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氯化锶-89治疗转移性前列腺癌后骨吸收生化标志物的定量分析。

Quantitation of biochemical markers of bone resorption following strontium-89-chloride therapy for metastatic prostatic carcinoma.

作者信息

Papatheofanis F J

机构信息

Department of Radiology, University of California, San Diego 92103-8758, USA.

出版信息

J Nucl Med. 1997 Aug;38(8):1175-9.

PMID:9255144
Abstract

UNLABELLED

The urinary production of pyridinium collagen cross-links, pyridinoline (PYD) and deoxypyridinoline (DPD), has been correlated to increased bone resorption in patients with neoplasms. This study investigated the production of these compounds in patients with metastatic prostate carcinoma who received palliative treatment that did and did not include 89Sr-chloride therapy.

METHODS

Urinary production of PYD and DPD was measured by high-performance liquid chromatography and natural flucrescence detection methods. The urine from several age-matched groups of patients was examined for these compounds including healthy controls (n = 20), patients with early-stage (Stage A-B) prostate carcinoma (n = 8), patients with metastatic prostate carcinoma treated with conventional analgesic and radiotherapeutic palliation (n = 20), patients with metastatic disease who underwent 89Sr-chloride therapy (n = 20) and patients with mild Paget's disease (n = 5). Patients were also monitored for urinary PYD and DPD production for a 6-mo interval after a palliative intervention.

RESULTS

Elevated PYD and DPD (p < 0.05) concentrations were measured in patients with metastatic and nonmetastatic prostate cancer and Paget's disease. The urinary production of these compounds remained unchanged for 6 mo after 89Sr-chloride therapy for symptomatic osseous metastases. However, the patients who did not undergo 89Sr-chloride therapy exhibited a two-fold increase in PYD and a four-fold increase in DPD above controls during the interval.

CONCLUSION

PYD and DPD are sensitive and specific bone resorption markers which demonstrate a slowing of bone resorption after palliative 89Sr-chloride therapy in patients with bone metastases.

摘要

未标注

吡啶啉胶原交联物、吡啶啉(PYD)和脱氧吡啶啉(DPD)的尿生成量已与肿瘤患者骨吸收增加相关。本研究调查了接受姑息治疗(包括和不包括氯化锶-89治疗)的转移性前列腺癌患者中这些化合物的生成情况。

方法

采用高效液相色谱法和自然荧光检测法测量PYD和DPD的尿生成量。检测了几个年龄匹配组患者的尿液中的这些化合物,包括健康对照者(n = 20)、早期(A - B期)前列腺癌患者(n = 8)、接受传统镇痛和放射治疗姑息治疗的转移性前列腺癌患者(n = 20)、接受氯化锶-89治疗的转移性疾病患者(n = 20)以及轻度佩吉特病患者(n = 5)。在姑息干预后,还对患者进行了为期6个月的尿PYD和DPD生成量监测。

结果

在转移性和非转移性前列腺癌患者以及佩吉特病患者中,检测到PYD和DPD浓度升高(p < 0.05)。对于有症状的骨转移患者,氯化锶-89治疗后6个月内,这些化合物的尿生成量保持不变。然而,在此期间,未接受氯化锶-89治疗的患者的PYD比对照组增加了两倍,DPD增加了四倍。

结论

PYD和DPD是敏感且特异的骨吸收标志物,表明骨转移患者接受姑息性氯化锶-89治疗后骨吸收减缓。

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