血清I型胶原n端前肽与乳腺癌和前列腺癌骨转移数量及其他骨相关标志物相关

Biomarkers in cancer Pub Date : 2011-03-03 eCollection Date: 2011-01-01 DOI:10.4137/BIC.S6484
D J Leeming, M Koizumi, P Qvist, V Barkholt, C Zhang, K Henriksen, I Byrjalsen, M A Karsdal
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引用次数: 25

摘要

背景:许多生物标志物已被证明具有潜在的指示癌症患者骨转移(BM)的能力。本研究的目的是研究新开发的I型胶原蛋白n端前肽(PINP)人血清检测癌症患者BM的相对效用。该试验具有相应的大鼠PINP试验,未来可能有助于啮齿动物和人类试验之间的转化科学。方法:研究对象为161例前列腺癌、肺癌和乳腺癌患者,按BM数量(Soloway评分)分层。评估PINP并与BM数量相关。此外,PINP标记物与年轻骨(ALPHA CTX-I)和老年骨(BETA CTX-I)的骨吸收相关;破骨细胞数量(抗酒石酸酸性磷酸酶5b, TRACP5B)和破骨细胞活性(CTX-I/ TRACP5B)。结果:与-BM相比,乳腺癌和前列腺癌+BM患者的PINP显著升高(P < 0.001),但肺癌患者的PINP无显著升高。PINP与脑转移灶数量呈明显的线性关系。在Soloway评分1-4时,观察到PINP显著升高(结论:数据表明,目前的PINP可能确定乳腺癌或前列腺癌患者的骨骼受累情况。相关性表明,在乳腺癌和前列腺癌患者中,骨吸收和骨形成之间的耦合仍然存在。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Serum N-Terminal Propeptide of Collagen Type I is Associated with the Number of Bone Metastases in Breast and Prostate Cancer and Correlates to Other Bone Related Markers.

Serum N-Terminal Propeptide of Collagen Type I is Associated with the Number of Bone Metastases in Breast and Prostate Cancer and Correlates to Other Bone Related Markers.

Serum N-Terminal Propeptide of Collagen Type I is Associated with the Number of Bone Metastases in Breast and Prostate Cancer and Correlates to Other Bone Related Markers.

Serum N-Terminal Propeptide of Collagen Type I is Associated with the Number of Bone Metastases in Breast and Prostate Cancer and Correlates to Other Bone Related Markers.

Background: A number of biomarkers have been proven potentially useful for their ability to indicate bone metastases (BM) in cancer patients. The aim of this study was to investigate the relative utility of a newly developed N-terminal propeptide of collagen type I (PINP) human serum assay for the detection of BM in cancer patients. This assay has a corresponding rat PINP assay which in the future might help in translational science between rodent and human trials.

Methods: Participants were 161 prostate, lung and breast cancer patients stratified by number of BM (Soloway score). PINP was assessed and correlated to number of BM. Additionally, the PINP marker was correlated to bone resorption of young (ALPHA CTX-I)- and aged bone (BETA CTX-I); number of osteoclasts (Tartrate-resistant acid phosphatase 5b, TRACP5B) and osteoclast activity (CTX-I/ TRACP5B).

Results: PINP was significantly elevated in breast- and prostate cancer patients +BM, compared to -BM (P < 0.001), however not in lung cancer patients. A strong linear association was seen between PINP and the number of BMs. Significant elevation of PINP was observed at Soloway scores 1-4 (<0 BM) compared with score 0 (0 BM) (P < 0.001). The correlation between bone resorption of young bone or aged bone and bone formation was highly significant in patients +BM and -BM (P < 0.0001).

Conclusions: Data suggest that the present PINP potentially could determine skeletal involvement in patients with breast or prostate cancer. Correlations suggested that coupling between bone resorption and bone formation was maintained in breast- and prostate cancer patients.

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