Jin-Ran Chen, Dongzheng Gai, Perry C Caviness, Oxana P. Lazarenko, Jennifer F. Chen, Christopher E Randolph, Zijun Zhang, Yan Cheng, Fumou Sun, Hongwei Xu, Michael Blackburn, Guido J Tricot, John D. Shaughnessy, Fenghuang Zhan
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In this study, both MM- and ovariectomy (OVX)-induced osteoporotic mouse models were used to compare the effects of recombinant mouse CST6 (rmCst6) and ZA on preventing bone loss. µCT showed that rmCst6 and ZA had similar effects on improving percent bone volume, and inhibited differentiation of non-adherent bone marrow cells into mature osteoclasts. Single-cell RNA sequencing showed that rmCst6 and not ZA treatment reduced bone marrow macrophage percentage in the MM mouse model compared to controls. Protein and mRNA arrays showed that both rmCst6 and ZA significantly inhibit OVX-induced expression of inflammatory cytokines. For OVX mice, ERα protein expression in bone was brought to sham surgery level by only rmCst6 treatments. rmCst6 significantly increased mRNA and protein levels of ERα and significantly increased total intracellular estrogen concentrations for ex vivo osteoclast precursor cell cultures. 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引用次数: 0
摘要
摘要 在多发性骨髓瘤(MM)患者中,破骨细胞分化的增加导致大多数MM患者形成溶骨性病变。双膦酸盐,如唑来膦酸(ZA),可用于改善骨吸收,但由于存在严重副作用的风险以及无法修复现有病变,因此需要新型抗骨吸收药物。此前,MM 缺乏溶骨病变与 MM 细胞分泌的半胱氨酸蛋白酶抑制剂胱抑素 M/E(CST6)水平升高密切相关。本研究使用 MM 和卵巢切除术(OVX)诱导的骨质疏松小鼠模型,比较重组小鼠 CST6(rmCst6)和 ZA 对防止骨质流失的作用。µCT显示,rmCst6和ZA对提高骨量百分比的效果相似,都能抑制非粘附骨髓细胞向成熟破骨细胞的分化。单细胞 RNA 测序显示,在 MM 小鼠模型中,与对照组相比,rmCst6 而非 ZA 治疗能降低骨髓巨噬细胞的百分比。蛋白质和 mRNA 阵列显示,rmCst6 和 ZA 都能显著抑制 OVX 诱导的炎症细胞因子的表达。rmCst6能显著提高ERα的mRNA和蛋白质水平,并能显著提高体外破骨细胞前体细胞培养物的细胞内雌激素总浓度。基于这些结果,我们得出结论:CST6 可通过增加破骨细胞前体细胞内雌激素受体的表达和细胞内雌激素浓度,抑制破骨细胞前体细胞的成熟,从而改善 MM 或 OVX 骨丢失模型。
Cystatin M/E ameliorates bone resorption through increasing osteoclastic cell estrogen influx
Abstract In multiple myeloma (MM), increased osteoclast differentiation leads to the formation of osteolytic lesions in most MM patients. Bisphosphonates, such as zoledronic acid (ZA), are used to ameliorate bone resorption, but due to risk of serious side effects as well as the lack of repair of existing lesions, novel anti-bone resorption agents are required. Previously, the absence of osteolytic lesions in MM was strongly associated with elevated levels of cystatin M/E (CST6), a cysteine protease inhibitor, secreted by MM cells. In this study, both MM- and ovariectomy (OVX)-induced osteoporotic mouse models were used to compare the effects of recombinant mouse CST6 (rmCst6) and ZA on preventing bone loss. µCT showed that rmCst6 and ZA had similar effects on improving percent bone volume, and inhibited differentiation of non-adherent bone marrow cells into mature osteoclasts. Single-cell RNA sequencing showed that rmCst6 and not ZA treatment reduced bone marrow macrophage percentage in the MM mouse model compared to controls. Protein and mRNA arrays showed that both rmCst6 and ZA significantly inhibit OVX-induced expression of inflammatory cytokines. For OVX mice, ERα protein expression in bone was brought to sham surgery level by only rmCst6 treatments. rmCst6 significantly increased mRNA and protein levels of ERα and significantly increased total intracellular estrogen concentrations for ex vivo osteoclast precursor cell cultures. Based on these results, we conclude that CST6 improves MM or OVX bone loss models by increasing the expression of estrogen receptors as well as the intracellular estrogen concentration in osteoclast precursors, inhibiting their maturation.