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首页> 外文期刊>Tissue engineering, Part A >The protective role of the pericellular matrix in chondrocyte apoptosis.
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The protective role of the pericellular matrix in chondrocyte apoptosis.

机译:细胞周基质在软骨细胞凋亡中的保护作用。

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INTRODUCTION: This study was designed to quantify the role of the pericellular matrix (PCM) in chondrocyte apoptosis using chondrons, which are a cartilage functional unit including a chondrocyte and its associated PCM. METHODS: Chondrocytes and chondrons were enzymatically isolated from human articular cartilage and exposed to monosodium iodoacetate (MIA) and staurosporine for apoptosis induction. Chondrons were defined by the presence of type VI collagen, a basic component of the PCM. Apoptosis of chondrocytes and chondrons was measured with annexin V binding by flow cytometry and verified with terminal dUTP nick end-labeling staining. In a separate experiment, isolated chondrocytes were treated with soluble type VI collagen, before or after apoptosis induction with MIA, and cell death was measured by the activity of LDH and terminal dUTP nick end-labeling staining. RESULTS: Chondrocytes treated with MIA incurred 27% cell death, compared with 12% in chondrons. On treating with MIA, 9% of chondrocytes underwent apoptosis, compared with only 1.6% of chondrons. Similarly, staurosporine induced 13% apoptosis in chondrocytes, whereas it was 3% in chondrons. Preincubation of type VI collagen effectively prevented chondrocytes from MIA-induced cell death. After apoptosis was induced with MIA, however, treatment with type VI collagen failed to rescue chondrocytes from death. CONCLUSION: The PCM, a native microenvironment of chondrocytes, protects chondrocytes from apoptosis. Type VI collagen is a functional component of the PCM that contributes to the survival of chondrocytes.
机译:简介:本研究旨在通过使用软骨素来量化细胞周围基质(PCM)在软骨细胞凋亡中的作用,软骨素是包括软骨细胞及其相关PCM的软骨功能单元。方法:通过酶法从人关节软骨中分离软骨细胞和软骨细胞,并将其暴露于碘乙酸单钠(MIA)和星形孢菌素中诱导凋亡。软骨素是由PCM的基本成分VI型胶原蛋白定义的。用膜联蛋白V结合通过流式细胞术测量软骨细胞和软骨的凋亡,并用末端dUTP缺口末端标记染色进行验证。在单独的实验中,在用MIA诱导凋亡之前或之后,用可溶性VI型胶原处理分离的软骨细胞,并通过LDH活性和末端dUTP缺口末端标记染色来测量细胞死亡。结果:用MIA处理的软骨细胞可导致27%的细胞死亡,而在软骨细胞中则为12%。用MIA治疗时,9%的软骨细胞发生凋亡,而只有1.6%的软骨细胞凋亡。同样,星形孢菌素在软骨细胞中诱导13%的细胞凋亡,而在软骨细胞中则为3%。 VI型胶原的预温育可有效防止软骨细胞免于MIA诱导的细胞死亡。但是,用MIA诱导凋亡后,用VI型胶原进行的治疗未能使软骨细胞免于死亡。结论:PCM是软骨细胞的天然微环境,可保护软骨细胞免于凋亡。 VI型胶原蛋白是PCM的功能成分,有助于软骨细胞的存活。

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