Complement System Is Not Activated in Primary Biliary Cirrhosis

Marco Gardinali , Luisa Conciato , Cristina Cafaro , Andrea Crosignani , Pier Maria Battezzati , Angelo Agostoni , Mauro Podda
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引用次数: 10

Abstract

There is controversial evidence suggesting that the classical pathway of complement system is chronically activated in primary biliary cirrhosis (PBC) and that complement activation may be important in development of bile duct injury. We have reevaluated this issue by measuring by-products of complement activation such as C4a, C3a, Bb, and terminal complement complexes (SC5b-9) in plasma of 44 PBC patients with sensitive methods not previously used to detect complement activation in this disease. Age-matched healthy women and patients with chronic hepatitis of different etiology were studied as controls. We found that PBC patients have normal C4a concentrations. This finding argues strongly against chronic classical pathway activation. Although a minor increase of C3a levels was observed in a minority of PBC patients, the C3a/C3 ratio, an index used to evaluate the extent of native protein conversion, was remarkably similar in all groups. Potentially lytic terminal complement complexes were not increased. PBC patients had normal Bb plasma levels, indicating that the alternative pathway is also not activated. C3 concentration was higher in PBC patients than in healthy subjects and in chronic hepatitis patients, particularly in the early stages of the disease. C3 and C4 concentrations became lower in PBC and chronic hepatitis with the progression of the disease. The increase of C3 concentration in PBC does not reflect liver inflammation, since serum levels of C-reactive protein are normal. We found high serum C3 levels in patients with rare chronic cholestatic syndromes without superimposed infections and observed that serum C3 levels paralleled those of bilirubin in a patient with benign recurrent intrahepatic cholestasis. In conclusion, our data indicate that complement is not activated in PBC and that the increase of serum C3 levels is related to cholestasis.

原发性胆汁性肝硬化补体系统未被激活
有争议的证据表明,补体系统的经典途径在原发性胆汁性肝硬化(PBC)中被慢性激活,补体激活可能在胆管损伤的发展中起重要作用。通过测量44例PBC患者血浆中补体激活的副产物,如C4a、C3a、Bb和末端补体复合物(SC5b-9),我们重新评估了这个问题,这些方法以前没有用于检测这种疾病的补体激活。以年龄匹配的健康女性和不同病因的慢性肝炎患者为对照。我们发现PBC患者的C4a浓度正常。这一发现有力地反驳了慢性经典通路激活的观点。尽管在少数PBC患者中观察到C3a水平的轻微增加,但C3a/C3比率(用于评估天然蛋白转化程度的指标)在所有组中都非常相似。潜在的溶解末端补体复合物没有增加。PBC患者血浆Bb水平正常,表明替代途径也未被激活。PBC患者的C3浓度高于健康受试者和慢性肝炎患者,特别是在疾病的早期阶段。随着PBC和慢性肝炎的进展,C3和C4浓度降低。PBC中C3浓度升高不反映肝脏炎症,因为血清c反应蛋白水平正常。我们发现,在没有叠加感染的罕见慢性胆汁淤积综合征患者中血清C3水平较高,并观察到血清C3水平与良性复发性肝内胆汁淤积患者的胆红素水平相似。总之,我们的数据表明补体在PBC中不被激活,血清C3水平的升高与胆汁淤积有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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