RelA/p65的基因失活使成年小鼠肝细胞在体内和体外对肿瘤坏死因子（TNF）诱导的凋亡敏感。

Genetic inactivation of RelA/p65 sensitizes adult mouse hepatocytes to TNF-induced apoptosis in vivo and in vitro.

作者信息

Geisler Fabian, Algül Hana, Paxian Stephan, Schmid Roland M

机构信息

Second Department of Internal Medicine, Klinikum rechts der Isar, Technical University of Munich, Munich.

出版信息

Gastroenterology. 2007 Jun;132(7):2489-503. doi: 10.1053/j.gastro.2007.03.033. Epub 2007 Mar 21.

DOI:10.1053/j.gastro.2007.03.033

PMID:17570221

Abstract

BACKGROUND & AIMS: The transcription factor nuclear factor (NF)-kappaB plays a critical role in mediating survival of hepatocytes in response to tumor necrosis factor (TNF)-alpha during development because mice deficient for the NF-kappaB subunit RelA/p65 die in utero because of TNF-induced liver apoptosis. For the adult liver, conflicting concepts exist as to whether soluble TNF can trigger apoptosis when NF-kappaB activation is impaired. By creating a mouse model in which the transactivating NF-kappaB subunit RelA/p65 can be genetically inactivated in hepatocytes using the Cre/lox system, we sought to clarify the role of NF-kappaB in TNF-mediated hepatocyte apoptosis.

METHODS

Deletion of RelA/p65 in the liver was achieved using an inducible conditional knockout system (rela(F/F)MxCre mice) or, hepatocyte-specifically, using a developmental conditional knockout system (rela(F/F)AlbCre mice).

RESULTS

Disruption of RelA/p65 rendered mice sensitive to lethal liver injury upon TNF administration. Primary RelA/p65-deficient hepatocytes showed no NF-kappaB activation and undergo rapid apoptosis after TNF treatment. In contrast, hepatocytes deficient for I kappa B-kinase beta (IKK beta), displayed residual NF-kappaB activity and consecutively only mild apoptosis in response to TNF. TNF-induced apoptosis in RelA/p65-deficient hepatocytes was accompanied by prolonged activation of c-jun activating kinase (JNK) and rapid, largely proteasome-independent elimination of the long splice form of the antiapoptotic cellular FLICE inhibitor protein (c-FLIP(L)). Gene silencing of caspase-8, caspase-inhibitors, inhibition of JNK, or administration of antioxidants inhibited apoptosis and elimination of c-FLIP(L).

CONCLUSIONS

RelA/p65 is essential for TNF-induced NF-kappaB activation in adult hepatocytes. Genetic deletion of a functional RelA/p65 sensitizes these cells to apoptosis in response to soluble TNF in vivo and in vitro.

摘要

背景与目的

转录因子核因子（NF）-κB在发育过程中介导肝细胞对肿瘤坏死因子（TNF）-α的存活反应中起关键作用，因为缺乏NF-κB亚基RelA/p65的小鼠因TNF诱导的肝脏凋亡而在子宫内死亡。对于成年肝脏，关于当NF-κB激活受损时可溶性TNF是否能触发凋亡存在相互矛盾的观点。通过创建一种小鼠模型，其中可使用Cre/lox系统在肝细胞中对具有转录激活作用的NF-κB亚基RelA/p65进行基因失活，我们试图阐明NF-κB在TNF介导的肝细胞凋亡中的作用。

方法

使用诱导性条件性敲除系统（rela(F/F)MxCre小鼠）或肝细胞特异性地使用发育性条件性敲除系统（rela(F/F)AlbCre小鼠）实现肝脏中RelA/p65的缺失。

结果

RelA/p65的破坏使小鼠在给予TNF后对致命性肝损伤敏感。原发性RelA/p65缺陷型肝细胞未显示NF-κB激活，且在TNF处理后迅速凋亡。相比之下，缺乏IκB激酶β（IKKβ）的肝细胞显示出残余的NF-κB活性，因此对TNF仅表现出轻度凋亡。RelA/p65缺陷型肝细胞中TNF诱导的凋亡伴随着c-jun激活激酶（JNK）的延长激活以及抗凋亡细胞FLICE抑制蛋白（c-FLIP(L)）长剪接形式的快速、主要不依赖蛋白酶体的消除。半胱天冬酶-8、半胱天冬酶抑制剂的基因沉默、JNK的抑制或抗氧化剂的给予可抑制凋亡和c-FLIP(L)的消除。