骨重建标志物在单克隆伽玛病的治疗中是有用的。

José M Hernández, Begoña Suquía, José A Queizan, Rosa M Fisac, José J Sanchez, Francisco J Fernández-Calvo, Ramón García-Sanz, Carmen Olivier, Abelardo Bárez, María J Calmuntia, Javier García-Frade, Juan A Portero, Rosa López, Carmen Aguilera, Jose A Navajo, Jesús F San-Miguel
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引用次数: 14

摘要

常规放射学对多发性骨髓瘤(MM)骨病的评价重复性低。在过去的十年中,一些血清和尿液生化参数,用于评估骨转换,已经成为可用的。本研究旨在探讨六种骨重建标志物的价值。对176例新诊断的单克隆伽玛病(107例MM和69例意义不明的单克隆伽玛病(MGUS))患者进行了研究。我们选取25例良性骨质疏松症患者(BO)和32例健康人(HI)作为对照组。分析的骨标志物包括:骨吸收标志物(BRM)(总吡啶啉、总脱氧吡啶啉、游离脱氧吡啶啉和I型胶原c端末端肽)和骨形成标志物(BFM)(骨碱性磷酸酶(bAP)和骨钙素(OC))。MM患者血清或尿中BRM水平显著高于MGUS患者、BO患者和HI患者(P < 0.001)。有溶解性病变的MM患者BRM较高。然而,只有c端端肽能够区分无骨病变的MM患者和MGUS患者。在上述比较中,BFM没有显示出显著差异,尽管观察到早期骨矫形患者的OC值较高,bAP值较低。含bAP的BRM/BFM的比值在MM组和其他实体之间以及不同MM亚组之间表现出最显著的差异。事实上,BRM/bAP比值在未裂解的MM亚组和MGUS组之间具有区别(P < 0.01)。BRM和BFM,尤其是比值,在单克隆伽玛病患者的骨病变评估中是有用的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Bone remodelation markers are useful in the management of monoclonal gammopathies.

The evaluation of bone disease in multiple myeloma (MM) by conventional radiology has low reproducibility. In the last decade, several serum and urine biochemical parameters, for evaluation of bone turnover, have become available. The present study was designed to explore the value of six bone remodelation markers. It was studied in a series of 176 newly diagnosed patients with monoclonal gammopathies (107 MM and 69 monoclonal gammopathies of unknown significance (MGUS)). As control groups we used 25 patients with benign osteoporosis (BO) and 32 healthy individuals (HI). The bone markers analyzed included: bone resorption markers (BRM) (total pyridinoline, total deoxypyridinoline, free deoxypyridinoline and C-terminal telopeptide of collagen I) and bone formation markers (BFM) (bone alkaline phosphatase (bAP) and osteocalcin (OC)). Serum or urinary levels of BRM were significantly higher in MM patients than in MGUS patients, BO patients or HI (P < 0.001, respectively). BRM were higher in MM patients with lytic lesions. However, only C-terminal telopeptide discriminated MM patients without bone lesions from MGUS patients. BFM did not show significant differences in the aforementioned comparisons, although a trend toward higher values of OC and lower values of bAP in patients with early bone affectation was observed. Ratios BRM/BFM that contained bAP exhibited differences that were most significant between the MM group and other entities, as well as between the different MM subgroups. In fact, the ratios BRM/bAP provided discrimination between the MM subgroup without lyses and MGUS group (P < 0.01). BRM and BFM, especially the ratios, are useful in the evaluation of bone lesions in patients with monoclonal gammopathies.

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