DEC1 deficiency protects against bone loss induced by ovariectomy by inhibiting inflammation.

IF 2.4 4区医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL Journal of Biomedical Research Pub Date : 2024-05-29 DOI:10.7555/JBR.38.20240069

Lan Lin, Zhiyi Qiang, Kaiao Chen, Ying Huo, Wei Liu, Jian Yang

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Abstract

Studies have shown that differentiated embryo-chondrocyte expressed gene 1 (DEC1) promotes osteoblast osteogenesis. To investigate the role of DEC1 in postmenopausal osteoporosis, we used the two genotypes of mice ( Dec1 ^+/+ and Dec1 ^-/-) to establish an ovariectomy model and found that the bone loss was significantly lower in Dec1 ^-/- ovariectomy mice than in Dec1 ^+/+ ovariectomy mice. The expression levels of RUNX2 and OSX were significantly increased in Dec1 ^-/- ovariectomy mice, compared with Dec1 ^+/+ ovariectomy mice; however, the expression levels of NFATc1, c-Fos, CTSK, and RANKL/OPG ratio were significantly decreased in Dec1 ^-/- ovariectomy mice, compared with those in Dec1 ^+/+ ovariectomy mice. Likewise, DEC1 deficiency also suppressed the expression levels of IL-6 and IL-1β. Further results showed that the mRNA expression levels of Runx2, Osx, and Alp were significantly increased in bone marrow mesenchymal stem cells of Dec1 ^-/- ovariectomy mice, compared with those of Dec1 ^+/+ ovariectomy mice. Moreover, the mRNA levels of Il1b, Il6, Tnfa, and Ifng were significantly increased in bone marrow-derived macrophages (BMMs) of Dec1 ^+/+ovariectomy mice, compared with those of Dec1 ^+/+ sham mice, but not in Dec1 ^-/- ovariectomy BMMs, when compared with those in Dec1 ^-/- sham BMMs. Additionally, the expression levels of p-IκBα and p-P65 were significantly increased in Dec1 ^+/+ ovariectomy BMMs, compared with those in Dec1 ^+/+ sham BMMs, but did not increase in Dec1 ^-/- ovariectomy BMMs, compared with those in Dec1 ^-/- sham BMMs. Taken together, DEC1 deficiency inhibited the NF-κB pathway induced by ovariectomy, thereby decreasing cytokines and subsequently inhibiting the decrease of osteogenesis and the increase of osteoclastogenesis caused by ovariectomy. The findings may provide a novel understanding of postmenopausal osteoporosis development, and offer potential avenues for the disease intervention.

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DEC1 缺乏症可通过抑制炎症防止卵巢切除术引起的骨质流失。

先前的研究表明，分化胚胎软骨细胞表达基因1（DEC1）可促进成骨细胞的成骨过程。为了研究 DEC1 在绝经后骨质疏松症（PMOP）中的作用，我们利用两种类型（DEC1 +/+、DEC1 -/-）的小鼠建立了卵巢切除（OVX）模型，发现 DEC1 -/- OVX 小鼠的骨量丢失远低于 DEC1 +/+ OVX 小鼠。与 DEC1 +/+ OVX 小鼠相比，DEC1 -/- OVX 小鼠中 RUNX2 和 OSX 的表达水平明显升高。与 DEC1 +/+ OVX 小鼠相比，DEC1 -/- OVX 小鼠的 NFATc1、c-Fos、CTSK 和 RANKL/OPG 表达水平明显下降。同样，DEC1 的缺乏也抑制了 IL-6 和 IL-1β。进一步研究发现，与 DEC1 +/+ OVX BMSCs 相比，DEC1 -/- OVX BMSCs 中的 Runx2、Osx、Alp 和 Ocn 明显增加。与 DEC1 +/+ 假 BMMs 相比，DEC1 +/+ OVX BMMs 中 IL-1β、IL-6、Tnf-α 和 Ifn-γ 的 mRNA 水平明显升高，但与 DEC1 -/- 假 BMMs 相比，DEC1 -/- OVX BMMs 的 mRNA 水平没有升高。此外，与 DEC1 +/+ 假 BMM 相比，DEC1 +/+ OVX BMM 的 p-IκBα 和 p-P65 明显增加，但与 DEC1 -/- 假 BMM 相比，DEC1 -/- OVX BMM 的 p-IκBα 和 p-P65 没有增加。综上所述，DEC1缺乏可抑制OVX诱导的NF-κB通路，从而减少细胞因子，进而抑制OVX引起的成骨减少和破骨细胞生成增加。这些发现为了解绝经后骨质疏松症的发展提供了新的思路，为干预策略提供了潜在的途径。

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

Journal of Biomedical Research MEDICINE, RESEARCH & EXPERIMENTAL-

CiteScore

4.60

自引率

0.00%

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