SRT2183 and SRT1720, but not Resveratrol, Inhibit Osteoclast Formation and Resorption in the Presence or Absence of Sirt1

R. Thiyagarajan, María Rodríguez-Gonzalez, Catherine Zaw, K. Seldeen, Mireya Hernandez, M. Pang, B. Troen
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Abstract

Background: Osteoclastic bone resorption markedly increases with aging, leading to osteoporosis characterized by weak and fragile bones. Mice exhibit greater bone resorption and poor bone mass when Sirt1 is removed from their osteoclasts. Here we investigated the ex vivo impacts of putative Sirt1 activators, Resveratrol (RSV), SRT2183, and SRT1720, on osteoclast formation and activity in primary mouse bone marrow cells (BMCs) derived from wild-type (WT) and osteoclast specific Sirt1 knockout (OC-Sirt1KO) mice and in the RAW264.7 mouse macrophage cell line. Results: We found that SRT2183 and SRT1720 inhibit the formation of osteoclasts and actin belts in BMCs and RAW264.7 cells, whereas RSV does not. We also observed that the OC-Sirt1KO mice exhibited less bone mineral density, and the BMCs harvested from these mice yielded more osteoclasts than BMCs harvested from littermate controls. Interestingly, both SRT2183 and SRT1720 reduced osteoclast and actin belt formation in BMCs from OC-Sirt1KO mice. SRT2183 and SRT1720 also significantly disrupted actin belts of mature osteoclasts generated from BMCs of WT mice, within 3 and 6 hours of administration, respectively. Furthermore, these compounds inhibited the resorption activity of mature osteoclasts, while RSV did not. Conclusion: Our findings suggest SRT2183 and SRT1720 impede bone resorption by disrupting actin belts of mature osteoclasts, inhibit actin belt formation, and inhibit osteoclastogenesis even in the absence of Sirt1. Thus, the mechanism of action of these compounds appears to extend beyond Sirt1 activation and possibly pave the way for potential new therapies in alleviating osteoporosis associated bone loss.
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SRT2183和SRT1720,而不是白藜芦醇,在存在或不存在Sirt1的情况下抑制破骨细胞的形成和吸收
背景:随着年龄的增长,骨碎屑骨吸收显著增加,导致骨质疏松症,其特征是骨骼脆弱。当从破骨细胞中去除Sirt1时,小鼠表现出更大的骨吸收和较差的骨量。在这里,我们研究了推定的Sirt1激活剂白藜芦醇(RSV)、SRT2183和SRT1720对来源于野生型(WT)和破骨细胞特异性Sirt1敲除(OC-Sirt1KO)小鼠的原代小鼠骨髓细胞(BMCs)和RAW264.7小鼠巨噬细胞系中破骨细胞形成和活性的离体影响。结果:我们发现SRT2183和SRT1720抑制BMCs和RAW264.7细胞中破骨细胞和肌动蛋白带的形成,而RSV则不抑制。我们还观察到,OC-Sirt1KO小鼠表现出较少的骨密度,并且从这些小鼠收获的BMCs比从同窝对照收获的BMC产生更多的破骨细胞。有趣的是,SRT2183和SRT1720都减少了OC-Sirt1KO小鼠BMCs中破骨细胞和肌动蛋白带的形成。SRT2183和SRT1720也分别在给药3小时和6小时内显著破坏了WT小鼠BMCs产生的成熟破骨细胞的肌动蛋白带。此外,这些化合物抑制了成熟破骨细胞的吸收活性,而呼吸道合胞病毒则没有。结论:我们的研究结果表明,SRT2183和SRT1720通过破坏成熟破骨细胞的肌动蛋白带来阻碍骨吸收,抑制肌动蛋白带的形成,甚至在没有Sirt1的情况下也能抑制破骨细胞生成。因此,这些化合物的作用机制似乎超越了Sirt1的激活,并可能为缓解骨质疏松症相关骨丢失的潜在新疗法铺平道路。
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SRT2183 and SRT1720, but not Resveratrol, Inhibit Osteoclast Formation and Resorption in the Presence or Absence of Sirt1. SRT2183 and SRT1720, but not Resveratrol, Inhibit Osteoclast Formation and Resorption in the Presence or Absence of Sirt1 Synthetic Peptide CK2.3 Enhances Bone Mineral Density in Senile Mice.
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