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与完整甲状旁腺激素(PTH)检测相比,使用PTH检测低钙血症性PTH片段抑制剂能更准确地评估肾性骨营养不良。

The assay of the hypocalcemic PTH fragment inhibitor with PTH provides a more accurate assessment of renal osteodystrophy compared to the intact PTH assay.

作者信息

Cantor T, Sci B

机构信息

Scantibodies Laboratory, Inc., 9336 Abraham Way, Santee, CA 92071-2862, USA.

出版信息

Nefrologia. 2003;23 Suppl 2:69-72.

Abstract

As the chronic kidney disease patient is being managed for PTH, calcium, phosphate, vitamin D, calcium x phosphate product and bone quality an accurate PTH measurement is essential. Over and under PTH suppressive therapies pose significant risks of mineral metabolism disturbances, osteodystrophies and soft tissue calcifications. Until recently it was thought that there was only one hormone secreted by the parathyroid gland, 1-84 PTH (or CAP). It is now known that there is another hormone secreted by the parathyroid gland (CIP) which is most likely 7-84 PTH. 7-84 PTH has been demonstrated to be an antagonist of 1-84 PTH with inverse biological activities. 7-84 PTH has been demonstrated to be hypocalcemic and able to lower bone turnover through an inhibition of osteoclast formation resulting in an overall inhibition of bone resorption. Whereas, 1-84 PTH operates through the PTH/PTHrp receptor the 7-84 PTH appears to operate through a C terminal PTH receptor. The CAP/CIP ratio decreases in the dialysis patient when calcium increases and vice versa. The 2nd generation "intact" PTH assays measure the sum of CAP plus CIP which render them ineffective at predicting bone turnover (72% predictive) and monitoring PTH suppressive treatments. By contrast the CAP/CIP ratio predicts bone turnover in the dialysis patient with a histologically determined 93% predictability. An elevated CAP/CIP ratio indicates high bone turnover and a decreased CAP/CIP ratio indicates adynamic low bone turnover.

摘要

在对慢性肾脏病患者进行甲状旁腺激素(PTH)、钙、磷、维生素D、钙磷乘积及骨质量的管理时,准确测量PTH至关重要。PTH抑制治疗过度或不足都会带来矿物质代谢紊乱、骨营养不良和软组织钙化的重大风险。直到最近,人们还认为甲状旁腺仅分泌一种激素,即1-84 PTH(或CAP)。现在已知甲状旁腺还分泌另一种激素(CIP),很可能是7-84 PTH。已证实7-84 PTH是1-84 PTH的拮抗剂,具有相反的生物学活性。已证实7-84 PTH具有降钙作用,能够通过抑制破骨细胞形成来降低骨转换,从而全面抑制骨吸收。而1-84 PTH通过PTH/PTHrp受体发挥作用,7-84 PTH似乎通过C末端PTH受体发挥作用。透析患者的CAP/CIP比值会随钙水平升高而降低,反之亦然。第二代“完整”PTH检测方法测量的是CAP与CIP之和,这使得它们在预测骨转换(预测率72%)和监测PTH抑制治疗方面效果不佳。相比之下,CAP/CIP比值在组织学测定中对透析患者骨转换的预测率为93%。CAP/CIP比值升高表明骨转换高,而CAP/CIP比值降低表明骨转换低动力。

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