Effect of oxytocin receptor antagonist (GSK-221-149-A) on mandibular bone porosity in peri-menopausal rats

Pub Date : 2024-05-01 DOI:10.52083/xmjo8562
Ahmed S. Ahmed, Liju S Mathew, Marwa M. Mona, Omaima K. Docmac, Hoda A. Ibrahim, A. Elshamy, E. Hantash, Rasha A. Elsisy
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Abstract

The period of peri-menopause (PMP) is characterized by hormonal fluctuations that impact the strength and health of bones. Oxytocin (OX), a small peptide known to be present in bone tissue, is the focus of this study. The objective of this research is to gain a better understanding of how OX precisely functions in the remodeling process of the mandibular bone. This understanding is seen as a crucial step in preventing the loss of both cortical and trabecular bone during the PMP. The current findings indicate that OX plays a role in preserving both compact and trabecular bone tissues, enhancing the mineral-to-matrix ratio, and regulating bone markers. Furthermore, it reduces porosity in both cortical and trabecular bone levels. Interestingly, these effects are reversed when an oxytocin receptor antagonist (GSK-221,149-A) is introduced, suggesting that OX’s bone-preserving action is primarily mediated through the oxytocin receptor, rather than other mechanisms.
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催产素受体拮抗剂(GSK-221-149-A)对围绝经期大鼠下颌骨孔隙率的影响
围绝经期(PMP)的特点是激素波动影响骨骼的强度和健康。催产素(OX)是已知存在于骨组织中的一种小肽,是本研究的重点。这项研究的目的是更好地了解 OX 如何在下颌骨的重塑过程中准确发挥作用。这种了解被认为是防止 PMP 期间皮质骨和小梁骨流失的关键一步。目前的研究结果表明,OX 在保存密实骨组织和骨小梁组织、提高矿物质与基质的比例以及调节骨标记物方面发挥作用。此外,它还能降低骨皮质和骨小梁的孔隙率。有趣的是,当引入催产素受体拮抗剂(GSK-221,149-A)时,这些作用会被逆转,这表明 OX 的保骨作用主要是通过催产素受体而不是其他机制介导的。
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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