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骨质疏松症:病理生理学、预防、诊断及治疗

Osteoporosis: pathophysiology, prevention, diagnosis, and treatment.

作者信息

Odell W D, Heath H

机构信息

University of Utah, Salt Lake City.

出版信息

Dis Mon. 1993 Nov;39(11):789-867.

PMID:8223093
Abstract

Bone is a living tissue; throughout life, new bone formation coexists with bone resorption. Although a large number of hormones and cytokines modulate osteoblast and osteoclast function, osteoporosis results from any disorder in which bone formation becomes uncoupled from bone resorption. Many disorders are associated with the uncoupling of bone formation and resorption. The most common is loss of gonadal steroid action on bone, as occurs in menopause or in male and female hypogonadism not associated with menopause. Other relatively common causes include primary hyperparathyroidism and endogenous or exogenous hypercortisolism and thyrotoxicosis. A large number of other, less frequent disorders also cause osteoporosis. Treatment of osteoporosis consists first of removing the cause if possible, for example, abolishing hypercortisolism, thyrotoxicosis, or hyperparathyroidism. In menopausal women or hypogonadal men or women, replacement of estrogens or androgens represents effective therapy. Estrogens and androgens given to hypogonadal subjects strikingly reduce bone resorption. For patients with established osteoporosis who either cannot take gonadal steroids or who are not hypogonadal, calcitonin decreases bone resorption and may stabilize bone mass. Estrogen replacement and calcitonin are approved by the Food and Drug Administration for treatment of osteoporosis. Experimental therapies presently include 1,25-dihydroxyvitamin D (calcitriol), bisphosphonates in intermittent treatment regimes, and fluoride in lower dosages than were used in previous studies. The use of fluoride is controversial, and to some extent it has fallen into disrepute. Effective use of any treatment is predicated on understanding the pathophysiology in any particular disease setting.

摘要

骨骼是一种活组织;在整个生命过程中,新骨形成与骨吸收同时存在。尽管大量激素和细胞因子调节成骨细胞和破骨细胞的功能,但骨质疏松症是由任何导致骨形成与骨吸收解偶联的疾病引起的。许多疾病都与骨形成和吸收的解偶联有关。最常见的是性腺类固醇对骨骼作用的丧失,如在绝经时或与绝经无关的男性和女性性腺功能减退时发生的情况。其他相对常见的原因包括原发性甲状旁腺功能亢进、内源性或外源性皮质醇增多症以及甲状腺毒症。还有许多其他不太常见的疾病也会导致骨质疏松症。骨质疏松症的治疗首先是尽可能消除病因,例如,消除皮质醇增多症、甲状腺毒症或甲状旁腺功能亢进。对于绝经后妇女或性腺功能减退的男性或女性,补充雌激素或雄激素是有效的治疗方法。给予性腺功能减退患者雌激素和雄激素可显著减少骨吸收。对于已确诊骨质疏松症且不能服用性腺类固醇或并非性腺功能减退的患者,降钙素可减少骨吸收并可能稳定骨量。雌激素替代疗法和降钙素已获美国食品药品监督管理局批准用于治疗骨质疏松症。目前的实验性疗法包括1,25 - 二羟维生素D(骨化三醇)、间歇治疗方案中的双膦酸盐以及比以往研究使用剂量更低的氟化物。氟化物的使用存在争议,在某种程度上已声名狼藉。任何治疗方法的有效应用都基于对任何特定疾病背景下病理生理学的理解。

相似文献

1
Osteoporosis: pathophysiology, prevention, diagnosis, and treatment.骨质疏松症:病理生理学、预防、诊断及治疗
Dis Mon. 1993 Nov;39(11):789-867.
2
Osteoporosis: new hope for the future.骨质疏松症:未来的新希望。
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Osteoporosis: detection, prevention, and treatment in primary care.骨质疏松症:初级保健中的检测、预防与治疗
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Osteoporosis prevention and treatment.骨质疏松症的预防与治疗。
Med J Aust. 2000 Mar 6;172(5):226-9.
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Osteoporosis--a review.
Clin Ther. 1989;11(1):3-14.
6
Osteoporosis management.骨质疏松症管理
Int J Fertil Womens Med. 1999 Sep-Oct;44(5):241-9.
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Clinical practice guidelines for the diagnosis and management of osteoporosis. Scientific Advisory Board, Osteoporosis Society of Canada.骨质疏松症诊断与管理临床实践指南。加拿大骨质疏松症协会科学咨询委员会。
CMAJ. 1996 Oct 15;155(8):1113-33.
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Osteoporosis: preventive strategies.骨质疏松症:预防策略
Int J Fertil Womens Med. 1998 Mar-Apr;43(2):56-64.
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[Prevention and treatment of corticosteroid-induced osteoporosis].[糖皮质激素性骨质疏松症的防治]
Rev Med Suisse Romande. 2000 Oct;120(10):787-91.
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Management of osteoporosis due to ovarian failure.卵巢功能衰竭所致骨质疏松的管理
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