Effects of Anti-Sclerostin Antibody Release from Porous Microparticles on Bone Resorption Inhibition of Osteoblasts

Q2 Pharmacology, Toxicology and Pharmaceutics
T. Ikoma, Hajime Watanabe, Yasuhiro Nakagawa, S. Hattori, T. Minowa, N. Hanagata
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引用次数: 0

Abstract

Anti-sclerostin antibodies are among the most efficient drugs for the treatment of osteoporosis, and have been also expected for the treatment of local bone disorders. We have previously developed porous microparticles of hydroxyapatite and chondroitin sulfate loading anti-sclerostin antibodies formulated with zinc cations. However, the biological behavior and concentration dependence of anti-sclerostin antibodies in vitro released from the microparticles remain unclear. Bolus administration and the subsequent release of anti-sclerostin antibodies from the microparticles formulated with or without zinc cations were investigated; bone-resorptive inhibitory effects on mouse MC3T3-E1 osteoblast function were revealed by cell culture using a cell culture insert plate. Differentiation induction culture of osteoblasts was performed after maintaining the concentrations of anti-sclerostin antibodies and sclerostin at previously reported concentrations of 5.0 and 1.0 µg/mL for the first 3 days. Subsequently, the medium was replaced with fresh medium that did not contain anti-sclerostin antibodies but microparticles loading anti-sclerostin antibodies (20 or 80 µg/mg) with or without zinc cations in the cell culture insert. After 11 days of incubation, the bioactivity of the osteoblasts was evaluated using the polymerase chain reaction method. The formulation using zinc cations showed an increase of anti-sclerostin antibodies released from the microparticles, which increased the expression of receptor activator of the nuclear factor kappa-B ligand in the osteoblasts on day 14. This result indicates the inhibition of sclerostin-mediated bone resorption. However, the increase of loading amounts of anti-sclerostin antibodies extremely enhanced the subsequent release of anti-sclerostin antibodies, which decreased the inhibition of bone resorption contrary to expectations. The moderately sustained release of anti-sclerostin antibodies from the microparticles can promote the inhibition of bone resorption in osteoblasts, supporting the potential of this formulation for the treatment of localized bone disorders.
多孔微颗粒释放抗硬化抗体对成骨细胞骨吸收抑制的影响
抗硬化素抗体是治疗骨质疏松症最有效的药物之一,也有望用于治疗局部骨骼疾病。我们之前已经开发了羟基磷灰石和硫酸软骨素的多孔微粒,负载用锌阳离子配制的抗硬化素抗体。然而,从微粒中释放的抗硬化素抗体的生物学行为和浓度依赖性尚不清楚。研究了Bolus给药和随后从含有或不含有锌阳离子的微粒中释放抗硬化素抗体;通过使用细胞培养插入板的细胞培养揭示了对小鼠MC3T3-E1成骨细胞功能的骨吸收抑制作用。在前3天将抗硬化蛋白抗体和硬化蛋白的浓度维持在先前报道的5.0和1.0µg/mL的浓度后,进行成骨细胞的分化诱导培养。随后,用新鲜培养基代替培养基,所述新鲜培养基不包含抗硬化蛋白抗体,但在细胞培养插入物中含有或不含有锌阳离子的载有抗硬化素抗体的微粒(20或80µg/mg)。培养11天后,使用聚合酶链式反应方法评估成骨细胞的生物活性。使用锌阳离子的制剂显示从微粒释放的抗硬化素抗体增加,这在第14天增加了成骨细胞中核因子κB配体的受体激活剂的表达。这一结果表明硬化素介导的骨吸收受到抑制。然而,抗硬化蛋白抗体负载量的增加极大地增强了抗硬化蛋白的随后释放,这与预期相反地降低了对骨吸收的抑制。从微粒中适度持续释放抗硬化素抗体可以促进对成骨细胞骨吸收的抑制,支持该制剂治疗局部骨疾病的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Drug Delivery Letters
Drug Delivery Letters Pharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (miscellaneous)
CiteScore
1.70
自引率
0.00%
发文量
30
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