Santos Silvane B, Porto Aurélia F, Muniz André Luiz, Luna Tania, Nascimento Márcia C, Guerreiro Jaqueline B, Oliveira-Filho Jamary, Morgan Daniel J, Carvalho Edgar M
Serviço de Imunologia, Hospital Universitário Professor Edgard Santos, Salvador, Brazil.
Neuroimmunomodulation. 2006;13(3):145-51. doi: 10.1159/000097259. Epub 2006 Nov 21.
Human T lymphotropic virus-type 1 (HTLV-1) activates the immune system leading to a persistent and exacerbated T-cell response with increased production of IFN-gamma and TNF-alpha. Overproduction of pro-inflammatory cytokines is correlated with the development of HTLV-1-associated myelopathy/tropical spastic paraparesis (HAM/TSP), although some HTLV-1 carriers also show high levels of these cytokines. In this study, the ability of regulatory cytokines and cytokine antagonists to inhibit spontaneous IFN-gamma production was investigated.
IFN-gamma levels were measured by ELISA before and after addition of cytokines or anti-cytokines.
Addition of IL-10 significantly reduced spontaneous IFN-gamma synthesis in cell cultures from HTLV-1 carriers, while no differences were observed in HAM/TSP patients. There was also a tendency to decreased IFN-gamma levels in cell cultures from HTLV-1 carriers with exogenous addition of TGF-beta. In paired analysis, neutralization of IL-2 significantly decreased IFN-gamma production in HTLV-1 carriers but not in HAM/TSP patients. Neutralization of IL-15 was less effective than neutralization of IL-2 in modulating IFN-gamma production. In HTLV-1 carriers, anti-IL-2 and simultaneous addition of anti-IL-2 and anti-IL-15 decreased IFN-gamma synthesis by 46 and 64%, respectively, whereas in patients with HAM/TSP simultaneous neutralization of both anti-cytokines only decrease IFN-gamma levels by 27%.
Although a large proportion of HTLV-1 carriers produced high levels of pro-inflammatory cytokines similar to those observed in HAM/TSP patients, immune response can be downregulated by cytokines or cytokine antagonists in most HTLV-1 carriers. This modulation can be an important step in the prevention of tissue damage and progression from the HTLV-1 carrier state to HAM/TSP.
1型人类嗜T淋巴细胞病毒(HTLV-1)激活免疫系统,导致持续性且加剧的T细胞反应,伴随γ干扰素(IFN-γ)和肿瘤坏死因子-α(TNF-α)产生增加。促炎细胞因子的过量产生与HTLV-1相关脊髓病/热带痉挛性截瘫(HAM/TSP)的发展相关,尽管一些HTLV-1携带者也表现出这些细胞因子的高水平。在本研究中,研究了调节性细胞因子和细胞因子拮抗剂抑制自发性IFN-γ产生的能力。
在添加细胞因子或抗细胞因子之前和之后,通过酶联免疫吸附测定(ELISA)测量IFN-γ水平。
添加白细胞介素-10(IL-10)显著降低了HTLV-1携带者细胞培养物中的自发性IFN-γ合成,而在HAM/TSP患者中未观察到差异。在外源性添加转化生长因子-β(TGF-β)的情况下,HTLV-1携带者的细胞培养物中IFN-γ水平也有降低的趋势。在配对分析中,中和IL-2显著降低了HTLV-1携带者中的IFN-γ产生,但在HAM/TSP患者中未降低。中和IL-15在调节IFN-γ产生方面不如中和IL-2有效。在HTLV-1携带者中,抗IL-2以及同时添加抗IL-2和抗IL-15分别使IFN-γ合成降低了46%和64%,而在HAM/TSP患者中,同时中和两种抗细胞因子仅使IFN-γ水平降低了27%。
尽管很大一部分HTLV-1携带者产生的促炎细胞因子水平与HAM/TSP患者中观察到的相似,但在大多数HTLV-1携带者中,细胞因子或细胞因子拮抗剂可下调免疫反应。这种调节可能是预防组织损伤以及从HTLV-1携带者状态进展为HAM/TSP的重要步骤。
