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利用小鼠的遗传学方法来理解Rel/NF-κB和IκB的功能:转基因和基因敲除技术

Genetic approaches in mice to understand Rel/NF-kappaB and IkappaB function: transgenics and knockouts.

作者信息

Gerondakis S, Grossmann M, Nakamura Y, Pohl T, Grumont R

机构信息

The Walter and Eliza Hall Institute of Medical Research, Post Office, The Royal Melbourne Hospital, Parkville, Victoria 3050, Australia.

出版信息

Oncogene. 1999 Nov 22;18(49):6888-95. doi: 10.1038/sj.onc.1203236.

Abstract

Rel/NF-kappaB transcription factors have been implicated in regulating a wide variety of genes important in cellular processes that include cell division, cell survival, differentiation and immunity. Here genetic models in which various Rel/NF-kappaB and IkappaB proteins have either been over-expressed or deleted in mice will be reviewed. Although expressed fairly ubiquitously, homozygous disruption of individual Rel/NF-kappaB genes generally affects the development of proper immune cell function. One exception is rela, which is essential for embryonic liver development. The disruption of genes encoding the individual subunits of the IkappaB kinase, namely IKKalpha and IKKbeta, has demonstrated that IKKbeta transmits the response to most common NF-kappaB inducing agents, whereas IKKalpha has an unexpected role in keratinocyte differentiation. Future studies will no doubt focus on the effect of multiple gene disruptions of members of this signaling pathway, on tissue-specific disruptions of these genes, and on the use of these mice as models for human diseases.

摘要

Rel/NF-κB转录因子参与调控细胞进程中多种重要基因,这些进程包括细胞分裂、细胞存活、分化及免疫。本文将综述各种Rel/NF-κB和IκB蛋白在小鼠中过表达或缺失的遗传模型。尽管Rel/NF-κB基因表达相当广泛,但单个Rel/NF-κB基因的纯合缺失通常会影响正常免疫细胞功能的发育。一个例外是RelA,它对胚胎肝脏发育至关重要。编码IκB激酶各个亚基(即IKKα和IKKβ)的基因的破坏表明,IKKβ传递对大多数常见NF-κB诱导剂的反应,而IKKα在角质形成细胞分化中具有意想不到的作用。未来的研究无疑将聚焦于该信号通路成员的多基因破坏效应、这些基因的组织特异性破坏以及将这些小鼠用作人类疾病模型的应用。

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