p53 非依赖性诱导 p21 未能控制小鼠肝损伤模型中的再生和肝癌发生。

p53-Independent Induction of p21 Fails to Control Regeneration and Hepatocarcinogenesis in a Murine Liver Injury Model.

机构信息

Department of Gastroenterology, Hepatology and Endocrinology, Hannover Medical School, Hannover, Germany.

First Department of Medicine, University Hospital Schleswig-Holstein, Campus Lübeck, Lübeck, Germany.

出版信息

Cell Mol Gastroenterol Hepatol. 2021;11(5):1387-1404. doi: 10.1016/j.jcmgh.2021.01.006. Epub 2021 Jan 21.

DOI:10.1016/j.jcmgh.2021.01.006

PMID:33484913

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8024980/

Abstract

BACKGROUND & AIMS: A coordinated stress and regenerative response is important after hepatocyte damage. Here, we investigate the phenotypes that result from genetic abrogation of individual components of the checkpoint kinase 2/transformation-related protein 53 (p53)/cyclin-dependent kinase inhibitor 1A (p21) pathway in a murine model of metabolic liver injury.

METHODS

Nitisinone was reduced or withdrawn in Fah mice lacking Chk2, p53, or p21, and survival, tumor development, liver injury, and regeneration were analyzed. Partial hepatectomies were performed and mice were challenged with the Fas antibody Jo2.

RESULTS

In a model of metabolic liver injury, loss of p53, but not Chk2, impairs the oxidative stress response and aggravates liver damage, indicative of a direct p53-dependent protective effect on hepatocytes. Cell-cycle control during chronic liver injury critically depends on the presence of both p53 and its downstream effector p21. In p53-deficient hepatocytes, unchecked proliferation occurs despite a strong induction of p21, showing a complex interdependency between p21 and p53. The increased regenerative potential in the absence of p53 cannot fully compensate the surplus injury and is not sufficient to promote survival. Despite the distinct phenotypes associated with the loss of individual components of the DNA damage response, gene expression patterns are dominated by the severity of liver injury, but reflect distinct effects of p53 on proliferation and the anti-oxidative stress response.

CONCLUSIONS

Characteristic phenotypes result from the genetic abrogation of individual components of the DNA damage-response cascade in a liver injury model. The extent to which loss of gene function can be compensated, or affects injury and proliferation, is related to the level at which the cascade is interrupted. Accession numbers of repository for expression microarray data: GSE156983, GSE156263, GSE156852, and GSE156252.

摘要

背景与目的

在肝损伤后，协调的应激和再生反应非常重要。在此，我们研究了在代谢性肝损伤的小鼠模型中，通过遗传方法敲除细胞周期检验点激酶 2/转化相关蛋白 53（p53）/细胞周期依赖性激酶抑制剂 1A（p21）途径的单个成分时会产生哪些表型。

方法

在缺乏 Chk2、p53 或 p21 的 Fah 小鼠中减少或停用尼替西农，并分析其存活率、肿瘤发生、肝损伤和再生情况。进行部分肝切除术，并使用 Fas 抗体 Jo2 对小鼠进行挑战。

结果

在代谢性肝损伤模型中，缺失 p53 而非 Chk2 会损害氧化应激反应并加重肝损伤，表明 p53 对肝细胞具有直接的保护作用。慢性肝损伤期间的细胞周期控制严重依赖于 p53 及其下游效应物 p21 的存在。在 p53 缺陷的肝细胞中，尽管强烈诱导了 p21，但仍会发生不受控制的增殖，表明 p21 和 p53 之间存在复杂的相互依存关系。在缺乏 p53 的情况下，再生潜力增加，但仍不能完全代偿多余的损伤，也不足以促进存活。尽管在 DNA 损伤反应的单个成分缺失时会出现不同的表型，但基因表达模式主要受肝损伤严重程度的影响，但反映了 p53 对增殖和抗氧化应激反应的不同影响。