人血浆中循环微粒相关CD39家族外切核苷酸酶的特征分析
Characterization of circulating microparticle-associated CD39 family ecto-nucleotidases in human plasma.
作者信息
Jiang Z Gordon, Wu Yan, Csizmadia Eva, Feldbrügge Linda, Enjyoji Keiichi, Tigges John, Toxavidis Vasilis, Stephan Holger, Müller Christa E, McKnight C James, Moss Alan, Robson Simon C
机构信息
Division of Gastroenterology and Hepatology, Department of Medicine, Beth Israel Deaconess Medical Center, 330 Brookline Ave, Boston, MA, 02115, USA,
出版信息
Purinergic Signal. 2014 Dec;10(4):611-8. doi: 10.1007/s11302-014-9423-6. Epub 2014 Aug 28.
Phosphohydrolysis of extracellular ATP and ADP is an essential step in purinergic signaling that regulates key pathophysiological processes, such as those linked to inflammation. Classically, this reaction has been known to occur in the pericellular milieu catalyzed by membrane bound cellular ecto-nucleotidases, which can be released in the form of both soluble ecto-enzymes as well as being associated with exosomes. Circulating ecto-nucleoside triphosphate diphosphohydrolase 1 (NTPDase 1/CD39) and adenylate kinase 1 (AK1) activities have been shown to be present in plasma. However, other ecto-nucleotidases have not been characterized in depth. An in vitro ADPase assay was developed to probe the ecto-enzymes responsible for the ecto-nucleotidase activity in human platelet-free plasma, in combination with various specific biochemical inhibitors. Identities of ecto-nucleotidases were further characterized by chromatography, immunoblotting, and flow cytometry of circulating exosomes. We noted that microparticle-bound E-NTPDases and soluble AK1 constitute the highest levels of ecto-nucleotidase activity in human plasma. All four cell membrane expressed E-NTPDases are also found in circulating microparticles in human plasma, inclusive of: CD39, NTPDase 2 (CD39L1), NTPDase 3 (CD39L3), and NTPDase 8. CD39 family members and other ecto-nucleotidases are found on distinct microparticle populations. A significant proportion of the microparticle-associated ecto-nucleotidase activity is sensitive to POM6, inferring the presence of NTPDases, either -2 or/and -3. We have refined ADPase assays of human plasma from healthy volunteers and have found that CD39, NTPDases 2, 3, and 8 to be associated with circulating microparticles, whereas soluble AK1 is present in human plasma. These ecto-enzymes constitute the bulk circulating ADPase activity, suggesting a broader implication of CD39 family and other ecto-enzymes in the regulation of extracellular nucleotide metabolism.
细胞外ATP和ADP的磷酸水解是嘌呤能信号传导中的关键步骤,该信号传导调节着诸如与炎症相关的关键病理生理过程。传统上,已知这种反应发生在细胞膜结合的细胞外核苷酸酶催化的细胞周围环境中,这些酶可以以可溶性胞外酶的形式释放,也可以与外泌体相关联。循环中的外核苷三磷酸二磷酸水解酶1(NTPDase 1/CD39)和腺苷酸激酶1(AK1)活性已被证明存在于血浆中。然而,其他细胞外核苷酸酶尚未得到深入研究。我们开发了一种体外ADP酶测定法,结合各种特异性生化抑制剂,来探究负责无血小板人血浆中外核苷酸酶活性的胞外酶。通过循环外泌体的色谱分析、免疫印迹和流式细胞术进一步表征了细胞外核苷酸酶的特性。我们注意到,微粒结合的E-NTPDases和可溶性AK1构成了人血浆中最高水平的外核苷酸酶活性。人血浆中的循环微粒中也发现了所有四种细胞膜表达的E-NTPDases,包括:CD39、NTPDase 2(CD39L1)、NTPDase 3(CD39L3)和NTPDase 8。CD39家族成员和其他细胞外核苷酸酶存在于不同的微粒群体中。很大一部分与微粒相关的外核苷酸酶活性对POM6敏感,这表明存在NTPDases -2或/和-3。我们改进了健康志愿者人血浆的ADP酶测定法,发现CD39、NTPDases 2、3和8与循环微粒相关,而可溶性AK1存在于人血浆中。这些胞外酶构成了循环中主要的ADP酶活性,表明CD39家族和其他胞外酶在细胞外核苷酸代谢调节中具有更广泛的意义。
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