Charles J Malemud, Yan Sun, Eric Pearlman, Nell M Ginley, Amad Awadallah, Bradley A Wisler, James E Dennis
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Using normal human chondrocytes, monosodium urate or recombinant tumor necrosis factor-α increased the frequency of apoptosis and activity of xanthine oxidase. However, the xanthine oxidase-specific inhibitor, febuxostat, failed to blunt this response. Monosodium urate, tumor necrosis factor-α or the Janus kinase inhibitor, AG-490, increased the frequency of apoptotic nuclei in macroaggregate pellet cultures initiated from juvenile human chondrocytes, but not in pellet cultures derived from mesenchymal stem cells. In OA chondrocytes, activation of p38, C-Jun-NH<sub>2</sub>-kinase and signal transducer and activator of transcription-3 preceded apoptosis. Activation of signal transducer and activator of transcription-3 also was seen in pellet cultures initiated from juvenile chondrocytes and MSCs incubated with MSU, recombinant tumor necrosis factor-α or febuxostat, but apoptosis was increased only in the pellet cultures derived from juvenile chondrocytes. 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引用次数: 35
摘要
尿酸钠和肿瘤坏死因子-α是两种不同炎症反应途径的有效介质,在关节炎关节中,炎症可能伴随着软骨细胞凋亡而丧失活力。为了在体外解决这种可能性,采用软骨细胞培养来确定尿酸钠和重组TNF-α改变软骨细胞凋亡频率的程度。我们还研究了凋亡在p38激酶、c - jun末端激酶、转录-3信号转导和激活因子和/或黄嘌呤氧化酶活性中的作用。用正常人软骨细胞,尿酸钠或重组肿瘤坏死因子-α增加细胞凋亡频率和黄嘌呤氧化酶活性。然而,黄嘌呤氧化酶特异性抑制剂非布司他未能减弱这种反应。尿酸钠、肿瘤坏死因子-α或Janus激酶抑制剂AG-490在幼年人软骨细胞培养的大聚集颗粒中增加凋亡核的频率,但在间充质干细胞培养的颗粒中没有增加凋亡核的频率。在OA软骨细胞中,p38、c - jun - nh2激酶和信号转导及转录激活因子-3的激活在细胞凋亡之前发生。在幼年软骨细胞和MSCs与MSU、重组肿瘤坏死因子-α或非布司他孵育的颗粒培养中,信号换能器和转录激活因子-3也被激活,但凋亡仅在幼年软骨细胞培养的颗粒培养中增加。虽然AG-490或AG-490与非布司他联合抑制信号转导和转录-3激活因子的激活,但细胞凋亡不受影响。结果表明,重组肿瘤坏死因子-α、尿酸钠和AG-490增加了正常人软骨细胞、OA软骨细胞和人幼年软骨细胞颗粒的凋亡,但在MSCs培养的软骨细胞颗粒中没有增加凋亡。重组肿瘤坏死因子-α或尿酸钠对软骨细胞凋亡频率的影响不依赖于STAT3的激活或XO的活性。
Monosodium Urate and Tumor Necrosis Factor-α Increase Apoptosis in Human Chondrocyte Cultures.
Monosodium urate and tumor necrosis factor-α, are two potent mediators of separate inflammatory response pathways in arthritic joints where inflammation may be accompanied by the loss of chondrocyte vitality via apoptosis. To address this possibility in vitro, chondrocyte cultures were employed to determine the extent to which monosodium urate and recombinant TNF-α altered the frequency of apoptotic chondrocytes. Apoptosis as a function of the activation of p38 kinase, C-Jun-terminal kinase, signal transducer and activator of transcription-3 and/or the activity of xanthine oxidase was also studied. Using normal human chondrocytes, monosodium urate or recombinant tumor necrosis factor-α increased the frequency of apoptosis and activity of xanthine oxidase. However, the xanthine oxidase-specific inhibitor, febuxostat, failed to blunt this response. Monosodium urate, tumor necrosis factor-α or the Janus kinase inhibitor, AG-490, increased the frequency of apoptotic nuclei in macroaggregate pellet cultures initiated from juvenile human chondrocytes, but not in pellet cultures derived from mesenchymal stem cells. In OA chondrocytes, activation of p38, C-Jun-NH2-kinase and signal transducer and activator of transcription-3 preceded apoptosis. Activation of signal transducer and activator of transcription-3 also was seen in pellet cultures initiated from juvenile chondrocytes and MSCs incubated with MSU, recombinant tumor necrosis factor-α or febuxostat, but apoptosis was increased only in the pellet cultures derived from juvenile chondrocytes. Although AG-490 or the combination of AG-490 and febuxostat inhibited signal transducer and activator of transcription-3 activation, apoptosis was unaffected. These results showed that recombinant tumor necrosis factor-α, monosodium urate and AG-490 increased apoptosis in normal human chondrocytes, OA chondrocytes and human juvenile chondrocyte pellet cultures, but not in chondrocyte pellet cultures initiated from MSCs. The increased frequency of apoptotic chondrocytes in response to recombinant tumor necrosis factor-α or monosodium urate was not dependent on either activation of STAT3 or the activity of XO.
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