Radiotherapy is an important method for the treatment of malignant tumors. It can directly or indirectly lead to the formation of free radicals and DNA damage, resulting in a series of biological effects, including tumor cell death and normal tissue damage. These radiation effects are typically accompanied by the abnormal expression of sirtuin 1 (Sirt1), which deacetylates histones and non-histones. These Sirt1 substrates, including transcription factors and some catalytic enzymes, play a crucial role in anti-oxidative stress, DNA damage repair, autophagy regulation, anti-senescence, and apoptosis, which are closely related to triggering cell defense and survival in radiation-induced damage. In this article, we review the mechanisms underlying cellular responses to ionizing radiation and the role of Sirt1 in the process, with the aim of providing a theoretical basis for protection against radiation by Sirt1 as well as novel targets for developing radioprotective agents.
How to translate text using browser tools
30 August 2021
Protective Effect of Sirt1 against Radiation-Induced Damage
Haoren Qin,
Heng Zhang,
Shiwu Zhang,
Siwei Zhu,
Hui Wang
ACCESS THE FULL ARTICLE
Radiation Research
Vol. 196 • No. 6
December 2021
Vol. 196 • No. 6
December 2021