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血清I型前胶原羧基末端前肽与III型前胶原氨基末端前肽的比值,对于慢性病毒性肝病中的进行性纤维化形成来说,是比每种单一前肽及IV型胶原7S结构域更好的指标。

Serum carboxy terminal propeptide of type I procollagen to amino terminal propeptide of type III procollagen ratio is a better indicator than each single propeptide and 7S domain type IV collagen for progressive fibrogenesis in chronic viral liver diseases.

作者信息

Lin D Y, Chu C M, Sheen I S, Liaw Y F

机构信息

Liver Unit, Chang Gung Memorial Hospital, Taipei, Taiwan.

出版信息

Dig Dis Sci. 1995 Jan;40(1):21-7. doi: 10.1007/BF02063936.

Abstract

Twenty chronic viral hepatitis patients, mainly with hepatitis B related with progression to liver cirrhosis were included for an assay of serum collagen markers: PICP (carboxy terminal propeptide of type I procollagen), PIIINP (amino terminal propeptide of type III procollagen), and 7S-IV (7S-domain type IV collagen). PICP is increased in 20% of chronic hepatitis patients with a mean of 190.3 ng/ml, which is not different from that of the follow-up concentration in liver cirrhosis, where 35% of cases were abnormal with a mean of 220.5 ng/ml. The serum level and percent of abnormality of PIIICP in chronic hepatitis and in liver cirrhosis are 23.5 ng/ml vs 14.8 ng/ml and 90% vs 100%, respectively (P > 0.05). PICP/PIIINP is significantly higher during liver cirrhosis (15.11 vs 10.08, P < 0.05). PICP during chronic hepatitis is not related to serum biochemical changes, while PICP during liver cirrhosis and PIIINP are correlated with hepatic enzymes. 7S-IV in chronic hepatitis and in liver cirrhosis is 14.0 ng/ml vs 10.9 ng/ml, respectively; both were positively correlated with hepatic enzymes. These results suggest that PICP/PIIINP is a better indicator of hepatic fibrogenesis than either PICP or PIIINP alone in viral hepatitis. A ratio of more than 12 is suggestive of liver cirrhosis.

摘要

纳入了20例慢性病毒性肝炎患者,主要为与进展至肝硬化相关的乙型肝炎患者,进行血清胶原标志物检测:I型前胶原羧基端前肽(PICP)、III型前胶原氨基端前肽(PIIINP)和IV型胶原7S结构域(7S-IV)。20%的慢性肝炎患者PICP升高,平均为190.3 ng/ml,这与肝硬化随访浓度无差异,肝硬化患者中35%异常,平均为220.5 ng/ml。慢性肝炎和肝硬化患者中PIIICP的血清水平及异常百分比分别为23.5 ng/ml对14.8 ng/ml和90%对100%(P>0.05)。肝硬化期间PICP/PIIINP显著更高(15.11对10.08,P<0.05)。慢性肝炎期间PICP与血清生化变化无关,而肝硬化期间PICP和PIIINP与肝酶相关。慢性肝炎和肝硬化患者中7S-IV分别为14.0 ng/ml和10.9 ng/ml;两者均与肝酶呈正相关。这些结果表明,在病毒性肝炎中,PICP/PIIINP比单独的PICP或PIIINP是更好的肝纤维化指标。比值大于12提示肝硬化。

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