Inhibition of the Multidrug-Resistant Phenotype by Targeting YB-1 with a Conditionally Oncolytic Adenovirus: Implications for Combinatorial Treatment Regimen with Chemotherapeutic Agents.

Mantwill, K; Köhler-Vargas, N; Bernshausen, A; Bieler, A; Lage, H; Kaszubiak, A; Surowiak, P; Dravits, T; Treiber, U; Hartung, R; Gansbacher, B; Holm, PS

doi:10.1158/0008-5472.CAN-05-2339

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2006

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Title:: Inhibition of the Multidrug-Resistant Phenotype by Targeting YB-1 with a Conditionally Oncolytic Adenovirus: Implications for Combinatorial Treatment Regimen with Chemotherapeutic Agents.
Document type:: Journal Article; Article
Author(s):: Mantwill, K; Köhler-Vargas, N; Bernshausen, A; Bieler, A; Lage, H; Kaszubiak, A; Surowiak, P; Dravits, T; Treiber, U; Hartung, R; Gansbacher, B; Holm, PS
Abstract:: Bearing in mind the limited success of available treatment modalities for the therapy of multidrug-resistant tumor cells, alternative and complementary strategies need to be developed. It is known that the transcriptional activation of genes, such as MDR1 and MRP1, which play a major role in the development of a multidrug-resistant phenotype in tumor cells, involves the Y-box protein YB-1. Thus, YB-1 is a promising target for new therapeutic approaches to defeat multidrug resistance. In addition, it has been reported previously that YB-1 is an important factor in adenoviral replication because it activates transcription from the adenoviral E2-late promoter. Here, we report that an oncolytic adenovirus, named Xvir03, expressing the viral proteins E1B55k and E4orf6, leads to nuclear translocation of YB-1 and in consequence to viral replication and cell lysis in vitro and in vivo. Moreover, we show that Xvir03 down-regulates the expression of MDR1 and MRP1, indicating that recruiting YB-1 to the adenoviral E2-late promoter for viral replication is responsible for this effect. Thus, nuclear translocation of YB-1 by Xvir03 leads to resensitization of tumor cells to cytotoxic drugs. These data reveal a link between chemotherapy and virotherapy based on the cellular transcription factor YB-1 and provide the basis for formulating a model for a novel combined therapy regimen named Mutually Synergistic Therapy. (Cancer Res 2006; 66(14): 7195-202). «
Bearing in mind the limited success of available treatment modalities for the therapy of multidrug-resistant tumor cells, alternative and complementary strategies need to be developed. It is known that the transcriptional activation of genes, such as MDR1 and MRP1, which play a major role in the development of a multidrug-resistant phenotype in tumor cells, involves the Y-box protein YB-1. Thus, YB-1 is a promising target for new therapeutic approaches to defeat multidrug resistance. In addition... »
Journal title abbreviation:: Cancer Res
Year:: 2006
Journal volume:: 66
Journal issue:: 14
Pages contribution:: 7195-202
Language:: eng
Fulltext / DOI:: doi:10.1158/0008-5472.CAN-05-2339
Pubmed ID:: http://view.ncbi.nlm.nih.gov/pubmed/16849566
Print-ISSN:: 0008-5472
TUM Institution:: Institut für Experimentelle Onkologie und Therapieforschung; Urologische Klinik und Poliklinik
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mediaTUM Gesamtbestand Einrichtungen Schools TUM School of Medicine and Health Ehemalige Einrichtungen Institut für Experimentelle Onkologie und Therapieforschung 2006

mediaTUM Gesamtbestand Einrichtungen Schools TUM School of Medicine and Health Departments Clinical Medicine Klinik und Poliklinik für Urologie (Prof. Gschwend)2006