相反,EU-IDU 个体的浆细胞样树突状细胞(PDC)与对照未感染供体相比表现出更高的成熟度(CD83)(P=0.0011,n=12)。在体外刺激时,EU-IDU 个体的 PDC 和 NK 细胞均保持强大的效应细胞功能,并且没有表现出衰竭的迹象。

结论

PDC 的成熟增加与 EU-IDU 个体中 NK 激活增加有关,这表明固有免疫成分的两个成员都可能有助于 EU-IDU 个体抵抗 HIV-1 感染。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e54e/3253656/875169a9872a/nihms229205f1.jpg

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