Department of Orthopedics, Sun Yat-sen Memorial Hospital of Sun Yat-sen University, #107 West Yan Jiang Road, Guangzhou, 510120, Guangdong, China.
Department of Orthopedics, the First Affiliated Hospital of Sun Yat-sen University, #58 Zhongshan Road II, Guangzhou, 510080, Guangdong, China.
Mol Med. 2019 Aug 28;25(1):43. doi: 10.1186/s10020-019-0107-0.
The protective effect of melatonin against bone metabolism imbalance in osteoporosis (OP) induced by drugs such as retinoic acid (RA) is unclear. The aim of this study was to explore the role of melatonin in bone destruction based on a mouse model.
RA-induced OP model mice were established. To assess the effect of melatonin on these mice, micro-CT was used to characterize the trabecular structure of normal mice and those treated with RA (model), RA + low-dose melatonin (Mlt-L), RA + high-dose melatonin (Mlt-H), and RA + alendronate sodium (positive control). The shape of the trabecular bone, the length and diameter of the femoral head and the height and diameter of vertebra(L1) of each group were also measured and the number of osteoclasts was determined by Tartrate-resistant acid phosphatase (TRACP) staining. Meanwhile, the expression of alkaline phosphatase (ALP) was evaluated by immunohistochemistry assays. The differences between groups in terms of liver and kidney oxidation-related indexes and serum and urinary indicators related to bone metabolism were also analyzed. Furthermore, qRT-PCR and western blotting were used to evaluate the effect of melatonin on osteogenic and osteoclastic differentiation in MC3T3-E1 and RAW264.7 cells, respectively.
RA induction led to a decrease in the amount and density of trabecular bone, a decrease in the length and diameter of the femur and height, diameter of the vertebra (L1), a decrease in bone mass and density and the expression of ALP, and an increase in the number of osteoclasts. Melatonin treatment alleviated these effects induced by RA, increasing the amount of trabecular bone in OP mice, improving the microstructure of the femur and vertebra(L1) and increasing bone mass bone density and the expression of ALP, as well as decreasing the number of osteoclasts. Additionally, blood and urinary bone metabolism-related indicators showed that melatonin promoted bone formation and inhibited bone resorption. Determination of oxidant and antioxidant biomarkers in the livers and kidneys of the mice revealed that melatonin promoted the antioxidant level and suppressed the level of oxidant molecules in these organs. In vitro, RA promoted osteoclasts and inhibit osteogenesis by increasing oxidative stress levels in the RAW264.7 and MC3T3-E1 cells, but melatonin reversed this effect. Melatonin may, therefore, play a role in the ERK/SMAD and NF-κB pathways.
Melatonin can alleviate bone loss in RA-induced OP model mice, repair the trabecular microstructure, and promote bone formation. These effects may be related to reducing oxidation levels in vivo and vitro through the ERK/SMAD and NF-κB pathways.
褪黑素对维甲酸(RA)等药物诱导的骨质疏松症(OP)骨代谢失衡的保护作用尚不清楚。本研究旨在通过建立小鼠模型探讨褪黑素在骨破坏中的作用。
建立 RA 诱导的 OP 模型小鼠。为评估褪黑素对这些小鼠的影响,使用 micro-CT 对正常小鼠和接受 RA(模型)、RA+低剂量褪黑素(Mlt-L)、RA+高剂量褪黑素(Mlt-H)和 RA+阿仑膦酸钠(阳性对照)治疗的小鼠的小梁结构进行特征分析。还测量了每组的小梁骨形状、股骨头长度和直径以及 L1 椎体高度和直径,并通过抗酒石酸酸性磷酸酶(TRACP)染色确定破骨细胞数量。同时,通过免疫组织化学法评估碱性磷酸酶(ALP)的表达。还分析了各组肝肾功能氧化相关指标以及血清和尿液骨代谢相关指标的差异。此外,使用 qRT-PCR 和 Western blot 分别评估褪黑素对 MC3T3-E1 和 RAW264.7 细胞成骨和成骨细胞分化的影响。
RA 诱导导致小梁骨数量和密度减少,股骨长度和直径以及 L1 椎体高度、直径减小,骨量和密度降低,ALP 表达减少,破骨细胞数量增加。褪黑素治疗缓解了 RA 诱导的这些作用,增加了 OP 小鼠的小梁骨量,改善了股骨和 L1 椎体的微观结构,增加了骨量和骨密度,增加了 ALP 的表达,并减少了破骨细胞的数量。此外,血液和尿液骨代谢相关指标显示褪黑素促进骨形成并抑制骨吸收。测定小鼠肝脏和肾脏的氧化还原生物标志物表明,褪黑素促进了这些器官的抗氧化水平并抑制了氧化分子水平。在体外,RA 通过增加 RAW264.7 和 MC3T3-E1 细胞的氧化应激水平促进破骨细胞形成并抑制成骨细胞,但褪黑素逆转了这一作用。因此,褪黑素可能在 ERK/SMAD 和 NF-κB 通路中发挥作用。
褪黑素可减轻 RA 诱导的 OP 模型小鼠的骨丢失,修复小梁微观结构,并促进骨形成。这些作用可能与通过 ERK/SMAD 和 NF-κB 通路降低体内和体外的氧化水平有关。
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