Publication date: Available online 13 December 2018
Source: Free Radical Biology and Medicine
Author(s): Natália Cestari Moreno, Camila Carrião Machado Garcia, Veridiana Munford, Clarissa Ribeiro Reily Rocha, Alessandra Luiza Pelegrini, Camila Corradi, Alain Sarasin, Carlos Frederico Martins Menck
Abstract
The UVA component of sunlight induces DNA damage, which are basically responsible for skin cancer formation. Xeroderma Pigmentosum Variant (XP-V) patients are defective in the DNA polymerase pol eta that promotes translesion synthesis after sunlight-induced DNA damage, implying in a clinical phenotype of increased frequency of skin cancer. However, the role of UVA-light in the carcinogenesis of these patients is not completely understood. The goal of this work was to characterize UVA-induced DNA damage and the consequences to XP-V cells, compared to complemented cells. DNA damage were induced in both cells by UVA, but lesion removal was particularly affected in XP-V cells, possibly due to the oxidation of DNA repair proteins, as indicated by the increase of carbonylated proteins. Moreover, UVA irradiation promoted replication fork stalling and cell cycle arrest in the S-phase for XP-V cells. Interestingly, when cells were treated with the antioxidant N-acetylcysteine, all these deleterious effects were consistently reverted, revealing the role of oxidative stress in these processes. Together, these results strongly indicate the crucial role of oxidative stress in UVA-induced cytotoxicity and are of interest for the protection of XP-V patients.
Graphical abstract
from ! Human Diseases via Alexandros G.Sfakianakis on Inoreader https://ift.tt/2UJb5XE
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