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接受阿法骨化醇治疗的血液透析患者血浆骨特异性碱性磷酸酶的变化

Plasma bone-specific alkaline phosphatase changes in hemodialysis patients treated by alfacalcidol.

作者信息

Ureña P, Bernard-Poenaru O, Cohen-Solal M, de Vernejoul M C

机构信息

Service de Néphrologie-Dialyse, Clinique de l'Orangerie, Aubervilliers, France.

出版信息

Clin Nephrol. 2002 Apr;57(4):261-73. doi: 10.5414/cnp57261.

Abstract

Vitamin D derivatives correct high bone remodeling by decreasing plasma iPTH concentration in uremic patients with secondary hyperparathyroidism. However, without bone biopsy, plasma iPTH alone might not provide sufficient information regarding vitamin D-induced bone changes. Plasma bone-specific alkaline phosphatase (bAP) seems more sensitive than iPTH in assessing the degree of bone remodeling. We prospectively studied the evolution of iPTH and bAP in 14 adult hemodialysis patients treated for 1 year by i.v. alfacalcidol pulses. The mean total alfacalcidol dose was 0.08 +/- 0.02 g/kg/week. Ten patients completed the study, 2 patients had to be parathyroidectomized before week 24 because of hypercalcemia and uncontrolled hyperphosphatemia, and 2 other patients died before week 36. Mean iPTH levels diminished from 826 +/- 300 pg/ml (range 507 - 1,500 pg/ml) at baseline to 436 +/- 371 pg/ml (range 18 - 1,095 pg/ml) after 52 weeks of treatment (48% of decrease). Only 2 patients normalized plasma iPTH levels while 8/10 normalized bAP. Five patients remained with plasma iPTH concentrations higher than 5-fold the normal value. In contrast, plasma bAP levels declined from 47.6 +/- 32.2 ng/ml (range 15.4 - 130.0 ng/ml) at baseline to 17.8 +/- 9.9 ng/ml (range 8.0 +/- 38.0 ng/ml) at week 52 (63% of decrease). Bone histomorphometry was available in 6 patients after 15.8 +/- 5.1 months of alfacalcidol treatment. None of them met the criteria of adynamic bone disease as they had increased bone resorption and marrow bone fibrosis. Bone formation rate was normal in 2 patients and unmeasurable in the other 4. Two patients showed signs of osteomalacia. In conclusion, alfacalcidol preferentially reduced bone formation rate rather than the other histological parameters of secondary hyperparathyroidism. It reduced plasma bAP more efficiently than iPTH.

摘要

维生素D衍生物可通过降低继发性甲状旁腺功能亢进的尿毒症患者的血浆全段甲状旁腺激素(iPTH)浓度来纠正高骨转换。然而,在未进行骨活检的情况下,仅血浆iPTH可能无法提供足够的关于维生素D诱导的骨变化的信息。血浆骨特异性碱性磷酸酶(bAP)在评估骨转换程度方面似乎比iPTH更敏感。我们前瞻性地研究了14例接受静脉注射阿法骨化醇脉冲治疗1年的成年血液透析患者的iPTH和bAP的变化。阿法骨化醇的平均总剂量为0.08±0.02μg/kg/周。10例患者完成了研究,2例患者因高钙血症和无法控制的高磷血症在第24周前接受了甲状旁腺切除术,另外2例患者在第36周前死亡。治疗52周后,平均iPTH水平从基线时的826±300pg/ml(范围507 - 1500pg/ml)降至436±371pg/ml(范围18 - 1095pg/ml)(下降48%)。只有2例患者的血浆iPTH水平恢复正常,而10例中有8例bAP恢复正常。5例患者的血浆iPTH浓度仍高于正常值的5倍。相比之下,血浆bAP水平从基线时的47.6±32.2ng/ml(范围15.4 - 130.0ng/ml)降至第52周时的17.8±9.9ng/ml(范围8.0 - 38.0ng/ml)(下降63%)。在接受阿法骨化醇治疗15.8±5.1个月后,6例患者进行了骨组织形态计量学检查。他们均不符合骨再生障碍性骨病的标准,因为他们的骨吸收增加且骨髓骨纤维化。2例患者的骨形成率正常,另外4例无法测量。2例患者出现骨软化迹象。总之,阿法骨化醇优先降低骨形成率,而非继发性甲状旁腺功能亢进的其他组织学参数。它降低血浆bAP的效率比iPTH更高。

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