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Markers of type I collagen degradation and synthesis in the monitoring of treatment response in bone metastases from breast carcinoma

机译:I型胶原蛋白降解和合成的标志物监测乳腺癌骨转移的治疗反应

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Thirty-six patients with bone metastases included in a trial of supportive calcitonin on the treatment response to systemic therapy were monitored by conventional radiography, conventional indicators of bone metabolism [alkaline phosphatase (AP), osteocalcin (gla), urinary hydroxyproline excretion (OHP), urinary calcium (uCa), serum calcium (sCa)] and collagen metabolites (ICTP, the pyridinoline cross-linked carboxy-terminal telopeptide of type I collagen; PICP, the carboxy-terminal propeptide of type I procollagen; and PIIINP the amino-terminal propeptide of type III procollagen). All patients had been on the same systemic treatment for at least 3 months at the start of the trial. There was a positive correlation between the concentrations of ICTP and PICP at baseline (Spearman's rank-order correlation coefficient rs = 0.62). Both ICTP and PICP showed statistically significant correlations to the other markers of bone metabolism (except sCa and uCa) as well as to the number of bone metastases on bone scans. Reduction in ICTP correlated significantly with the treatment response at three months (rs = - 0.57). while PICP showed a borderline negative correlation to therapy response (rs = - 0.37). Of all the biochemical parameters studied the changes in ICTP showed the best correlation with the treatment response. PICP and ICTP changes in patients with progressive disease differed significantly from those in patients with responding and stable metastases, whereas no difference was found between responders and stable patients.
机译:通过常规放射照相,常规骨代谢指标[碱性磷酸酶(AP),骨钙蛋白(gla),尿羟脯氨酸排泄(OHP)]监测支持降钙素对全身治疗反应的试验中纳入的36例骨转移患者。 ,尿钙(uCa),血清钙(sCa)]和胶原代谢产物(ICTP,吡啶啉I型胶原的羧基末端端肽; PICP,I型胶原原的羧基末端前肽; PIIINP,氨基III型胶原原末端肽)。在试验开始时,所有患者均接受了相同的全身治疗至少3个月。基线时ICTP和PICP的浓度之间呈正相关(Spearman等级相关系数rs = 0.62)。 ICTP和PICP均显示与骨代谢的其他标志物(sCa和uCa除外)以及与骨扫描的骨转移数在统计学上显着相关。 ICTP降低与三个月的治疗反应显着相关(rs =-0.57)。而PICP与治疗反应之间呈临界负相关(rs =-0.37)。在所有研究的生化参数中,ICTP的变化显示出与治疗反应的最佳相关性。进展性疾病患者的PICP和ICTP变化与有反应和稳定转移的患者相比有显着差异,而有反应者和稳定患者之间没有发现差异。

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