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使用新开发的检测II型胶原降解产物的方法评估双膦酸盐对软骨更新的影响。

Effect of bisphosphonates on cartilage turnover assessed with a newly developed assay for collagen type II degradation products.

作者信息

Lehmann H J, Mouritzen U, Christgau S, Cloos P A C, Christiansen C

机构信息

Centre for Clinical and Basic Research, Ballerup, Denmark Osteometer Biotech A/S, Herlev, Denmark.

出版信息

Ann Rheum Dis. 2002 Jun;61(6):530-3. doi: 10.1136/ard.61.6.530.

Abstract

BACKGROUND

Animal studies of arthritis have suggested that bisphosphonates may have chondroprotective abilities.

OBJECTIVE

To evaluate the effect of bisphosphonate treatment on cartilage degradation.

METHODS

Type II collagen is almost exclusively localised in cartilage, where it is the major structural component of the tissue. Hence fragments derived from this protein should represent a specific index for cartilage degradation. The urinary concentration of collagen type II C-telopeptide degradation products (CTX-II) was measured by a new immunoassay (enzyme linked immunosorbent assay (ELISA)). The serum concentration of collagen type I C-telopeptide degradation products (CTX-I), a marker of bone degradation, was also measured by ELISA.

PARTICIPANTS

Two groups were studied. The alendronate group included 63 healthy postmenopausal women aged 45-54 randomly allocated to receive three years' treatment with 1 mg, 5 mg, 10 mg, or 20 mg alendronate daily or placebo. In the third year the women receiving 20 mg were switched to placebo. The ibandronate group included 119 women at least 10 years after the menopause aged <75 randomly allocated to receive 12 months' treatment with 0.25 mg, 0.5 mg, 1.0 mg, 2.5 mg, or 5 mg ibandronate daily or placebo followed by 12 months without treatment.

RESULTS

20 mg of alendronate and 2.5 and 5 mg of ibandronate treatment produced significant decreases in urinary CTX-II to about 50% of baseline. The level reached after three months of treatment remained practically constant during the following 12-36 treatment months. When treatment was withdrawn CTX-II values returned towards baseline. Serum CTX-I also decreased rapidly within three months, but to a level of about 30% of baseline.

CONCLUSIONS

The urinary excretion of CTX-II, a new marker of cartilage degradation, decreases significantly in response to bisphosphonate. This suggests that bisphosphonates may have chondroprotective effects in humans. By measurement of CTX-II it should be possible to monitor the effects of drugs that potentially inhibit cartilage destruction.

摘要

背景

关节炎的动物研究表明,双膦酸盐可能具有软骨保护能力。

目的

评估双膦酸盐治疗对软骨降解的影响。

方法

II型胶原蛋白几乎仅存在于软骨中,是该组织的主要结构成分。因此,源自该蛋白质的片段应代表软骨降解的特定指标。通过一种新的免疫测定法(酶联免疫吸附测定法(ELISA))测量尿中II型胶原C-末端肽降解产物(CTX-II)的浓度。还通过ELISA测量血清I型胶原C-末端肽降解产物(CTX-I)的浓度,其为骨降解的标志物。

参与者

研究了两组。阿仑膦酸钠组包括63名45 - 54岁的健康绝经后妇女,她们被随机分配接受为期三年的每日1毫克、5毫克、10毫克或20毫克阿仑膦酸钠治疗或安慰剂治疗。在第三年,接受20毫克治疗的妇女改用安慰剂。伊班膦酸钠组包括119名绝经至少10年且年龄小于75岁的妇女,她们被随机分配接受为期12个月的每日0.25毫克、0.5毫克、1.0毫克、2.5毫克或5毫克伊班膦酸钠治疗或安慰剂治疗,随后12个月不接受治疗。

结果

20毫克阿仑膦酸钠以及2.5毫克和5毫克伊班膦酸钠治疗使尿CTX-II显著降低至基线的约50%。治疗三个月后达到的水平在随后的12 - 36个治疗月期间基本保持不变。当停止治疗时,CTX-II值恢复至基线水平。血清CTX-I在三个月内也迅速下降,但降至基线的约30%。

结论

作为软骨降解的新标志物,CTX-II的尿排泄量因双膦酸盐而显著降低。这表明双膦酸盐在人类中可能具有软骨保护作用。通过测量CTX-II,应该能够监测潜在抑制软骨破坏的药物的效果。

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