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Transcriptional modulation of cartilage-specific collagen gene expression by interferon gamma and tumour necrosis factor alpha in cultured human chondrocytes.

机译：干扰素γ和肿瘤坏死因子α在培养的人类软骨细胞中的转录调节软骨特异性胶原基因表达。

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To examine the possibility that cytokines produced in inflamed joint tissues may contribute to the loss of articular cartilage by causing inhibition of synthesis of cartilage-specific matrix macromolecules, we studied the effects of interferon gamma (IFN gamma) and tumour necrosis factor alpha (TNF alpha), alone and in combination, on the expression of the genes for types-II, -IX and -XI collagens in cultured human chondrocytes. Chondrocytes isolated from human fetal epiphyseal cartilage by sequential enzymic digestions were cultured in the presence of IFN gamma (30 pM), TNF alpha (15 pM) or a combination of suboptimal concentrations of both cytokines (1.5 pM IFN gamma plus 0.3 pM TNF alpha). IFN gamma caused a maximal decrease of 23.3-32.6% in the biosynthesis of collagen by chondrocytes. TNF alpha was a more potent inhibitor causing a 42.8-45.3% decrease at one-half the concentration of IFN gamma. A synergistic inhibitory effect of 58.2% was observed with the combination of 1.5 pM IFN gamma plus 0.3 pM TNF alpha. Electrophoretic analysis of the biosynthesized proteins showed a co-ordinate decrease in the production of the three cartilage-specific collagen types II, IX and XI. These effects were accompanied by parallel changes in the steady-state levels of their corresponding mRNAs. In vitro transcription assays showed that the collagen inhibitory effects of the cytokines occurred largely at the transcriptional level. Similar effects of the cytokines were observed on biosynthesis of types-II, -IX and -XI collagens and steady-state mRNA levels for type-II collagen by chondrocytes obtained from adult articular cartilage. These observations indicate that IFN gamma and TNF alpha can induce a synergistic inhibition of the synthesis of cartilage-specific collagens by fetal and adult human chondrocytes and suggest that these effects may contribute to the articular cartilage loss that occurs in inflammatory joint diseases.

机译：为了检查发炎的关节组织中产生的细胞因子可能通过抑制软骨特异性基质大分子合成而导致关节软骨丧失的可能性，我们研究了干扰素γ（IFN gamma）和肿瘤坏死因子α（TNF alpha）的作用。）单独或组合使用）在培养的人软骨细胞中表达II型，-IX型和-XI型胶原蛋白的基因。通过连续酶消化从人胎儿epi骨软骨分离的软骨细胞在IFNγ（30 pM），TNFα（15 pM）或两种细胞因子浓度不理想的组合下（1.5 pM IFNγ加0.3 pM TNFα）进行培养。 IFNγ导致软骨细胞生物合成胶原蛋白的最大量减少了23.3-32.6％。 TNFα是一种更强效的抑制剂，在一半的IFNγ浓度下可降低42.8-45.3％。 1.5 pM IFNγ加0.3 pM TNFα的组合观察到58.2％的协同抑制作用。生物合成蛋白质的电泳分析显示，三种特定于软骨的II型，IX型和XI型软骨的坐标降低。这些作用伴随着其相应的mRNA稳态水平的平行变化。体外转录试验表明，细胞因子的胶原蛋白抑制作用主要发生在转录水平。在成年软骨获得的软骨细胞中，观察到了细胞因子对II型，-IX和-XI型胶原蛋白的生物合成以及II型胶原蛋白的稳态mRNA水平的相似作用。这些观察结果表明，IFNγ和TNFα可以诱导胎儿和成年人软骨细胞对软骨特异性胶原蛋白的合成的协同抑制作用，并表明这些作用可能导致在炎性关节疾病中发生的关节软骨损失。

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期刊名称 Biochemical Journal
作者
A M Reginato; C Sanz-Rodriguez; A Diaz; R M Dharmavaram; S A Jimenez;
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年(卷),期 1993(294),Pt 3
年度 1993
页码 761–769
总页数 9
原文格式 PDF
正文语种
中图分类分子生物学 ;
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专利

1. Transcriptional modulation of cartilage-specific collagen gene expression by interferon γ and tumour necrosis factor α in cultured human chondrocytes [J] . A Diaz, A M Reginato, C Sanz-Rodriguez, The biochemical journal . 1993 ,第3期

机译：干扰素γ和肿瘤坏死因子α对人软骨细胞中软骨特异性胶原基因表达的转录调控
2. alpha-melanocyte-stimulating hormone modulates lipopolysaccharide plus interferon-gamma-induced tumor necrosis factor-alpha expression but not tumor necrosis factor-alpha receptor expression in cultured hypothalamic neurons. [J] . Caruso C, Sanchez M, Durand D, Journal of Neuroimmunology: Official Bulletin of the Research Committee on Neuroimmunology of the World Federation of Neurology . 2010 ,第1a2期

机译：在培养的下丘脑神经元中，α-刺激黑素细胞的激素调节脂多糖加干扰素-γ诱导的肿瘤坏死因子-α表达，但不调节肿瘤坏死因子-α受体表达。
3. Induction of interferon regulatory factor 1 expression in human dermal endothelial cells by interferon-gamma and tumor necrosis factor-alpha is transcriptionally regulated and requires iron. [J] . Gira AK, Casper KA, Otto KB, The Journal of investigative dermatology. . 2003 ,第5期

机译：干扰素-γ和肿瘤坏死因子-α诱导人皮肤内皮细胞中干扰素调节因子1的表达受到转录调节，需要铁。
4. Pravastatin and Rosiglitazone May Attenuate Coronary Artery Disease by Decreasing Interferon-gamma, Tumor Necrosis Factor-alpha, Interleukin-6, Macrophage Chemotactic Protein-1, C-Reactive Protein, and Increasing Interleukin-4 [C] . L.G. Tan, S.A. Tan, L.S. Berk International Congress on Coronary Artery Disease . 2007

机译：普伐他汀和罗格列酮可以通过减少干扰素-γ，肿瘤坏死因子-α，白细胞介素-6，巨噬细胞趋化蛋白-1，C反应蛋白和增加白细胞介素-4
5. Tumour gene therapy using adenoviral vectors expressing tumour necrosis factor alpha. [D] . Marr, Robert Anthony. 2000

机译：使用表达肿瘤坏死因子α的腺病毒载体进行肿瘤基因治疗。
6. Tumor necrosis factor-alpha and interferon-gamma suppress the activation of human type I collagen gene expression by transforming growth factor-beta 1. Evidence for two distinct mechanisms of inhibition at the transcriptional and posttranscriptional levels. [O] . V M Kähäri, Y Q Chen, M W Su, 1990

机译：肿瘤坏死因子-α和干扰素-γ通过转化生长因子-β1抑制人类I型胶原基因表达的激活。在转录和转录后水平存在两种不同抑制机制的证据。
7. Tumor necrosis factor-alpha and interferon-gamma suppress the activation of human type I collagen gene expression by transforming growth factor-beta 1. Evidence for two distinct mechanisms of inhibition at the transcriptional and posttranscriptional levels. [O] . Kähäri, V M, Chen, Y Q, Su, M W, 1990

机译：肿瘤坏死因子-α和干扰素-γ通过转化生长因子-β1抑制人类I型胶原基因表达的激活。证据表明在转录和转录后水平存在两种不同的抑制机制。
8. IL-1 and Tumor Necrosis Factor-Alpha Each Up-Regulate Both the Expression of IFN-Gamma Receptors and Enhance IFN-Gamma-Induced HLA-DR Expression on Human Monocytes and a Human Monocytic Cell Line (THP-1) [R] . Krakauer, T., Oppenheim, J. J. 1993

机译：IL-1和肿瘤坏死因子-α各自上调IFN-γ受体的表达并增强人单核细胞和人单核细胞系（THp-1）上IFN-γ诱导的HLa-DR表达

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Transcriptional modulation of cartilage-specific collagen gene expression by interferon gamma and tumour necrosis factor alpha in cultured human chondrocytes.

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