中心体扩增诱导的衰老相关的变异分泌表型构成了激活缺氧诱导因子-1α的途径

IF 8 1区医学 Q1 CELL BIOLOGY Aging Cell Pub Date : 2023-01-20 DOI:10.1111/acel.13766

Selwin K. Wu, Juliana Ariffin, Shu Chian Tay, Remigio Picone

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引用次数: 3

摘要

衰老相关分泌表型(senescence associated secretory phenotype, SASP)可以促进旁分泌入侵，同时抑制肿瘤生长，从而产生复杂的表型结果。同样，中心体扩增可以诱导增殖阻滞，但也促进肿瘤侵袭。然而，中心体扩增细胞的最终命运仍然难以捉摸。在这里，我们报道了中心体扩增诱导SASP的变体，这构成了激活旁分泌入侵的途径。中心体扩增诱导的SASP是非典型的，因为它缺乏典型的可检测DNA损伤和显著的NF-κB激活，但涉及Rac激活和活性氧的产生。因此，它诱导缺氧诱导因子1α和相关基因，包括促迁移因子如ANGPTL4。值得注意的是，细胞衰老既可以通过旁分泌信号诱导肿瘤发生，也可以通过p53诱导反过来抑制肿瘤发生。通过类比，中心体扩增诱导的SASP可能因此是在一些实验模型中额外中心体促进恶性肿瘤而在其他模型中是中性的原因之一。

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The variant senescence-associated secretory phenotype induced by centrosome amplification constitutes a pathway that activates hypoxia-inducible factor-1α

The senescence-associated secretory phenotype (SASP) can promote paracrine invasion while suppressing tumour growth, thus generating complex phenotypic outcomes. Likewise, centrosome amplification can induce proliferation arrest yet also facilitate tumour invasion. However, the eventual fate of cells with centrosome amplification remains elusive. Here, we report that centrosome amplification induces a variant of SASP, which constitutes a pathway activating paracrine invasion. The centrosome amplification-induced SASP is non-canonical as it lacks the archetypal detectable DNA damage and prominent NF-κB activation, but involves Rac activation and production of reactive oxygen species. Consequently, it induces hypoxia-inducible factor 1α and associated genes, including pro-migratory factors such as ANGPTL4. Of note, cellular senescence can either induce tumourigenesis through paracrine signalling or conversely suppress tumourigenesis through p53 induction. By analogy, centrosome amplification-induced SASP may therefore be one reason why extra centrosomes promote malignancy in some experimental models but are neutral in others.

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来源期刊

Aging Cell Biochemistry, Genetics and Molecular Biology-Cell Biology

自引率

2.60%

发文量

212

期刊介绍： Aging Cell is an Open Access journal that focuses on the core aspects of the biology of aging, encompassing the entire spectrum of geroscience. The journal's content is dedicated to publishing research that uncovers the mechanisms behind the aging process and explores the connections between aging and various age-related diseases. This journal aims to provide a comprehensive understanding of the biological underpinnings of aging and its implications for human health. The journal is widely recognized and its content is abstracted and indexed by numerous databases and services, which facilitates its accessibility and impact in the scientific community. These include: Academic Search (EBSCO Publishing) Academic Search Alumni Edition (EBSCO Publishing) Academic Search Premier (EBSCO Publishing) Biological Science Database (ProQuest) CAS: Chemical Abstracts Service (ACS) Embase (Elsevier) InfoTrac (GALE Cengage) Ingenta Select ISI Alerting Services Journal Citation Reports/Science Edition (Clarivate Analytics) MEDLINE/PubMed (NLM) Natural Science Collection (ProQuest) PubMed Dietary Supplement Subset (NLM) Science Citation Index Expanded (Clarivate Analytics) SciTech Premium Collection (ProQuest) Web of Science (Clarivate Analytics) Being indexed in these databases ensures that the research published in Aging Cell is discoverable by researchers, clinicians, and other professionals interested in the field of aging and its associated health issues. This broad coverage helps to disseminate the journal's findings and contributes to the advancement of knowledge in geroscience.