Human cells compromised for p53 function exhibit defective global and transcription-coupled nucleotide excision repair, whereas cells compromised for pRb function are defective only in global repair

Proceedings of the National Academy of Sciences of the United States of America

Volumn 96, Issue 26, 1999, Pages 15038-15043

  Therrien, Jean Philippe ^a   Drouin, Régen ^a   Baril, Caroline ^b   Drobetsky, Elliot A ^b  

^a UNIVERSITÉ LAVAL   (Canada)

^b UNIVERSITÉ DE MONTRÉAL   (Canada)

Author keywords

[No Author keywords available]

Indexed keywords

ONCOPROTEIN; PHOTOPROTEIN; PROTEIN P53; PYRIMIDINE DIMER; RETINOBLASTOMA PROTEIN;

ARTICLE; CANCER INHIBITION; DNA DAMAGE; DNA REPAIR; EXCISION REPAIR; GENOTOXICITY; HUMAN; HUMAN CELL; LUNG FIBROBLAST; MALIGNANT TRANSFORMATION; PHOTOTOXICITY; POLYMERASE CHAIN REACTION; PRIORITY JOURNAL; PROTEIN EXPRESSION; SKIN FIBROBLAST; TUMOR SUPPRESSOR GENE; ULTRAVIOLET B RADIATION; VIRUS CARCINOGENESIS; WART VIRUS;

DNA REPAIR; FIBROBLASTS; HUMANS; LI-FRAUMENI SYNDROME; LUNG; ONCOGENE PROTEINS, VIRAL; PYRIMIDINE DIMERS; RETINOBLASTOMA PROTEIN; SKIN; TRANSCRIPTION, GENETIC; TUMOR SUPPRESSOR PROTEIN P53; ULTRAVIOLET RAYS;

EUKARYOTA; HUMAN PAPILLOMAVIRUS; HUMAN PAPILLOMAVIRUS TYPES;

EID: 0033592978     PISSN: 00278424     EISSN: None     Source Type: Journal    
DOI: 10.1073/pnas.96.26.15038     Document Type: Article

References (61)