Genetic inactivation of the Fanconi anemia gene FANCC identified in the hepatocellular carcinoma cell line HuH-7 confers sensitivity towards DNA-interstrand crosslinking agents

Andreas Palagyi,Kornelia Neveling,Ursula Plinninger,Andreas Ziesch,Bianca-Sabrina Targosz,G Denk,Stephanie Ochs,Antonia Rizzani,Daniel Meier,Wolfgang E. Thasler,Helmut Hanenberg,Enrico N. De Toni,Florian Bassermann,Claus Schäfer,Burkhard Göke,Detlev Schindler,Eike Gallmeier

Genetic inactivation of the Fanconi anemia gene FANCC identified in the hepatocellular carcinoma cell line HuH-7 confers sensitivity towards DNA-interstrand crosslinking agents

2010

Andreas Palagyi
Kornelia Neveling
Ursula Plinninger
Andreas Ziesch
Bianca-Sabrina Targosz
G Denk
Stephanie Ochs
Antonia Rizzani
Daniel Meier
Wolfgang E. Thasler
Helmut Hanenberg
Enrico N. De Toni
Florian Bassermann
Claus Schäfer
Burkhard Göke
Detlev Schindler
Eike Gallmeier

Background Inactivation of the Fanconi anemia (FA) pathway through defects in one of 13 FA genes occurs at low frequency in various solid cancer entities among the general population. As FA pathway inactivation confers a distinct hypersensitivity towards DNA interstrand-crosslinking (ICL)-agents, FA defects represent rational targets for individualized therapeutic strategies. Except for pancreatic cancer, however, the prevalence of FA defects in gastrointestinal (GI) tumors has not yet been systematically explored.

Keywords:

Biology
Molecular biology
DNA Interstrand Crosslinking
Cancer research
Cancer
Pancreatic cancer
Gene silencing
Population
Fanconi anemia, complementation group C
Gene
Fanconi anemia
DNA

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