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甲状旁腺对骨代谢的影响。

Influence of the parathyroid glands on bone metabolism.

作者信息

Malluche H H, Koszewski N, Monier-Faugere M C, Williams J P, Mawad H

机构信息

University of Kentucky, Lexington, KY 40536, USA.

出版信息

Eur J Clin Invest. 2006 Aug;36 Suppl 2:23-33. doi: 10.1111/j.1365-2362.2006.01664.x.

DOI:10.1111/j.1365-2362.2006.01664.x
PMID:16884395
Abstract

Bone is a classic target tissue for parathyroid hormone (PTH), whose calciotropic effect is mediated largely via catabolic actions on this tissue. Paradoxically, PTH also exerts anabolic actions, with intermittent injections of PTH or its amino-terminal fragments causing an increase in bone formation and bone mass, actions that form the basis for the use of PTH in the treatment of osteoporosis. Besides vitamin D, PTH is the only other known bone anabolic agent. High-affinity PTH receptors (PTH-1R) have been detected on osteoblasts and osteoclasts (albeit in lower numbers). Bone turnover, which includes activation of osteoclasts and osteoblasts, appears to be best reflected not by absolute concentrations of PTH (which can vary based on the assay and antibody used) but by a balance of circulating full-length PTH-(1-84) and amino-terminally truncated C-PTH fragments. When PTH-(1-84) is predominant, bone turnover is promoted. Among PTH fragments, PTH-(7-84) appears to be the most potent antagonist of PTH-(1-84). The mechanisms involved in these effects are unclear although mediation via unique C-terminal receptors has been suggested. We propose that, within the range of total PTH (100-1000 pg mL(-1)), the ratio of PTH-(1-84)/C-PTH fragment is a valuable tool for diagnosis of bone turnover. Data indicate that at PTH levels < 100-150 pg mL(-1) and > 1000 pg mL(-1), the ratio looses its predictive power. Assay type, patient characteristics (race, underlying renal disease) and treatment attributes (vitamin D, corticosteroids, phosphate binders) have an impact on the PTH ratio, and care should be used in interpreting assay results and making subsequent treatment decisions.

摘要

骨骼是甲状旁腺激素(PTH)的经典靶组织,其对钙的影响主要通过对该组织的分解代谢作用来介导。矛盾的是,PTH也具有合成代谢作用,间歇性注射PTH或其氨基末端片段会导致骨形成增加和骨量增加,这些作用构成了使用PTH治疗骨质疏松症的基础。除了维生素D,PTH是唯一已知的其他骨合成代谢剂。在成骨细胞和破骨细胞上已检测到高亲和力的PTH受体(PTH-1R)(尽管数量较少)。骨转换包括破骨细胞和成骨细胞的激活,似乎最佳反映指标不是PTH的绝对浓度(其可能因所用的检测方法和抗体而异),而是循环中全长PTH-(1-84)和氨基末端截短的C-PTH片段的平衡。当PTH-(1-84)占主导时,骨转换会被促进。在PTH片段中,PTH-(7-84)似乎是PTH-(1-84)最有效的拮抗剂。尽管有人提出通过独特的C末端受体介导,但这些作用所涉及的机制尚不清楚。我们提出,在总PTH(100 - 1000 pg mL⁻¹)范围内,PTH-(1-84)/C-PTH片段的比值是诊断骨转换的有价值工具。数据表明,当PTH水平<100 - 150 pg mL⁻¹和>1000 pg mL⁻¹时,该比值失去其预测能力。检测类型、患者特征(种族、潜在肾病)和治疗属性(维生素D、皮质类固醇、磷酸盐结合剂)会对PTH比值产生影响,在解释检测结果和做出后续治疗决策时应谨慎。

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