磷酸柠檬酸和磷酸柠檬酸-β-乙酯对部分半月板切除术诱导的骨关节炎的疾病修饰作用。
Disease-modifying effects of phosphocitrate and phosphocitrate-β-ethyl ester on partial meniscectomy-induced osteoarthritis.
作者信息
Sun Yubo, Haines Nikkole, Roberts Andrea, Ruffolo Michael, Mauerhan David R, Mihalko Kim L, Ingram Jane, Cox Michael, Hanley Edward N
机构信息
Department of Orthopedic Surgery, Carolinas Medical Center, PO Box 32861, Charlotte, NC, 28232, USA.
Department of Comparative Medicine, Carolinas Medical Center, PO Box 32861, Charlotte, NC, 28232, USA.
出版信息
BMC Musculoskelet Disord. 2015 Sep 30;16:270. doi: 10.1186/s12891-015-0724-x.
BACKGROUND
It is believed that phosphocitrate (PC) exerts its disease-modifying effects on osteoarthritis (OA) by inhibiting the formation of crystals. However, recent findings suggest that PC exerts its disease-modifying effect, at least in part, through a crystal-independent action. This study sought to examine the disease-modifying effects of PC and its analogue PC-β-ethyl ester (PC-E) on partial meniscectomy-induced OA and the structure-activity relationship.
METHODS
Calcification- and proliferation-inhibitory activities were examined in OA fibroblast-like synoviocytes (FLSs) culture. Disease-modifying effects were examined using Hartley guinea pigs undergoing partial meniscectomy. Cartilage degeneration was examined with Indian ink, safranin-O, and picrosirius red. Levels of matrix metalloproteinase-13 (MMP-13), ADAM metallopeptidase with thrombospondin type 1 motif 5 (ADAMTS5), chemokine (C-C motif) ligand 5 (CCL5), and cyclooxygenase-2 (Cox-2) were examined with immunostaining. The effects of PC-E and PC on gene expressions in OA FLSs were examined with microarray. Results are expressed as mean ± standard deviation and analyzed using Student's t test or Wilcoxon rank sum test.
RESULTS
PC-E was slightly less powerful than PC as a calcification inhibitor but as powerful as PC in the inhibition of OA FLSs proliferation. PC significantly inhibited cartilage degeneration in the partial meniscectomied right knee. PC-E was less powerful than PC as a disease-modifying drug, especially in the inhibition of cartilage degeneration in the non-operated left knee. PC significantly reduced the levels of ADAMTS5, MMP-13 and CCL5, whereas PC-E reduced the levels of ADAMTS5 and CCL5. Microarray analyses revealed that PC-E failed to downregulate the expression of many PC-downregulated genes classified in angiogenesis and inflammatory response.
CONCLUSIONS
PC is a disease-modifying drug for posttraumatic OA therapy. PC exerts its disease-modifying effect through two independent actions: inhibiting pathological calcification and modulating the expression of many genes implicated in OA. The β-carboxyl group of PC plays an important role in the inhibition of cartilage degeneration, little role in the inhibition of FLSs proliferation, and a moderate role in the inhibition of FLSs-mediated calcification.
背景
据信,磷酸柠檬酸(PC)通过抑制晶体形成对骨关节炎(OA)发挥疾病修饰作用。然而,最近的研究结果表明,PC至少部分地通过与晶体无关的作用发挥其疾病修饰作用。本研究旨在探讨PC及其类似物PC-β-乙酯(PC-E)对部分半月板切除术诱导的OA的疾病修饰作用及其构效关系。
方法
在OA成纤维细胞样滑膜细胞(FLS)培养中检测钙化抑制和增殖抑制活性。使用接受部分半月板切除术的Hartley豚鼠检测疾病修饰作用。用印度墨水、番红O和天狼星红检测软骨退变情况。用免疫染色法检测基质金属蛋白酶-13(MMP-13)、含血小板反应蛋白基序的解聚素金属蛋白酶5(ADAMTS5)、趋化因子(C-C基序)配体5(CCL5)和环氧合酶-2(Cox-2)的水平。用微阵列检测PC-E和PC对OA FLS中基因表达的影响。结果以平均值±标准差表示,并使用学生t检验或Wilcoxon秩和检验进行分析。
结果
作为钙化抑制剂,PC-E的效力略低于PC,但在抑制OA FLS增殖方面与PC效力相当。PC显著抑制部分半月板切除术后右膝的软骨退变。作为一种疾病修饰药物,PC-E的效力低于PC,尤其是在抑制未手术的左膝软骨退变方面。PC显著降低ADAMTS5、MMP-13和CCL5的水平,而PC-E降低ADAMTS5和CCL5的水平。微阵列分析显示,PC-E未能下调许多在血管生成和炎症反应中分类的PC下调基因的表达。
结论
PC是一种用于创伤后OA治疗的疾病修饰药物。PC通过两种独立作用发挥其疾病修饰作用:抑制病理性钙化和调节许多与OA相关的基因表达。PC的β-羧基在抑制软骨退变中起重要作用,在抑制FLS增殖中作用较小,在抑制FLS介导的钙化中起中等作用。
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