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RAS 通路病中的衰老:一种可能导致复杂表型的新型新因素。

Senescence in RASopathies, a possible novel contributor to a complex pathophenoype.

机构信息

Institute of Comparative Molecular Endocrinology, Ulm University, Helmholtzstr. 8/1, 89081, Ulm, Germany.

Institute of Comparative Molecular Endocrinology, Ulm University, Helmholtzstr. 8/1, 89081, Ulm, Germany.

出版信息

Mech Ageing Dev. 2021 Mar;194:111411. doi: 10.1016/j.mad.2020.111411. Epub 2020 Dec 9.

Abstract

Senescence is a biological process that induces a permanent cell cycle arrest and a specific gene expression program in response to various stressors. Following studies over the last few decades, the concept of senescence has evolved from an antiproliferative mechanism in cancer (oncogene-induced senescence) to a critical component of physiological processes associated with embryonic development, tissue regeneration, ageing and its associated diseases. In somatic cells, oncogenic mutations in RAS-MAPK pathway genes are associated with oncogene-induced senescence and cancer, while germline mutations in the same pathway are linked to a group of monogenic developmental disorders generally termed RASopathies. Here, we consider that in these disorders, senescence induction may result in opposing outcomes, a tumour protective effect and a possible contributor to a premature ageing phenotype identified in Costello syndrome, which belongs to the RASopathy group. In this review, we will highlight the role of senescence in organismal homeostasis and we will describe the current knowledge about senescence in RASopathies. Additionally, we provide a perspective on examples of experimentally characterised RASopathy mutations that, alone or in combination with various stressors, may also trigger an age-dependent chronic senescence, possibly contributing to the age-dependent worsening of RASopathy pathophenotype and the reduction of lifespan.

摘要

衰老(Senescence)是一种生物过程,它会在受到各种应激源的影响后,引发细胞周期的永久停滞和特定的基因表达程序。经过过去几十年的研究,衰老的概念已经从癌症中的一种抗增殖机制(癌基因诱导的衰老)发展为与胚胎发育、组织再生、衰老及其相关疾病相关的生理过程的关键组成部分。在体细胞中,RAS-MAPK 通路基因的致癌突变与癌基因诱导的衰老和癌症有关,而同一通路中的种系突变与一组通常称为 RAS 病的单基因发育障碍有关。在这里,我们认为在这些疾病中,衰老的诱导可能会产生相反的结果,对肿瘤具有保护作用,并可能导致 Costello 综合征(属于 RAS 病组)中鉴定出的过早衰老表型。在这篇综述中,我们将强调衰老在机体稳态中的作用,并描述 RAS 病中衰老的现有知识。此外,我们还提供了对实验中鉴定出的 RAS 病突变的看法,这些突变单独或与各种应激源结合,也可能引发与年龄相关的慢性衰老,这可能有助于 RAS 病表型的年龄相关恶化,并缩短寿命。

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