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首页> 美国卫生研究院文献>Biochemical Journal >Extracellular RNA is a natural cofactor for the (auto-)activation of Factor VII-activating protease (FSAP)
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Extracellular RNA is a natural cofactor for the (auto-)activation of Factor VII-activating protease (FSAP)

机译:细胞外RNA是因子(VII)激活蛋白酶(FSAP)(自)激活的天然辅因子

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FSAP (Factor VII-activating protease) is a new plasma-derived serine protease with putative dual functions in haemostasis, including activation of coagulation Factor VII and generation of urinary-type plasminogen activator (urokinase). The (auto-)activation of FSAP is facilitated by polyanionic glycosaminoglycans, such as heparin or dextran sulphate, whereas calcium ions stabilize the active form of FSAP. In the present study, extracellular RNA was identified and characterized as a novel FSAP cofactor. The conditioned medium derived from various cell types such as smooth muscle cells, endothelial cells, osteosarcoma cells or CHO (Chinese-hamster ovary) cells contained an acidic factor that initiated (auto-)activation of FSAP. RNase A, but not other hydrolytic enzymes (proteases, glycanases and DNase), abolished the FSAP cofactor activity, which was subsequently isolated by anion-exchange chromatography and unequivocally identified as RNA. In purified systems, as well as in plasma, different forms of natural RNA (rRNA, tRNA, viral RNA and artificial RNA) were able to (auto-)activate FSAP into the two-chain enzyme form. The specific binding of FSAP to RNA (but not to DNA) was shown by mobility-shift assays and UV crosslinking, thereby identifying FSAP as a new extracellular RNA-binding protein, the KD estimated to be 170–350 nM. Activation of FSAP occurred through an RNA-dependent template mechanism involving a nucleic acid size of at least 100 nt. In a purified system, natural RNA augmented the FSAP-dependent Factor VII activation several-fold (as shown by subsequent Factor Xa generation), as well as the FSAP-mediated generation of urokinase. Our results provide evidence for the first time that extracellular RNA, present at sites of cell damage or vascular injury, can serve an important as yet unrecognized cofactor function in haemostasis by inducing (auto-)activation of FSAP through a novel surface-dependent mechanism.
机译:FSAP(因子VII活化蛋白酶)是一种新的血浆来源的丝氨酸蛋白酶,具有止血双重功能,包括凝血因子VII的活化和尿型纤溶酶原激活剂(尿激酶)的产生。聚阴离子糖胺聚糖(例如肝素或硫酸葡聚糖)可促进FSAP的(自)活化,而钙离子可稳定FSAP的活性形式。在本研究中,细胞外RNA被鉴定为新型FSAP辅助因子。来自各种细胞类型的条件培养基,例如平滑肌细胞,内皮细胞,骨肉瘤细胞或CHO(中国仓鼠卵巢)细胞均含有酸性因子,可引发FSAP的(自)活化。 RNase A消除了FSAP辅酶活性,但没有其他水解酶(蛋白酶,甘氨酸酶和DNase)消除了FSAP辅酶活性,该活性随后通过阴离子交换色谱法进行了分离,并明确地鉴定为RNA。在纯化的系统以及血浆中,不同形式的天然RNA(rRNA,tRNA,病毒RNA和人工RNA)能够将FSAP(自动)活化为双链酶形式。 FSAP与RNA的特异性结合(但不与DNA结合)通过迁移率变动分析和紫外线交联来显示,从而确定FSAP是一种新的细胞外RNA结合蛋白,KD估计为170-350nM。 FSAP的激活是通过RNA依赖性模板机制实现的,该机制涉及至少100 nt的核酸。在纯化的系统中,天然RNA将FSAP依赖的VII因子活化增强了几倍(如随后的Xa因子生成所示),以及FSAP介导的尿激酶生成。我们的研究结果首次证明存在于细胞损伤或血管损伤部位的细胞外RNA可通过一种新颖的表面依赖性机制诱导FSAP的(自动)激活而在止血中起重要但尚未被认可的辅助因子功能。

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