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Seromarkers of collagen I and III metabolism in active Crohns disease. Relation to disease activity and response to therapy.

机译:活动性克罗恩病中胶原蛋白I和III代谢的血清标志物。与疾病活动和治疗反应的关系。

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摘要

Crohn's disease is characterised by gradual development of intestinal fibrotic lesions containing large amounts of collagen type I, III, and V. Measurement of circulating connective tissue metabolites has emerged as a useful tool for assessment of fibroproliferative activity in various diseases. Serum concentrations of procollagen peptides, N-terminal propeptide of type III procollagen (PII-INP), and C-terminal propeptide of type I procollagen (PICP), reflect the synthesis rate of the parent collagens, while the C-terminal telopeptide of type I collagen (ICTP) reflects its degradation. S-PIIINP, S-PICP, and S-ICTP were measured by radioimmunoassays in 29 patients with active Crohn's disease. S-ICTP was significantly increased, median 6.2 micrograms/l (95% CI 5.2 to 8.7 micrograms/l) versus controls 2.6 micrograms/l (2.5 to 2.7 micrograms/l) (p < 0.0001), S-PICP reduced, 100 micrograms/l (80 to 110 micrograms/l) versus 132 micrograms/l (124 to 141 micrograms/l) (p = 0.001), and S-PIIINP did not differ from controls. Patients with sustained clinical remission during prednisolone therapy exhibited an increase in S-PICP (p = 0.0052). S-PIIINP changed significantly (p = 0.0002), however, exhibiting a biphasic pattern. S-ICTP decreased (p = 0.015) in treatment responders but remained above the upper normal limit even when clinical remission had been achieved. Non-responders showed no significant changes in any of the marker molecules of collagen synthesis or degradation. Correlations were found between S-PIIINP and S-PICP (p < 0.005) and S-ICTP (p < 0.02), and between S-ICTP and S-orosomucoid (p < 0.005) and S-C reactive protein (p < 0.02). By contrast, there was no relation between the connective tissue metabolites and Harvey Bradshaw Index. These data provide evidence that collagen I degradation is increased not only in active Crohn's disease, but also in patients entering clinical remission. The concurrent normal/low-normal values of markers of collagen formation may reflect a changed local or systemic elimination of the propeptides.
机译:克罗恩病的特征是逐渐发展为包含大量I,III和V型胶原的肠纤维化病变。循环结缔组织代谢产物的测量已成为评估各种疾病中纤维增殖活性的有用工具。前胶原蛋白肽,III型胶原蛋白的N末端前肽(PII-INP)和I型胶原蛋白的C末端前肽(PICP)的血清浓度反映了母体胶原蛋白的合成速率,而C型胶原蛋白的终末浓度I胶原蛋白(ICTP)反映了其降解。 S-PIIINP,S-PICP和S-ICTP通过放射免疫分析法对29例活动性克罗恩病患者进行了测量。 S-ICTP显着增加,中位数为6.2微克/升(95%CI 5.2至8.7微克/升),而对照为2.6微克/升(2.5至2.7微克/升)(p <0.0001),S-PICP降低了100微克/ l(80至110微克/ l)与132微克/ l(124至141微克/ l)(p = 0.001),S-PIIINP与对照无差异。泼尼松龙治疗期间持续临床缓解的患者表现出S-PICP升高(p = 0.0052)。 S-PIIINP发生了显着变化(p = 0.0002),但是显示出双相模式。治疗反应者的S-ICTP降低(p = 0.015),但即使达到临床缓解,仍保持在正常上限之上。无反应者在胶原合成或降解的任何标记分子中均无明显变化。发现在S-PIIINP和S-PICP(p <0.005)和S-ICTP(p <0.02)之间,以及在S-ICTP和S-类蛋黄素(p <0.005)与S-C反应蛋白之间(p <0.02)之间存在相关性。相比之下,结缔组织代谢产物与Harvey Bradshaw指数之间没有关系。这些数据提供了证据,不仅在活跃的克罗恩病中,而且在进入临床缓解的患者中,胶原蛋白I的降解都有所增加。胶原蛋白形成标记的同时正常/低正常值可以反映前肽的局部或全身消除的变化。

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