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   1. <dc:title>β-Catenin activity induces an RNA biosynthesis program promoting therapy resistance in T-cell acute lymphoblastic leukemia</dc:title>

   2. <dc:creator>García Hernández, Violeta</dc:creator>

   3. <dc:creator>Arambilet, David</dc:creator>

   4. <dc:creator>Guillén, Yolanda</dc:creator>

   5. <dc:creator>Lobo-Jarne, Teresa</dc:creator>

   6. <dc:creator>Maqueda, Maria</dc:creator>

   7. <dc:creator>Gekas, Christos</dc:creator>

   8. <dc:creator>González, Jessica</dc:creator>

   9. <dc:creator>Iglesias, Arnau</dc:creator>

   10. <dc:creator>Vega García, Nerea</dc:creator>

   11. <dc:creator>Sentís Carreras, Inés 1990-</dc:creator>

   12. <dc:creator>Trincado Alonso, Juan Luis, 1987-</dc:creator>

   13. <dc:creator>Márquez-López, Ian</dc:creator>

   14. <dc:creator>Heyn, Holger</dc:creator>

   15. <dc:creator>Camós, Mireia</dc:creator>

   16. <dc:creator>Espinosa Blay, Lluís</dc:creator>

   17. <dc:creator>Bigas Salvans, Anna</dc:creator>

   18. <dc:subject>Kaiso</dc:subject>

   19. <dc:subject>RNA processing</dc:subject>

   20. <dc:subject>T-ALL</dc:subject>

   21. <dc:subject>Chemotherapy resistance</dc:subject>

   22. <dc:subject>β-catenin</dc:subject>

   23. <dc:description>Understanding the molecular mechanisms that contribute to the appearance of chemotherapy resistant cell populations is necessary to improve cancer treatment. We have now investigated the role of β-catenin/CTNNB1 in the evolution of T-cell Acute Lymphoblastic Leukemia (T-ALL) patients and its involvement in therapy resistance. We have identified a specific gene signature that is directly regulated by β-catenin, TCF/LEF factors and ZBTB33/Kaiso in T-ALL cell lines, which is highly and significantly represented in five out of six refractory patients from a cohort of 40 children with T-ALL. By subsequent refinement of this gene signature, we found that a subset of β-catenin target genes involved with RNA-processing function are sufficient to segregate T-ALL refractory patients in three independent cohorts. We demonstrate the implication of β-catenin in RNA and protein synthesis in T-ALL and provide in vitro and in vivo experimental evidence that β-catenin is crucial for the cellular response to chemotherapy, mainly in the cellular recovery phase after treatment. We propose that combination treatments involving chemotherapy plus β-catenin inhibitors will enhance chemotherapy response and prevent disease relapse in T-ALL patients.</dc:description>

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