Hydroxychloroquine and a low antiresorptive activity bisphosphonate conjugate prevent and reverse ovariectomy-induced bone loss in mice through dual antiresorptive and anabolic effects.

IF 14.3 1区 医学 Q1 CELL & TISSUE ENGINEERING
Zhenqiang Yao, Akram Ayoub, Venkatesan Srinivasan, Jun Wu, Churou Tang, Rong Duan, Aleksa Milosavljevic, Lianping Xing, Frank H Ebetino, Alison J Frontier, Brendan F Boyce
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引用次数: 0

Abstract

Osteoporosis remains incurable. The most widely used antiresorptive agents, bisphosphonates (BPs), also inhibit bone formation, while the anabolic agent, teriparatide, does not inhibit bone resorption, and thus they have limited efficacy in preventing osteoporotic fractures and cause some side effects. Thus, there is an unmet need to develop dual antiresorptive and anabolic agents to prevent and treat osteoporosis. Hydroxychloroquine (HCQ), which is used to treat rheumatoid arthritis, prevents the lysosomal degradation of TNF receptor-associated factor 3 (TRAF3), an NF-κB adaptor protein that limits bone resorption and maintains bone formation. We attempted to covalently link HCQ to a hydroxyalklyl BP (HABP) with anticipated low antiresorptive activity, to target delivery of HCQ to bone to test if this targeting increases its efficacy to prevent TRAF3 degradation in the bone microenvironment and thus reduce bone resorption and increase bone formation, while reducing its systemic side effects. Unexpectedly, HABP-HCQ was found to exist as a salt in aqueous solution, composed of a protonated HCQ cation and a deprotonated HABP anion. Nevertheless, it inhibited osteoclastogenesis, stimulated osteoblast differentiation, and increased TRAF3 protein levels in vitro. HABP-HCQ significantly inhibited both osteoclast formation and bone marrow fibrosis in mice given multiple daily PTH injections. In contrast, HCQ inhibited marrow fibrosis, but not osteoclast formation, while the HABP alone inhibited osteoclast formation, but not fibrosis, in the mice. HABP-HCQ, but not HCQ, prevented trabecular bone loss following ovariectomy in mice and, importantly, increased bone volume in ovariectomized mice with established bone loss because HABP-HCQ increased bone formation and decreased bone resorption parameters simultaneously. In contrast, HCQ increased bone formation, but did not decrease bone resorption parameters, while HABP also restored the bone lost in ovariectomized mice, but it inhibited parameters of both bone resorption and formation. Our findings suggest that the combination of HABP and HCQ could have dual antiresorptive and anabolic effects to prevent and treat osteoporosis.

Abstract Image

羟氯喹和一种低抗骨吸收活性的双膦酸盐共轭物通过抗骨吸收和合成代谢的双重作用,预防和逆转卵巢切除术诱发的小鼠骨质流失。
骨质疏松症仍然无法治愈。最广泛使用的抗骨质吸收剂双膦酸盐(BPs)也抑制骨形成,而同化剂特立帕肽(teriparatide)并不抑制骨吸收,因此它们在预防骨质疏松性骨折方面的疗效有限,而且会产生一些副作用。因此,开发预防和治疗骨质疏松症的双重抗骨质吸收和同化药物的需求尚未得到满足。用于治疗类风湿性关节炎的羟氯喹(HCQ)可防止 TNF 受体相关因子 3(TRAF3)的溶酶体降解,TRAF3 是一种 NF-κB 适配蛋白,可限制骨吸收并维持骨形成。我们尝试将 HCQ 与羟基烷基酚 BP(HABP)共价连接,使其具有预期的低抗骨吸收活性,从而将 HCQ 靶向输送到骨骼,以测试这种靶向性是否能提高其功效,防止 TRAF3 在骨骼微环境中降解,从而减少骨吸收,增加骨形成,同时减少其全身副作用。意外的是,研究发现 HABP-HCQ 在水溶液中以盐的形式存在,由质子化的 HCQ 阳离子和去质子化的 HABP 阴离子组成。尽管如此,它在体外仍能抑制破骨细胞生成、刺激成骨细胞分化并增加 TRAF3 蛋白水平。每日多次注射 PTH 的小鼠体内,HABP-HCQ 可明显抑制破骨细胞的形成和骨髓纤维化。相反,HCQ 可抑制骨髓纤维化,但不能抑制破骨细胞的形成,而单独使用 HABP 可抑制小鼠破骨细胞的形成,但不能抑制骨髓纤维化。HABP-HCQ 而非 HCQ 可防止小鼠卵巢切除术后的骨小梁流失,而且重要的是,由于 HABP-HCQ 可同时增加骨形成和降低骨吸收参数,因此可增加已形成骨流失的卵巢切除小鼠的骨量。相反,HCQ 增加了骨形成,但没有降低骨吸收参数,而 HABP 也恢复了卵巢切除小鼠丢失的骨量,但同时抑制了骨吸收和骨形成参数。我们的研究结果表明,HABP和HCQ的组合可具有抗骨质吸收和合成代谢的双重作用,从而预防和治疗骨质疏松症。
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来源期刊
Bone Research
Bone Research CELL & TISSUE ENGINEERING-
CiteScore
20.00
自引率
4.70%
发文量
289
审稿时长
20 weeks
期刊介绍: Established in 2013, Bone Research is a newly-founded English-language periodical that centers on the basic and clinical facets of bone biology, pathophysiology, and regeneration. It is dedicated to championing key findings emerging from both basic investigations and clinical research concerning bone-related topics. The journal's objective is to globally disseminate research in bone-related physiology, pathology, diseases, and treatment, contributing to the advancement of knowledge in this field.
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