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首页> 外文期刊>Proceedings of the Nutrition Society >Integrin antagonists as inhibitors of bone resorption: implications fortreatment
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Integrin antagonists as inhibitors of bone resorption: implications fortreatment

机译:整联蛋白拮抗剂作为骨吸收抑制剂:对治疗的影响

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摘要

Currently 'accepted' treatments for bone disease utilise drugs that inhibit osteoclastic bone resorption; these lead to a reduction in subsequent bone loss and thence, indirectly, to an increase in bone mass and fewer fractures. Three classes of compounds currently form the mainstay of therapy for osteoporosis: oestrogens (hormone-replacement therapy), 'selective oestrogen receptor modulators' and the bisphosphonates. Problems of patient compliance, real or theoretical long-term toxicological risks and the lack of bone anabolic agents of clinical utility suggest that there is a need for the development of further novel osteoclast resorption inhibitors. Recent biological and genetic findings in the area of bone cell function have led to the identification of new drug targets. These drugs include agents that (directly or indirectly): inhibit osteoclast adhesion to bone matrix; modify osteoclast differentiation; act on the proton pump and hence affect extracellullar acidification; antagonise extracellular enzymes that are involved in bone matrix protein degradation. Particular emphasis is placed in the present review on the evaluation of antagonists of alphav beta3 integrin-mediated cell adhesion for use in bone disease. The wealth of new agents being developed suggests that resorption inhibition will be the best treatment for osteoporosis in the short to medium term, with the long-term aim still being toward developing anabolic drugs or cell therapeutics.
机译:目前对骨病的“公认”疗法采用抑制破骨细胞骨吸收的药物。这些导致减少了随后的骨丢失,因此间接地导致了骨量的增加和骨折的减少。目前,三类化合物构成骨质疏松症治疗的主要手段:雌激素(激素替代疗法),“选择性雌激素受体调节剂”和双膦酸盐。患者依从性,实际或理论上的长期毒理学风险以及缺乏临床实用的骨合成代谢剂的问题表明需要开发进一步的新型破骨细胞吸收抑制剂。在骨细胞功能领域的最新生物学和遗传发现已导致新药靶标的鉴定。这些药物包括(直接或间接)抑制破骨细胞粘附于骨基质的药物;改变破骨细胞的分化;作用于质子泵上,从而影响细胞外酸化;拮抗参与骨基质蛋白降解的细胞外酶。在本综述中特别强调对用于骨疾病的αvβ3整联蛋白介导的细胞粘附拮抗剂的评价。正在开发的大量新药表明,在短期到中期,抑制吸收将是骨质疏松症的最佳治疗方法,而长期目标仍是开发合成代谢药物或细胞疗法。

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