Evidence for premature aging due to oxidative stress in iPSCs from Cockayne syndrome

Andrade, Luciana Nogueira de Sousa; Nathanson, Jason L.; Yeo, Gene W.; Menck, Carlos Frederico Martins; Muotri, Alysson Renato

Artículos de revistas

Fecha

2012

Registro en:

HUMAN MOLECULAR GENETICS, OXFORD, v. 21, n. 17, supl. 1, Part 1, pp. 3825-3834, SEP 1, 2012

0964-6906

http://www.producao.usp.br/handle/BDPI/42827

10.1093/hmg/dds211

http://dx.doi.org/10.1093/hmg/dds211

http://repositorioslatinoamericanos.uchile.cl/handle/2250/1635484

Autor

Andrade, Luciana Nogueira de Sousa

Nathanson, Jason L.

Yeo, Gene W.

Menck, Carlos Frederico Martins

Muotri, Alysson Renato

Institución

Universidade de São Paulo (Brasil)

Resumen

Cockayne syndrome (CS) is a human premature aging disorder associated with neurological and developmental abnormalities, caused by mutations mainly in the CS group B gene (ERCC6). At the molecular level, CS is characterized by a deficiency in the transcription-couple DNA repair pathway. To understand the role of this molecular pathway in a pluripotent cell and the impact of CSB mutation during human cellular development, we generated induced pluripotent stem cells (iPSCs) from CSB skin fibroblasts (CSB-iPSC). Here, we showed that the lack of functional CSB does not represent a barrier to genetic reprogramming. However, iPSCs derived from CSB patients fibroblasts exhibited elevated cell death rate and higher reactive oxygen species (ROS) production. Moreover, these cellular phenotypes were accompanied by an up-regulation of TXNIP and TP53 transcriptional expression. Our findings suggest that CSB modulates cell viability in pluripotent stem cells, regulating the expression of TP53 and TXNIP and ROS production.

Materias

Mostrar el registro completo del ítem