HIV-HCV合并感染和HCV单一感染中CD56(明亮型)自然杀伤细胞增加与其表型的独特改变有关。
Increased CD56(bright) NK cells in HIV-HCV co-infection and HCV mono-infection are associated with distinctive alterations of their phenotype.
作者信息
Bhardwaj Suvercha, Ahmad Fareed, Wedemeyer Heiner, Cornberg Marcus, Schulze Zur Wiesch Julian, van Lunzen Jan, Sarin Shiv K, Schmidt Reinhold E, Meyer-Olson Dirk
机构信息
Institute of Liver and Billiary Sciences, New Delhi, India.
Klinik für Immunologie und Rheumatologie, Medizinische Hochschule Hannover, Hannover, Germany.
出版信息
Virol J. 2016 Apr 18;13:67. doi: 10.1186/s12985-016-0507-5.
BACKGROUND
HIV-HCV co-infection is associated with accelerated progression to hepatic fibrosis, cirrhosis and hepatocellular carcinoma than HCV mono-infection. The contribution of innate immunity during HIV-HCV co-infection has been a relatively under-investigated area. Natural killer (NK) cells are pivotal sentinels of innate immunity against viruses and tumour cells. In this study we evaluated the effect of HIV-HCV co-infection on peripheral blood NK cell subsets with emphasis on the phenotype of CD56(bright) NK cells.
METHODS
Sixty patients were included in the study; HIV mono-infected (n = 12), HCV mono-infected (n = 15), HCV-HIV co-infected (n = 21) and healthy controls (n = 16). PBMCs were isolated and immunophenotyping of NK cells was performed by flowcytometry.
RESULTS
We observed an expansion of CD56(bright) NK cell subset in HIV-HCV co-infection as compared to healthy controls and HIV mono-infected group. All the infected groups had an upregulated expression of the activating receptor NKG2D on CD56(bright) NK cells in comparison to healthy controls while not differing amongst themselves. The expression of NKp46 in HIV-HCV co-infected group was significantly upregulated as compared to both HIV as well as HCV mono-infections while NKp30 expression in the HIV-HCV co-infected group significantly differed as compared to HIV mono-infection. The CD56(bright) NK cell subset was activated in HIV-HCV co-infection as assessed by the expression of CD69 as compared to healthy controls but was significantly downregulated in comparison to HIV mono-infection. CD95 expression on CD56(bright) NK cells followed the same pattern where there was an increased expression of CD95 in HIV mono-infection and HIV-HCV co-infection as compared to healthy controls. In contrast to CD69 expression, CD95 expression in HCV mono-infection was decreased when compared to HIV mono-infection and HIV-HCV co-infection. Finally, expression of CXCR3 on CD56(bright) NK cells was increased in HIV-HCV co-infection in comparison to HIV mono-infection while remaining similar to HCV mono-infection.
CONCLUSION
Thus, HIV-HCV co-infection is able to modulate the phenotype of CD56(bright) NK cell subset in a unique way such that NKp46 and CXCR3 expressions are distinct for co-infection while both mono-infections have an additive effect on CD56(bright), CD69 with CD95 expressions. HCV mono-infection has a dominant effect on NKp30 expression while NKG2D and CD127 expressions remained same in all the groups.
背景
与丙型肝炎病毒(HCV)单一感染相比,人类免疫缺陷病毒(HIV)-HCV合并感染与肝纤维化、肝硬化和肝细胞癌的进展加速相关。HIV-HCV合并感染期间固有免疫的作用一直是一个相对研究较少的领域。自然杀伤(NK)细胞是针对病毒和肿瘤细胞的固有免疫的关键哨兵。在本研究中,我们评估了HIV-HCV合并感染对外周血NK细胞亚群的影响,重点关注CD56(明亮型)NK细胞的表型。
方法
60名患者纳入本研究;HIV单一感染(n = 12)、HCV单一感染(n = 15)、HCV-HIV合并感染(n = 21)和健康对照(n = 16)。分离外周血单个核细胞(PBMC),通过流式细胞术对NK细胞进行免疫表型分析。
结果
我们观察到,与健康对照和HIV单一感染组相比,HIV-HCV合并感染组中CD56(明亮型)NK细胞亚群有所扩增。与健康对照相比,所有感染组中CD56(明亮型)NK细胞上激活受体NKG2D的表达上调,而各感染组之间无差异。与HIV单一感染以及HCV单一感染相比,HIV-HCV合并感染组中NKp46的表达显著上调,而HIV-HCV合并感染组中NKp30的表达与HIV单一感染相比有显著差异。与健康对照相比,通过CD69的表达评估,HIV-HCV合并感染组中CD56(明亮型)NK细胞亚群被激活,但与HIV单一感染相比显著下调。CD56(明亮型)NK细胞上CD95的表达遵循相同模式,与健康对照相比,HIV单一感染和HIV-HCV合并感染中CD95的表达增加。与CD69表达相反,与HIV单一感染和HIV-HCV合并感染相比,HCV单一感染中CD95的表达降低。最后,与HIV单一感染相比,HIV-HCV合并感染组中CD56(明亮型)NK细胞上CXCR3的表达增加,而与HCV单一感染组相似。
结论
因此,HIV-HCV合并感染能够以独特的方式调节CD56(明亮型)NK细胞亚群的表型,使得NKp46和CXCR3的表达在合并感染时不同,而两种单一感染对CD56(明亮型)、CD69和CD95的表达有累加效应。HCV单一感染对NKp30的表达有主导作用,而NKG2D和CD127的表达在所有组中保持相同。
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