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Literature DB >> 32684438

DNA Damage Response and Metabolic Reprogramming in Health and Disease.

Ourania Chatzidoukaki¹, Evi Goulielmaki¹, Björn Schumacher², George A Garinis³.

Abstract

Nuclear DNA damage contributes to cellular malfunction and the premature onset of age-related diseases, including cancer. Until recently, the canonical DNA damage response (DDR) was thought to represent a collection of nuclear processes that detect, signal and repair damaged DNA. However, recent evidence suggests that beyond nuclear events, the DDR rewires an intricate network of metabolic circuits, fine-tunes protein synthesis, trafficking, and secretion as well as balances growth with defense strategies in response to genotoxic insults. In this review, we discuss how the active DDR signaling mobilizes extranuclear and systemic responses to promote cellular homeostasis and organismal survival in health and disease.

Entities: Disease

Keywords: DNA damage; aging; cancer; disease; metabolism; stress response

Mesh：

Substances：
DNA Repair Enzymes

Year: 2020 PMID： 32684438 DOI： 10.1016/j.tig.2020.06.018

Source DB: PubMed Journal: Trends Genet ISSN： 0168-9525 Impact factor: 11.639

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Cited

13 in total

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3. The splicing factor XAB2 interacts with ERCC1-XPF and XPG for R-loop processing.

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Journal: Nat Commun Date: 2021-05-26 Impact factor: 14.919

4. R-loops trigger the release of cytoplasmic ssDNAs leading to chronic inflammation upon DNA damage.

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5. Integrated -omics approach reveals persistent DNA damage rewires lipid metabolism and histone hyperacetylation via MYS-1/Tip60.

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Review 6. Overcoming Radiation Resistance in Gliomas by Targeting Metabolism and DNA Repair Pathways.

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