CD4 IL-21 T细胞与调节性T细胞相关,并且在HIV感染期间IL-21可促进调节性T细胞的存活。
CD4IL-21T cells are correlated with regulatory T cells and IL-21 promotes regulatory T cells survival during HIV infection.
作者信息
Zhang Zi-Ning, Bai Li-Xin, Fu Ya-Jing, Jiang Yong-Jun, Shang Hong
机构信息
Key Laboratory of AIDS Immunology of National Health and Family Planning Commission, Department of Laboratory Medicine, The First Affiliated Hospital, China Medical University, Shenyang, Liaoning 110001, China; Collaborative Innovation Center for Diagnosis and Treatment of Infectious Diseases, Hangzhou, Zhejiang, China.
Key Laboratory of AIDS Immunology of National Health and Family Planning Commission, Department of Laboratory Medicine, The First Affiliated Hospital, China Medical University, Shenyang, Liaoning 110001, China.
出版信息
Cytokine. 2017 Mar;91:110-117. doi: 10.1016/j.cyto.2016.12.012. Epub 2016 Dec 31.
INTRODUCTION
IL-21 enhances T and natural killer cells survival and antiviral functions without promoting T cell activation during HIV infection, which makes it a better adjuvant in anti-HIV immunotherapy. Due to the pleiotropy and redundancy of cytokines, it is vital to have a comprehensive knowledge of the role of IL-21 in the regulation of immune responses. Regulatory T cells (Tregs) play an important role in immune regulation and are a determinant of immune therapeutic efficacy in certain circumstances. In this study, we explored the direct effect of IL-21 on Tregs during HIV infection, which has not been addressed before.
METHODS
Thirty-four HIV treatment-naïve patients were enrolled and the relationship between CD4IL-21T cells and Tregs were studied. The effects of IL-21 on CD4CD25CD127 Tregs' apoptosis, proliferation, and CTLA-4 and TGF-β expression in HIV-infected patients was investigated and compared with the effect of other common γ-chain cytokines.
RESULTS
We found the percentage and absolute numbers of CD4IL-21T cells were positively related to the frequency or absolute numbers of CD4CD25 or CD4CD25CD127 Tregs. Compared with the media-alone control, IL-21, IL-7, and IL-15 could significantly reduce apoptosis of Tregs (p<0.05). IL-21 did not promote the proliferation of Tregs as compared with media alone, while IL-2, IL-7, and IL-15 could significantly increase the proliferation of Tregs (p<0.05). IL-21 enhanced CTLA-4 expression by Tregs (p<0.05), but could not induce TGF-β secretion of Tregs from HIV infected patients. There were no significant differences of the fold induction of apoptosis, proliferation, or CTLA-4 and TGF-β expression by Tregs from HIV-infected patients and normal controls after IL-21 treatment. In vitro experiment showed that pretreatment with IL-21 significantly enhanced the suppressive effect of Tregs on CD8+ T cells' IFN-γ expression.
CONCLUSION
We conclude that IL-21 promotes the survival and CTLA-4 expression of Tregs and enhanced the suppressive capacity of Tregs during HIV infection. These results broaden the understanding of HIV pathogenesis and provide critical information for HIV interventions.
引言
白细胞介素-21(IL-21)可增强T细胞和自然杀伤细胞的存活及抗病毒功能,且在HIV感染期间不会促进T细胞活化,这使其成为抗HIV免疫治疗中更好的佐剂。由于细胞因子具有多效性和冗余性,全面了解IL-21在免疫反应调节中的作用至关重要。调节性T细胞(Tregs)在免疫调节中起重要作用,在某些情况下是免疫治疗效果的决定因素。在本研究中,我们探讨了HIV感染期间IL-21对Tregs的直接影响,此前尚未有相关研究。
方法
招募34例未接受过HIV治疗的患者,研究CD4IL-21T细胞与Tregs之间的关系。研究IL-21对HIV感染患者CD4CD25CD127 Tregs凋亡、增殖以及CTLA-4和TGF-β表达的影响,并与其他常见γ链细胞因子的作用进行比较。
结果
我们发现CD4IL-21T细胞的百分比和绝对数量与CD4CD25或CD4CD25CD127 Tregs的频率或绝对数量呈正相关。与单独使用培养基的对照组相比,IL-21、IL-7和IL-15可显著降低Tregs的凋亡(p<0.05)。与单独使用培养基相比,IL-21未促进Tregs的增殖,而IL-2、IL-7和IL-15可显著增加Tregs的增殖(p<0.05)。IL-21可增强Tregs的CTLA-4表达(p<0.05),但不能诱导HIV感染患者Tregs分泌TGF-β。IL-21处理后,HIV感染患者和正常对照的Tregs在凋亡、增殖或CTLA-4和TGF-β表达的诱导倍数方面无显著差异。体外实验表明,IL-21预处理可显著增强Tregs对CD8+ T细胞IFN-γ表达的抑制作用。
结论
我们得出结论,IL-21在HIV感染期间促进Tregs的存活和CTLA-4表达,并增强Tregs的抑制能力。这些结果拓宽了对HIV发病机制的理解,并为HIV干预提供了关键信息。
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