首页> 外文期刊>Calcified tissue international. >Serum CTX: a new marker of bone resorption that shows treatment effect more often than other markers because of low coefficient of variability and large changes with bisphosphonate therapy.
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Serum CTX: a new marker of bone resorption that shows treatment effect more often than other markers because of low coefficient of variability and large changes with bisphosphonate therapy.

机译:血清CTX:一种新的骨吸收标记物,由于变异系数低且双膦酸盐治疗变化大,因此比其他标记物更能显示治疗效果。

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Serum CrossLaps is a new assay for measuring carboxy-terminal collagen crosslinks (CTX) in serum. This measurement is reported to be more specific to bone resorption than other measurements. However, the utility of this and other markers in monitoring patients on antiresorptive therapy depends on how often changes anticipated with therapy exceed changes attributable to random variability. In a study where subjects received either placebo or pamidronate, we calculated the minimum significant change (MSC), that is, the change that was sufficiently large that it was unlikely to be due to spontaneous variability. We also examined the changes in markers of bone turnover in subjects treated with pamidronate (APD) (30 mg i.v. in 500 ml D5W over 4 hours) to see how often observed changes in turnover after treatment exceeded the MSC. The MSC for serum CTX was 30.2%, and was significantly (P < 0.05) lower than the MSC for urinary NTX (54.0%), and not significantly different from the MSC of urinary DPD (20.6%). Ninety percent of subjects treated with APD had a decline in serum CTX that exceeded the MSC, compared with 74% for bone-specific alkaline phophatase (BSAP), 57% for urinary N-telopeptide cross-links (NTX), and 48% for free deoxypyridinoline. Changes in serum CTX correlated reasonably well with changes in spine BMD after 2 years (r = 0.47), but this correlation did not quite reach statistical significance because of the small number of subjects. In conclusion, the serum CTX assay shows greater utility for assessing efficacy of antiresorptive treatment than some previously described markers.
机译:血清CrossLaps是一种新的测定血清中羧基末端胶原蛋白交联(CTX)的方法。据报道,该测量比其他测量对骨吸收更具特异性。但是,此标记和其他标记在监视患者接受抗吸收治疗方面的实用性取决于治疗预期的变化超过可归因于随机变异性的变化的频率。在一项研究中,受试者接受安慰剂或帕米膦酸盐治疗,我们计算了最小显着变化(MSC),即该变化足够大,以至于不太可能是由于自发变异引起的。我们还检查了用帕米膦酸(APD)(30 mg静脉内在500 ml D5W中历时4小时)进行治疗的受试者的骨转换标志物的变化,以观察治疗后观察到的转换率超过MSC的频率。血清CTX的MSC为30.2%,显着低于PNT(54.0%),与尿DPD的MSC(20.6%)无显着差异。 APD治疗的受试者中有90%的血清CTX下降超过了MSC,而骨特异性碱性磷酸酶(BSAP)下降了74%,尿N-端肽交联(NTX)下降了57%,而骨特异性碱性磷酸酶(NTX)下降了48%游离脱氧吡啶啉。血清CTX的变化与2年后脊柱BMD的变化有很好的相关性(r = 0.47),但是由于受试者人数少,这种相关性还没有达到统计学意义。总之,与某些先前描述的标记物相比,血清CTX测定法在评估抗吸收治疗的功效方面显示出更大的实用性。

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