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首页> 美国卫生研究院文献>Arthritis Research >Higher susceptibility to Fas ligand induced apoptosis and altered modulation of cell death by tumor necrosis factor-α in periarticular tenocytes from patients with knee joint osteoarthritis
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Higher susceptibility to Fas ligand induced apoptosis and altered modulation of cell death by tumor necrosis factor-α in periarticular tenocytes from patients with knee joint osteoarthritis

机译:Fas配体对膝关节骨关节炎患者关节周肌腱细胞中肿瘤坏死因子-α对Fas配体的敏感性较高并且改变了细胞死亡的调节

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The aim of the present study was to investigate the expression of Fas in periarticular tenocytes of patients with osteoarthritis (OA) and to study their susceptibility to Fas ligand-mediated apoptosis. Tendon samples were obtained from the quadriceps femoris muscle of patients with knee OA and used for histological evaluation, for immunohistochemical detection of Fas, and to establish tenocyte cultures. The expression of Fas mRNA was determined by quantitative PCR. Levels of soluble Fas and soluble tumour necrosis factor (TNF) receptor I were measured using ELISA. Apoptosis was induced with recombinant human Fas ligand and measured by a histone fragmentation assay and flow cytometry. The effects of TNF-α were studied by stimulation with TNF-α alone or 24 hours before the induction of apoptosis. Tendon samples from non-OA patients were used as controls. Histological evaluation revealed degenerative changes in the tendons of all OA patients but not in the controls. Fas was detected by immunohistochemistry in all specimens, but quantitative PCR revealed significantly higher levels of Fas mRNA in OA tenocytes. In contrast, lower levels of soluble Fas were found in OA tenocytes by ELISA. OA tenocytes were significantly more susceptible to Fas ligand induced apoptosis than were control cells. TNF-α reduced the Fas ligand induced apoptosis in OA tenocytes but had no effects on control tenocytes. These data suggest that knee OA is associated with higher susceptibility of periarticular tenocytes to Fas ligand induced apoptosis because of higher expression of Fas but lower levels of apoptosis-inhibiting soluble Fas. These changes may contribute to decreased cellularity in degenerative tendons and promote their rupturing. The antiapoptotic effects of TNF-α in OA tenocytes most likely reflect regenerative attempts and must be taken into account when anti-TNF strategies are considered for OA.
机译:本研究的目的是研究Fas在骨关节炎(OA)患者关节周围腱细胞中的表达,并研究其对Fas配体介导的细胞凋亡的敏感性。从膝OA患者的股四头肌获得肌腱样品,并用于组织学评估,Fas的免疫组织化学检测和建立肌腱细胞培养。通过定量PCR确定Fas mRNA的表达。使用ELISA测量可溶性Fas和可溶性肿瘤坏死因子(TNF)受体I的水平。用重组人Fas配体诱导细胞凋亡,并通过组蛋白片段化测定和流式细胞术测量。通过单独用TNF-α刺激或诱导细胞凋亡前24小时来研究TNF-α的作用。来自非OA患者的肌腱样品用作对照。组织学评估显示,所有OA患者的肌腱均出现退行性变化,而对照组则没有。通过免疫组织化学在所有标本中检测到Fas,但是定量PCR显示OA肌腱细胞中Fas mRNA的水平明显升高。相反,通过ELISA在OA肌腱细胞中发现较低水平的可溶性Fas。 OA肌腱细胞比Fas配体更易受Fas配体诱导的凋亡。 TNF-α减少了Fas配体诱导的OA肌腱细胞凋亡,但对对照肌腱细胞没有影响。这些数据表明,由于OAs的表达较高,但抑制凋亡的可溶性Fas的水平较低,因此膝OA与关节周围肌腱细胞对Fas配体诱导的凋亡的敏感性较高有关。这些变化可能导致变性肌腱细胞减少,并促进其断裂。 TNF-α在OA肌腱细胞中的抗凋亡作用很可能反映了再生尝试,在考虑针对OA的抗TNF策略时必须予以考虑。

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