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使用盐酸司维拉姆和维生素D疗法管理透析患者的钙、磷和骨代谢

Management of calcium, phosphorus and bone metabolism in dialysis patients using sevelamer hydrochloride and vitamin D therapy.

作者信息

Ishida Mari, Yao Naoyuki, Yachiku Setsuko, Anzai Tsutomu, Kobayashi Takeshi, Ishida Hironori

机构信息

Jinyukai Kitasaito Hospital, Asahikawa City, Hokkaido, Japan.

出版信息

Ther Apher Dial. 2005 Aug;9 Suppl 1:S16-21. doi: 10.1111/j.1744-9987.2005.00325.x.

Abstract

Abnormalities of mineral metabolism, including those of calcium (Ca), phosphorus (P), and parathyroid hormone (PTH) in patients on maintenance hemodialysis induce severe bone involvement, which manifests as renal osteodystrophy. Recently, vascular calcification caused by abnormal mineral metabolism has been attracting attention because cardiovascular diseases (CVD) are a major cause of death in hemodialysis patients. Since 2000, the treatment standard for overt secondary hyperparathyroidism (SHPT) in our facilities has shifted from conventional or pulse therapy with oral vitamin D3 (VitD) to intravenous pulse therapy with maxacalcitriol or calcitriol. After selecting the criterion of overt SHPT as intact-PTH>500 pg/mL, the proportion of overt SHPT cases among all hemodialysis patients decreased from 12% at the start of intravenous pulse treatment to 6.4% after 4 years' treatment. However, the number of patients who had an interruption to pulse treatment because of hypercalcemia and/or hyperphosphatemia was high and it became a bottleneck for the continuation of the therapy. The major cause of hypercalcemia is considered to be Ca load derived from oral calcium carbonate. In Japan, sevelamer hydrochrolide (SH), which does not contain Ca, has been available commercially since 2003 and potentially should enable a reduction in the incidence of overt SHPT during long-term intravenous treatment when combined with careful adjustment of the dose of VitD and strict monitoring of Ca and P level concentrations. In this study, we found that the proportion of patients who satisfy the recommended serum concentrations of Ca and P reported by K/DOQI guideline was low irrespective of the serum concentration of intact-PTH. The aortic calcification index was high in the patient group with lower intact-PTH level concentration, probably because of reduced Ca and P buffering ability associated with reduced bone turnover. We consider that VitD treatment with SH might give better control of the intact-PTH level concentration within the range recommended by the K/DOQI guideline.

摘要

维持性血液透析患者的矿物质代谢异常,包括钙(Ca)、磷(P)和甲状旁腺激素(PTH)异常,会导致严重的骨骼病变,表现为肾性骨营养不良。近年来,矿物质代谢异常引起的血管钙化备受关注,因为心血管疾病(CVD)是血液透析患者的主要死亡原因。自2000年以来,我们机构中明显继发性甲状旁腺功能亢进(SHPT)的治疗标准已从口服维生素D3(VitD)的传统或脉冲疗法转变为使用最大剂量骨化三醇或骨化三醇的静脉脉冲疗法。选择明显SHPT的标准为完整PTH>500 pg/mL后,所有血液透析患者中明显SHPT病例的比例从静脉脉冲治疗开始时的12%降至治疗4年后的6.4%。然而,因高钙血症和/或高磷血症而中断脉冲治疗的患者数量很多,这成为治疗持续进行的瓶颈。高钙血症的主要原因被认为是口服碳酸钙产生的钙负荷。在日本,不含钙的盐酸司维拉姆(SH)自2003年起已上市销售,与仔细调整VitD剂量和严格监测钙和磷水平浓度相结合,在长期静脉治疗期间可能会降低明显SHPT的发生率。在本研究中,我们发现无论完整PTH的血清浓度如何,符合K/DOQI指南推荐的钙和磷血清浓度的患者比例都很低。完整PTH水平浓度较低的患者组主动脉钙化指数较高,可能是因为骨转换减少导致钙和磷缓冲能力降低。我们认为,使用SH进行VitD治疗可能会在K/DOQI指南推荐的范围内更好地控制完整PTH水平浓度。

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