par McBride, David J;Orpana, Arto K;Sotiriou, Christos 
;Joensuu, Heikki;Stephens, Philip J;Mudie, Laura J;Hämäläinen, Eija;Stebbings, Lucy A;Andersson, Leif C;Flanagan, Adrienne M;Durbecq, Virginie ;Ignatiadis, Michail ;Kallioniemi, Olli;Heckman, Caroline A;Alitalo, Kari;Edgren, Henrik;Futreal, P Andrew;Stratton, Michael R;Campbell, Peter J
Référence Genes chromosomes & cancer, 49, 11, page (1062-1069)
Publication Publié, 2010-11
;Joensuu, Heikki;Stephens, Philip J;Mudie, Laura J;Hämäläinen, Eija;Stebbings, Lucy A;Andersson, Leif C;Flanagan, Adrienne M;Durbecq, Virginie ;Ignatiadis, Michail ;Kallioniemi, Olli;Heckman, Caroline A;Alitalo, Kari;Edgren, Henrik;Futreal, P Andrew;Stratton, Michael R;Campbell, Peter JRéférence Genes chromosomes & cancer, 49, 11, page (1062-1069)
Publication Publié, 2010-11
Article révisé par les pairs
| Résumé : | Detection of recurrent somatic rearrangements routinely allows monitoring of residual disease burden in leukemias, but is not used for most solid tumors. However, next-generation sequencing now allows rapid identification of patient-specific rearrangements in solid tumors. We mapped genomic rearrangements in three cancers and showed that PCR assays for rearrangements could detect a single copy of the tumor genome in plasma without false positives. Disease status, drug responsiveness, and incipient relapse could be serially assessed. In future, this strategy could be readily established in diagnostic laboratories, with major impact on monitoring of disease status and personalizing treatment of solid tumors. |
