Eltzschig Holger K, Köhler David, Eckle Tobias, Kong Tianqing, Robson Simon C, Colgan Sean P
Department of Anesthesiology and Perioperative Medicine, University of Colorado Health Sciences Center, Denver, CO, USA.
Blood. 2009 Jan 1;113(1):224-32. doi: 10.1182/blood-2008-06-165746. Epub 2008 Sep 23.
Hypoxia is common to several inflammatory diseases, where multiple cell types release adenine-nucleotides (particularly adenosine triphosphate/adenosine diphosphate). Adenosine triphosphate/adenosine diphosphate is metabolized to adenosine through a 2-step enzymatic reaction initiated by CD39 (ectonucleoside-triphosphate-diphosphohydrolase-1). Thus, extracellular adenosine becomes available to regulate multiple inflammatory endpoints. Here, we hypothesized that hypoxia transcriptionally up-regulates CD39 expression. Initial studies revealed hypoxia-dependent increases in CD39 mRNA and immunoreactivity on endothelia. Examination of the human CD39 gene promoter identified a region important in hypoxia inducibility. Multiple levels of analysis, including site-directed mutagenesis, chromatin immunoprecipitation, and inhibition by antisense, revealed a critical role for transcription-factor Sp1 in hypoxia-induction of CD39. Using a combination of cd39(-/-) mice and Sp1 small interfering RNA in in vivo cardiac ischemia models revealed Sp1-mediated induction of cardiac CD39 during myocardial ischemia. In summary, these results identify a novel Sp1-dependent regulatory pathway for CD39 and indicate the likelihood that CD39 is central to protective responses to hypoxia/ischemia.
缺氧是多种炎症性疾病的共同特征,多种细胞类型会释放腺嘌呤核苷酸(尤其是三磷酸腺苷/二磷酸腺苷)。三磷酸腺苷/二磷酸腺苷通过由CD39(外切核苷酸三磷酸二磷酸水解酶-1)启动的两步酶促反应代谢为腺苷。因此,细胞外腺苷可用于调节多个炎症终点。在此,我们假设缺氧会转录上调CD39的表达。初步研究揭示了内皮细胞上CD39 mRNA和免疫反应性的缺氧依赖性增加。对人类CD39基因启动子的检查确定了一个在缺氧诱导中起重要作用的区域。包括定点诱变、染色质免疫沉淀和反义抑制在内的多层次分析揭示了转录因子Sp1在CD39的缺氧诱导中起关键作用。在体内心脏缺血模型中使用cd39(-/-)小鼠和Sp1小干扰RNA的组合揭示了心肌缺血期间Sp1介导的心脏CD39诱导。总之,这些结果确定了一种新的Sp1依赖性CD39调节途径,并表明CD39很可能是对缺氧/缺血的保护性反应的核心。
