前列腺素E1通过抑制细胞凋亡对内皮祖细胞进行调控。
Regulation of endothelial progenitor cells by prostaglandin E1 via inhibition of apoptosis.
作者信息
Gensch Christoph, Clever Yvonne, Werner Christian, Hanhoun Milad, Böhm Michael, Laufs Ulrich
机构信息
Klinik für Innere Medizin III, Kardiologie, Angiologie und Internistische Intensivmedizin, Universitätsklinikum des Saarlandes, 66421 Homburg, Saar, Germany.
出版信息
J Mol Cell Cardiol. 2007 Mar;42(3):670-7. doi: 10.1016/j.yjmcc.2006.12.017. Epub 2007 Jan 9.
Bone marrow derived endothelial progenitor cells (EPC) improve endothelial function and neoangiogenesis. Prostaglandin E1 (PGE1) is used for the treatment of patients with peripheral artery disease (PAD). However, the molecular effects are only partially understood. Treatment of C57/Bl6 mice with PGE1, 10 microg/kg BW increased the number of circulating Sca-1/VEGFR-2 positive EPC in the blood compared to vehicle (122+/-7% and 119+/-6% after 10 and 20 days). EPC in the bone marrow were upregulated to 125+/-11% (10 days) and 142+/-15% (20 days). PGE1 increased DiLDL/Lectin positive spleen-derived EPC to 170+/-20% and 174+/-14% after 10 and 20 days. Treatment with PGE1 enhanced in-vivo neoangiogenesis by 2-fold (disk assay, 218+/-27%). PGE1 enhanced the SDF-1 induced migratory capacity per number of EPC to 140+/-11%, 146+/-22% and 160+/-16% after 10, 14 and 20 days. Greater migratory capacity was associated with upregulation of expression of telomere repeat-binding factor (TRF2). EPC of PGE1-treated mice were characterized by reduced apoptosis. Similarly, PGE1 prevented H(2)O(2)-induced apoptosis in cultured human EPC. The effect is mediated by PI3-kinase. The effects of PGE1 on EPC were completely prevented by co-treatment with the NO-inhibitor L-NAME, 50 mg kg(-1) p.o. Treatment with the prostaglandin I2 derivative iloprost (10 microg/kg BW, 20 days) did not alter EPC numbers or function. Physical exercise is the basis of the treatment of patients with PAD. Voluntary running increased EPC numbers in mice. Treatment with PGE1 resulted in an additional increase of Sca-1/VEGFR-2- and DiLDL/lectin positive EPC as well as migration. n=10-24 for all groups, all effects p<0.05. In summary, prostaglandin E1 increases the number of EPC in the blood and the bone marrow in mice. The effect is additive to physical exercise, depends on nitric oxide and is characterized by reduction of PI3-kinase mediated apoptosis. PGE1-mediated upregulation of EPC is associated with improved EPC function and enhanced angiogenesis.
骨髓来源的内皮祖细胞(EPC)可改善内皮功能和新生血管形成。前列腺素E1(PGE1)用于治疗外周动脉疾病(PAD)患者。然而,其分子效应仅得到部分了解。用10μg/kg体重的PGE1治疗C57/Bl6小鼠,与溶剂对照组相比,血液中循环的Sca-1/VEGFR-2阳性EPC数量增加(10天和20天后分别为122±7%和119±6%)。骨髓中的EPC上调至125±11%(10天)和142±15%(20天)。PGE1使DiLDL/凝集素阳性的脾源性EPC在10天和20天后分别增加至170±20%和174±14%。PGE1治疗使体内新生血管形成增加2倍(圆盘试验,218±27%)。PGE1使SDF-1诱导的每个EPC的迁移能力在10天、14天和20天后分别增强至140±11%。146±22%和160±16%。更大的迁移能力与端粒重复结合因子(TRF2)表达上调有关。PGE1处理小鼠的EPC凋亡减少。同样,PGE1可预防培养的人EPC中H2O2诱导的凋亡。该效应由PI3激酶介导。PGE1对EPC的作用可被50mg/kg口服的NO抑制剂L-NAME共同处理完全阻断。用前列腺素I2衍生物伊洛前列素(10μg/kg体重,20天)处理未改变EPC数量或功能。体育锻炼是PAD患者治疗的基础。自愿跑步可增加小鼠EPC数量。PGE1处理导致Sca-1/VEGFR-2和DiLDL/凝集素阳性EPC数量以及迁移进一步增加。所有组n = 10 - 24,所有效应p < 0.05。总之,前列腺素E1增加小鼠血液和骨髓中EPC的数量。该效应与体育锻炼具有叠加性,依赖于一氧化氮,其特征为减少PI3激酶介导的凋亡。PGE1介导的EPC上调与EPC功能改善和血管生成增强有关。
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