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22-氧杂骨化三醇对重度继发性甲状旁腺功能亢进血液透析患者骨组织学的影响。

Effect of 22-oxacalcitriol on bone histology of hemodialyzed patients with severe secondary hyperparathyroidism.

作者信息

Tsukamoto Y, Hanaoka M, Matsuo T, Saruta T, Nomura M, Takahashi Y

机构信息

Division of Nephrology, Fourth Department of Internal Medicine, Kitasato University School of Medicine, Kanagawa, Japan.

出版信息

Am J Kidney Dis. 2000 Mar;35(3):458-64. doi: 10.1016/s0272-6386(00)70198-3.

Abstract

To examine the effectiveness of 22-oxacalcitriol (OCT) injection on the improvement of severe osteitis fibrosa, we studied 10 hemodialyzed patients (age, 59 +/- 12 years). The initial OCT dose was 5 microg and was administered three times weekly at the end of each hemodialysis session. OCT doses (1, 3, 5, 10, 15, and 20 microg) were changed in subsequent weeks to maintain serum calcium levels at less than 11.5 mg/dL. Administration of OCT significantly suppressed serum intact parathyroid hormone (PTH) from an initial level of 1,193 +/- 584 to 775 +/- 552 pg/mL in the 24th week (n = 10). OCT increased PTH levels again to 857 +/- 635 pg/mL in the 48th week (n = 7). Among the 10 patients, 5 patients (high responders) showed more than a 50% suppression of serum intact PTH levels at the end of the study. The rest of the patients had hypercalcemia and did not receive increased OCT doses (low responders). At the start of the treatment, the only difference between high and low responders was serum calcium level. Serum calcium levels (adjusted for serum albumin level) increased from 9.7 +/- 0.7 mg/dL (n = 10) at the beginning to 10.5 +/- 0.6 mg/dL (n = 10) in the 24th week and to 11. 1 +/- 0.7 mg/dL (n = 7) in the 48th week. Six patients (1 to 6) agreed to undergo a second bone biopsy in the 24th week of OCT administration. In bone histomorphometric measurements, OCT significantly changed bone marrow fibrosis, mineralization (labeled mineralizing surface and bone formation rate), and osteoid formation (osteoid volume and thickness). In conclusion, intravenous OCT effectively suppressed PTH secretion and improved the bone histological characteristics of severe osteitis fibrosa, especially in patients with initial serum calcium levels less than 10 mg/dL. With concerns about OCT causing adynamic bone, additional bone histological data are needed to ensure the long-term safety of OCT.

摘要

为研究22 - 氧杂骨化三醇(OCT)注射剂改善重度纤维性骨炎的有效性,我们对10例血液透析患者(年龄59±12岁)进行了研究。初始OCT剂量为5微克,在每次血液透析结束时每周给药3次。在随后几周调整OCT剂量(1、3、5、10、15和20微克),以将血清钙水平维持在11.5毫克/分升以下。OCT给药显著抑制血清完整甲状旁腺激素(PTH)水平,从初始的1193±584皮克/毫升降至第24周时的775±552皮克/毫升(n = 10)。在第48周时,OCT又使PTH水平升至857±635皮克/毫升(n = 7)。10例患者中,5例(高反应者)在研究结束时血清完整PTH水平抑制超过50%。其余患者出现高钙血症,未增加OCT剂量(低反应者)。治疗开始时,高反应者与低反应者之间唯一的差异是血清钙水平。血清钙水平(根据血清白蛋白水平校正)从开始时的9.7±0.7毫克/分升(n = 10)升至第24周时的10.5±0.6毫克/分升(n = 10),并在第48周时升至11.1±0.7毫克/分升(n = 7)。6例患者(1至6号)同意在OCT给药第24周时接受第二次骨活检。在骨组织形态计量学测量中,OCT显著改变了骨髓纤维化、矿化(标记矿化表面和骨形成率)以及类骨质形成(类骨质体积和厚度)。总之,静脉注射OCT能有效抑制PTH分泌,改善重度纤维性骨炎的骨组织学特征,尤其是初始血清钙水平低于10毫克/分升的患者。鉴于担心OCT会导致骨无动力,需要更多的骨组织学数据来确保OCT的长期安全性。

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