首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Molecular cloning of a murine fibronectin receptor and its expression during inflammation. Expression of VLA-5 is increased in activated peritoneal macrophages in a manner discordant from major histocompatibility complex class II
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Molecular cloning of a murine fibronectin receptor and its expression during inflammation. Expression of VLA-5 is increased in activated peritoneal macrophages in a manner discordant from major histocompatibility complex class II

机译:鼠纤连蛋白受体的分子克隆及其在炎症过程中的表达。 VLA-5的表达在活化的腹膜巨噬细胞中以与主要组织相容性复合物II类不一致的方式增加

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摘要

Human fibronectin receptor (VLA-5) alpha and beta chain probes were used to identify their mouse homologues in a thioglycollate-elicited peritoneal exudate cell cDNA library. Sequence analysis of both alpha and beta chain-related murine clones revealed approximately 90% homology to their human counterparts by both nucleotide and derived amino acid sequence comparisons. Detectable alpha chain transcripts were seen predominantly in total RNA of peritoneal macrophages. beta chain expression, however, was detected at higher levels in lung, heart, brain, and kidney, suggesting the presence of a large murine VLA family similar to the human family. Analysis of levels of expression comparing resting peritoneal macrophages with macrophages elicited using inflammatory stimuli indicated that alpha chain message and surface VLA-5 expression were significantly increased using thioglycollate or Listeria monocytogenes as stimuli to elicit cells. Interestingly, beta chain message was unaffected by these inflammatory stimuli, suggesting that VLA-5 expression is regulated by VLA-5 alpha chain message levels. These results indicate that macrophage VLA-5 expression can be modulated in vivo and may provide an important mechanism by which macrophages are recruited to or adhere to fibronectin in inflammatory foci.
机译:使用人纤连蛋白受体(VLA-5)α和β链探针在硫代乙醇酸酯诱导的腹膜渗出液cDNA文库中鉴定其小鼠同源物。通过核苷酸和衍生的氨基酸序列比较,对与α和β链相关的鼠类克隆的序列分析显示出与它们的人类对应物大约90%的同源性。主要在腹膜巨噬细胞的总RNA中发现可检测的α链转录物。但是,在肺,心脏,大脑和肾脏中检测到较高水平的β链表达,这表明存在与人类家族相似的大型鼠VLA家族。比较静息腹膜巨噬细胞和使用炎症刺激引起的巨噬细胞的表达水平分析表明,使用巯基乙酸盐或单核细胞增生李斯特菌作为刺激细胞,α链信息和表面VLA-5表达显着增加。有趣的是,β链信息不受这些炎症刺激的影响,表明VLA-5表达受VLA-5α链信息水平的调节。这些结果表明巨噬细胞VLA-5表达可以在体内被调节,并且可以提供重要的机制,通过该机制巨噬细胞被募集到或粘附在炎症灶中的纤连蛋白上。

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