Article
Changes in protein expression due to deleterious mutations in the FA/BRCA pathway
Registro en:
SALLES, Daniela et al. Changes in protein expression due to deleterious mutations in the FA/BRCA pathway. Biochem. Biophys. Res. Commun, New York, v. 364, n. 4, p. 755-760, Dec. 2007.
0006-291X
10.1016/j.bbrc.2007.10.025
Autor
Salles, Daniela
Cabral, Rosa Estela Caseira
Paixão, Júlio César da
Almeida, Carlos Eduardo Bonacossa de
Seuánez, Héctor N.
Cabral-Neto, Januario Bispo
Resumen
Inherited deleterious mutations in one of the Fanconi anemia genes lead to a disease, characterized by bone marrow failure, myeloid
leukemia, and hypersensitivity to DNA damage. We identified proteins likely associated to the molecular signaling pathways involved in
DNA repair of interstrand cross-link lesions and in mechanisms of genomic stability mediated by FA/BRCA pathways. We compared
protein maps resolved by bidimensional electrophoresis and analyzed differentially expressed proteins, by mass spectrometry, between
FA complementation group C (FANCC)-deficient cells, and their ectopically corrected counterpart in physiological conditions or after
treatment with MMC. We found six differentially expressed proteins; among them, the checkpoint mediator protein MDC1 whose
expression was disrupted in FANCC/cells. The potential role of differentially expressed proteins in FA phenotype is discussed.
Materias
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