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Experimental Pharmacology of Glucosamine Sulfate

机译:硫酸葡萄糖胺的实验药理

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Several clinical studies demonstrated that glucosamine sulfate (GS) is effective in controlling osteoarthritis (OA), showing a structure-modifying action. However, little is known about the molecular mechanism(s) by which GS exerts such action and about the effects of GS at a tissue level on osteoarthritic cartilage and other joint structures. Here we provide mechanistic evidence suggesting that in vitro GS attenuates NF-κB activation at concentrations in the range of those observed after GS administration to volunteers and patients, thus strengthening previous findings. Furthermore, we describe the effects of GS at a tissue level on the progression of the disease in a relevant model of spontaneous OA, the STR/ort mouse. In this model, the administration of GS at human corresponding doses was associated with a significant decrease of OA scores. Histomorphometry showed that the lesion surface was also significantly decreased, while the number of viable chondrocytes within the matrix was significantly increased. GS improved the course of OA in the STR/Ort mouse, by delaying cartilage breakdown as assessed histologically and histomorphometrically.
机译:多项临床研究表明,硫酸氨基葡萄糖(GS)可有效控制骨关节炎(OA),显示出结构修饰作用。但是,关于GS发挥这种作用的分子机制以及组织水平上的GS对骨关节炎软骨和其他关节结构的影响知之甚少。在这里,我们提供了机械证据,表明体外GS可以在志愿者和患者服用GS后观察到的浓度范围内,减弱NF-κB的活化,从而加强了先前的发现。此外,我们在自发性OA的相关模型STR / ort小鼠中描述了组织水平上GS对疾病进展的影响。在该模型中,以人的相应剂量施用GS与OA得分显着降低有关。组织形态计量学显示,病变表面也显着减少,而基质内的存活软骨细胞数量显着增加。 GS通过延迟组织学和组织形态学评估的软骨破坏,改善了STR / Ort小鼠的OA进程。

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