首页> 外文OA文献 >Radioimmunoassay for the carboxy-terminal cross-linking domain of type IV (basement membrane) procollagen in body fluids. Characterization and application to collagen type IV metabolism in fibrotic liver disease.
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Radioimmunoassay for the carboxy-terminal cross-linking domain of type IV (basement membrane) procollagen in body fluids. Characterization and application to collagen type IV metabolism in fibrotic liver disease.

机译:体液中IV型(基底膜)原胶原的羧基末端交联结构域的放射免疫分析。表征和在纤维化肝病中应用于IV型胶原代谢。

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摘要

The carboxy-terminal cross-linking domain (NCl) of type IV procollagen was isolated from human placenta and used for the production of polyclonal and monoclonal antibodies. Purity of the antigen and specificity of the antibodies were verified by Western blotting and radioimmunoassays. A radioimmunoassay was developed using rabbit antiserum. Intra- and interassay coefficients of variation were 4.7% and 5.8%, respectively; recovery of NCl added to serum and bile was 95-105%. NCl concentration in sera of healthy volunteers was 6 +/- 2.9 ng/ml (mean +/- 2.5 SD) and was elevated up to 18 ng in sera of patients with autoimmune or metastatic tumor disease and up to 240 ng in sera of patients with fibrogenic liver disease. Substantial amounts of antigen were also found in bile, urine, and ascites. 67% of serum antigens eluted from an agarose A5M column with an apparent molecular weight of 60 kD and 23% with a molecular weight of 90 and 150 kD, well below the molecular weight of type IV procollagen (550 kD). Serum NCl is apparently derived from the degradation of basement membrane collagen. The time course of NCl concentrations in sera of patients with fibrogenic liver disease showed no correlation with the serum concentration of the amino-terminal procollagen type III peptide, a marker of hepatic collagen biosynthesis. A decline of serum NCl levels along with elevated serum procollagen type III peptides apparently indicates bad prognosis in fibrogenic liver disease. The radioimmunoassay for NCl is a useful tool for studying type IV collagen metabolism in conditions causing remodeling or breakdown of basement membranes.
机译:从人胎盘中分离出IV型胶原蛋白的羧基末端交联结构域(NC1),并将其用于生产多克隆和单克隆抗体。抗原的纯度和抗体的特异性通过蛋白质印迹法和放射免疫法进行了验证。使用兔抗血清开发了放射免疫测定法。批内和批间变异系数分别为4.7%和5.8%;加入血清和胆汁的NCl回收率为95-105%。健康志愿者血清中的NCI浓度为6 +/- 2.9 ng / ml(平均+/- 2.5 SD),自身免疫性或转移性肿瘤疾病患者的血清中NCI浓度升高至18 ng,患者血清中的NCI浓度升高至240 ng患有纤维化性肝病。在胆汁,尿液和腹水中也发现了大量抗原。 67%的血清抗原从琼脂糖A5M柱洗脱,表观分子量为60 kD,23%的分子量为90和150 kD,远低于IV型胶原蛋白的分子量(550 kD)。血清NCl显然源自基底膜胶原蛋白的降解。纤维化性肝病患者血清中NCl的浓度随时间的变化与肝脏胶原生物合成的标志物III型氨基末端胶原蛋白的血清浓度无关。血清NCI水平的降低以及血清III型胶原原胶原的升高显然表明了纤维化性肝病的不良预后。 NCl的放射免疫分析法是研究引起基底膜重塑或分解的条件下IV型胶原代谢的有用工具。

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