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急性酒精性肝炎中的细胞因子水平:一项序贯研究。

Cytokine levels in acute alcoholic hepatitis: a sequential study.

作者信息

Rodríguez-Rodríguez E, González-Reimers E, Santolaria-Fernández F, Milena-Abril A, Rodríguez-Moreno F, Oramas-Rodríguez J, Martínez-Riera A

机构信息

Departamento de Medicina Interna, Hospital Universitario de Canarias, Tenerife, Canary Islands, Spain.

出版信息

Drug Alcohol Depend. 1995 Jul;39(1):23-7. doi: 10.1016/0376-8716(95)01130-q.

Abstract

Chronic alcoholic liver disease is associated with several immunological alterations: depressed T-cell function, low serum gamma-interferon, and high serum tumour necrosis factor (TNF-alpha) and interleukin levels. Therefore, macrophage activity seems to be enhanced. Some cytokines, such as TNF-alpha, exert adverse effects on chronic alcoholic liver disease, so that protracted activation of macrophages with continuous TNF-alpha production may aggravate alcoholic hepatitis. Based on these facts we have sequentially determined serum levels of TNF-alpha, 1 beta interleukin (IL-1 beta), gamma-interferon and neopterin--a macrophage product--at admission, and at the end of the first, third and sixth weeks after admission, of 43 patients affected by alcoholic hepatitis, and of 20 age-matched sanitary workers as controls. Our patients showed higher levels of neopterin and lower levels of IL-1 beta and gamma-interferon than the controls; TNF-alpha levels in our patients were almost significantly higher than in controls. TNF-alpha levels at admission were higher in the patients who died (P = 0.025). TNF-alpha and neopterin levels showed no trend to normalization in patients who died, with higher levels of neopterin at first and third weeks and higher TNF-alpha and gamma-interferon levels at first week. Using logistic regression analysis, serum TNF-alpha levels at admission showed significant (P = 0.045), independent effects on mortality, as well as serum neopterin (P = 0.0026) at the first week. Thus, enhanced macrophage activity, measured by serum levels of TNF-alpha and neopterin seems to be related to a worse prognosis in alcoholic hepatitis.

摘要

慢性酒精性肝病与多种免疫改变有关

T细胞功能低下、血清γ-干扰素水平降低、血清肿瘤坏死因子(TNF-α)和白细胞介素水平升高。因此,巨噬细胞活性似乎增强。一些细胞因子,如TNF-α,对慢性酒精性肝病产生不利影响,因此巨噬细胞持续产生TNF-α的长期激活可能会加重酒精性肝炎。基于这些事实,我们连续测定了43例酒精性肝炎患者以及20名年龄匹配的卫生工作者(作为对照)入院时、入院后第一周、第三周和第六周结束时的血清TNF-α、白细胞介素1β(IL-1β)、γ-干扰素和蝶呤(一种巨噬细胞产物)水平。我们的患者蝶呤水平高于对照组,而IL-1β和γ-干扰素水平低于对照组;我们患者的TNF-α水平几乎显著高于对照组。死亡患者入院时的TNF-α水平更高(P = 0.025)。死亡患者的TNF-α和蝶呤水平没有恢复正常的趋势,在第一周和第三周蝶呤水平较高,在第一周TNF-α和γ-干扰素水平较高。使用逻辑回归分析,入院时血清TNF-α水平对死亡率有显著(P = 0.045)的独立影响,第一周时血清蝶呤水平也有显著影响(P = 0.0026)。因此,通过血清TNF-α和蝶呤水平测定的增强的巨噬细胞活性似乎与酒精性肝炎的预后较差有关。

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