Guo Deliang, Chien Shu, Shyy John Y-J
Division of Biomedical Sciences, University of California, Riverside, CA 92521-0121, USA.
Circ Res. 2007 Mar 2;100(4):564-71. doi: 10.1161/01.RES.0000259561.23876.c5. Epub 2007 Feb 1.
Steady laminar flow in the straight parts of the arterial tree is atheroprotective, whereas disturbed flow with oscillation in branch points and the aortic root are athero-prone, in part, because of the distinct roles of the flow patterns in regulating the cell cycle of vascular endothelial cells (ECs). To elucidate the molecular basis underlying the endothelial cell cycle regulated by distinct flow patterns, we conducted flow-channel experiments to investigate the effects of laminar versus oscillatory flows on activation of AMP-activated protein kinase (AMPK) and Akt in ECs. Laminar flow caused a transient activation of both AMPK and Akt, but oscillatory flow activated only Akt, with AMPK being maintained at its basal level. Constitutively active and dominant-negative mutants of AMPK and Akt were used to elucidate further the positive effect of Akt and negative role of AMPK in mediating mTOR (mammalian target of rapamycin) and its target p70S6 kinase (S6K) in response to laminar and oscillatory flows. Measurements of phosphorylation of mTOR Ser2448 and S6K Thr389 showed that AMPK, by counteracting Akt under laminar flow, resulted in a transient activation of S6K. Under oscillatory flow, because of the lack of AMPK activation to effect negative regulation, S6K was activated in a sustained manner. As a functional consequence, AMPK activation attenuated cell cycle progression in response to both laminar and oscillatory flows. In contrast, AMPK inhibition promoted EC cycle progression by decreasing the cell population in the G(0)/G(1) phase and increasing it in the S+G(2)/M phase. In vivo, phosphorylation of the promitotic S6K in mouse thoracic aorta was much less than that in mouse aortic root. In contrast, AMPK phosphorylation was higher in the thoracic aorta. These results provide a molecular mechanism by which laminar versus oscillatory flow regulates the endothelial cell cycle.
动脉树直管部分的稳定层流具有抗动脉粥样硬化作用,而分支点和主动脉根部的紊乱流动及振荡则易引发动脉粥样硬化,部分原因是流动模式在调节血管内皮细胞(ECs)细胞周期中具有不同作用。为阐明不同流动模式调节内皮细胞周期的分子基础,我们进行了流动通道实验,以研究层流与振荡流对ECs中AMP激活蛋白激酶(AMPK)和Akt激活的影响。层流导致AMPK和Akt瞬时激活,但振荡流仅激活Akt,AMPK维持在基础水平。使用AMPK和Akt的组成型激活和显性负性突变体进一步阐明Akt的正向作用和AMPK在介导雷帕霉素哺乳动物靶标(mTOR)及其靶标p70S6激酶(S6K)对层流和振荡流反应中的负向作用。对mTOR Ser2448和S6K Thr389磷酸化的测量表明,在层流条件下,AMPK通过拮抗Akt导致S6K瞬时激活。在振荡流条件下,由于缺乏AMPK激活以实现负调节,S6K持续激活。作为功能结果,AMPK激活减弱了对层流和振荡流的细胞周期进程。相反,AMPK抑制通过减少G(0)/G(1)期细胞数量并增加S+G(2)/M期细胞数量来促进EC周期进程。在体内,小鼠胸主动脉中促有丝分裂S6K的磷酸化远低于小鼠主动脉根部。相反,胸主动脉中AMPK磷酸化更高。这些结果提供了一种分子机制,通过该机制层流与振荡流调节内皮细胞周期。
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