Mao Quanfu, Gundavarapu Sravanthi, Patel Chintan, Tsai Amy, Luks Francois I, De Paepe Monique E
Department of Pathology, Women and Infants Hospital, Providence, Rhode Island 02905, USA.
Am J Respir Cell Mol Biol. 2008 Dec;39(6):717-29. doi: 10.1165/rcmb.2008-0052OC. Epub 2008 Jun 27.
The functional significance of the Fas/Fas-ligand (FasL) system in hyperoxia-induced lung injury and alveolar disruption in newborn lungs in vivo remains undetermined. To assess the role of the Fas/FasL system, we compared the effects of hyperoxia (95% O2 from birth to Postnatal Day [P]7) in Fas-deficient lpr mice and wild-type mice. Alveolar disruption was more severe in hyperoxic lpr mice than in wild-type mice. In addition, a transient alveolarization defect was noted in normoxic lpr mice. Hyperoxia induced marked up-regulation of pulmonary Fas expression in wild-type mice, as well as elevated mRNA levels of pro-apoptotic Bax, Bad, and Bak. Pulmonary apoptotic activity was similar in hyperoxic wild-type and lpr mice. In contrast, lung growth and proliferation, assessed by stereologic volumetry and Ki67 proliferation studies, were significantly higher in hyperoxic wild-type mice compared with lpr mice, suggesting the Fas/FasL system has a pro-proliferative role in hyperoxic conditions. Levels of the prosurvival MAPkinase, pERK1/2, were significantly higher in hyperoxic wild-type mice compared with lpr mice, while pAkt levels were similar. These data suggest that the primary role of the Fas/FasL system in hyperoxic newborn lungs is pro-proliferative, rather than pro-apoptotic, and likely mediated through a Fas-ERK1/2 pathway. Fas-induced proliferation and lung growth in hyperoxic newborn lungs may counteract, in part, the detrimental effects of apoptosis mediated by non-Fas pathways, such as pro-apoptotic Bax/Bcl-2 family members. The capacity of the Fas/FasL signaling pathway to mediate protective rather than destructive functions in hyperoxic newborn lungs highlights the versatility of this complex pathway.
Fas/ Fas配体(FasL)系统在新生鼠体内高氧诱导的肺损伤和肺泡破坏中的功能意义尚未明确。为了评估Fas/ FasL系统的作用,我们比较了高氧(从出生到出生后第7天给予95%氧气)对Fas缺陷型lpr小鼠和野生型小鼠的影响。高氧处理的lpr小鼠肺泡破坏比野生型小鼠更严重。此外,在常氧lpr小鼠中发现了短暂的肺泡化缺陷。高氧诱导野生型小鼠肺组织Fas表达显著上调,同时促凋亡蛋白Bax、Bad和Bak的mRNA水平升高。高氧处理的野生型小鼠和lpr小鼠的肺组织凋亡活性相似。相比之下,通过体视学体积测量和Ki67增殖研究评估,高氧处理的野生型小鼠的肺生长和增殖明显高于lpr小鼠,提示Fas/ FasL系统在高氧条件下具有促增殖作用。与lpr小鼠相比,高氧处理的野生型小鼠中促存活的丝裂原活化蛋白激酶pERK1/2水平显著升高,而pAkt水平相似。这些数据表明,Fas/ FasL系统在高氧新生鼠肺中的主要作用是促增殖,而非促凋亡,可能是通过Fas-ERK1/2途径介导的。Fas诱导的高氧新生鼠肺增殖和生长可能部分抵消了由非Fas途径介导的凋亡的有害影响,如促凋亡的Bax/Bcl-2家族成员。Fas/ FasL信号通路在高氧新生鼠肺中介导保护而非破坏功能的能力突出了这一复杂通路的多功能性。