Title of article
RAD51, genomic stability, and tumorigenesis
Author/Authors
Richardson، نويسنده , , Christine، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2005
Pages
13
From page
127
To page
139
Abstract
Genomic instability is characteristic of malignant cells, and a strong correlation exists between abnormal karyotype and tumorigenicity. Increased expression of the homologous recombination and DNA repair protein Rad51 has been reported in immortalized cell lines and multiple primary tumor cell types which could alter recombination pathways to contribute to the chromosomal rearrangements found in these cells. In addition, Rad51 participates in a complex network of interactions that includes DNA damage sensors, tumor suppressors, and cell cycle and apoptotic regulators, and mutation of many of these proteins have also been associated with tumor initiation or progression. Insights into the connection between disregulated Rad51 and malignant phenotype indicate that Rad51 is a potential target for new anti-cancer regimens including those that use siRNA technology.
Keywords
Rad51 , DNA repair , tumorigenesis , Recombination , genomic stability
Journal title
Cancer Letters
Serial Year
2005
Journal title
Cancer Letters
Record number
1807385
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