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同种异体抗原刺激的CD8 + T细胞抑制NF-κB和Ets-1 DNA结合活性,并抑制CD4 + T细胞中磷酸化的NF-κB p65核定位。

Allo-antigen stimulated CD8+ T-cells suppress NF-κB and Ets-1 DNA binding activity, and inhibit phosphorylated NF-κB p65 nuclear localization in CD4+ T-cells.

作者信息

Nagashima Ryuichi, Kawakami Fumitaka, Takahashi Shinichiro, Obata Fumiya, Kubo Makoto

机构信息

1 Division of Clinical Immunology, Graduate School of Medical Sciences, Kitasato University , Sagamihara, Japan .

出版信息

Viral Immunol. 2014 Aug;27(6):305-15. doi: 10.1089/vim.2013.0113. Epub 2014 May 20.

DOI:10.1089/vim.2013.0113
PMID:24844121
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4076998/
Abstract

CD8+ T-cells of asymptomatic HIV-1 carriers (AC) suppress human immunodeficiency virus type 1 (HIV-1) replication in a class I major histocompatibility complex (MHC-I)-restricted and -unrestricted manner. In order to investigate the mechanism of MHC-I-unrestricted CD8+ T-cell-mediated HIV-1 suppression, we previously established allo-antigen stimulated CD8+T-cells from HIV-1-uninfected donors. These allo-antigen stimulated CD8+ T-cells suppressed HIV-1 replication in acutely infected autologous CD4+ T-cells when directly co-cultured. To elucidate the mechanism of HIV-1 replication suppression, we analyzed DNA-binding activity and phosphorylation of transcriptional factors associated with HIV-1 replication by electrophoresis mobility shift assay and Western blotting. When CD4+ T-cells were cultured with allo-antigen stimulated CD8+ T-cells, the reduction of NF-κB and Ets-1 DNA-binding activity was observed. Nuclear localization of NF-κB p65 and Ets-1 was suppressed in CD4+ T-cells. Although NF-κB p65 and Ets-1 are known to be regulated by protein kinase A (PKA), no difference was observed in the expression and phosphorylation of the PKA catalytic subunit in CD4+ T-cells cultured with PHA-treated CD8+ T-cells or allo-antigen stimulated CD8+ T-cells. Cyclic AMP is also known to enter through gap junctions, but the suppression of HIV-1 replication mediated by allo-antigen stimulated CD8+ T-cells was not affected by the gap junction inhibitor. The nuclear transport of phosphorylated NF-κB p65 (Ser276) was inhibited only in CD4+ T-cells cultured with allo-antigen stimulated CD8+ T-cells. Our results indicate that allo-antigen stimulated CD8+ T-cells suppress the transcriptional activity of NF-κB p65 or Ets-1 in an antigen-nonspecific manner, and inhibit the nuclear transport of phosphorylated NF-κB p65 (Ser276).

摘要

无症状HIV-1携带者(AC)的CD8 + T细胞以I类主要组织相容性复合体(MHC-I)限制性和非限制性方式抑制1型人类免疫缺陷病毒(HIV-1)复制。为了研究MHC-I非限制性CD8 + T细胞介导的HIV-1抑制机制,我们之前从未感染HIV-1的供体中建立了同种异体抗原刺激的CD8 + T细胞。这些同种异体抗原刺激的CD8 + T细胞在直接共培养时可抑制急性感染的自体CD4 + T细胞中的HIV-1复制。为了阐明HIV-1复制抑制机制,我们通过电泳迁移率变动分析和蛋白质印迹分析了与HIV-1复制相关的转录因子的DNA结合活性和磷酸化情况。当CD4 + T细胞与同种异体抗原刺激的CD8 + T细胞共培养时,观察到NF-κB和Ets-1 DNA结合活性降低。CD4 + T细胞中NF-κB p65和Ets-1的核定位受到抑制。虽然已知NF-κB p65和Ets-1受蛋白激酶A(PKA)调节,但在用PHA处理的CD8 + T细胞或同种异体抗原刺激的CD8 + T细胞培养的CD4 + T细胞中,PKA催化亚基的表达和磷酸化没有差异。环磷酸腺苷也已知通过间隙连接进入,但同种异体抗原刺激的CD8 + T细胞介导的HIV-1复制抑制不受间隙连接抑制剂的影响。仅在用同种异体抗原刺激的CD8 + T细胞培养的CD4 + T细胞中,磷酸化的NF-κB p65(Ser276)的核转运受到抑制。我们的结果表明,同种异体抗原刺激的CD8 + T细胞以抗原非特异性方式抑制NF-κB p65或Ets-1的转录活性,并抑制磷酸化的NF-κB p65(Ser276)的核转运。

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