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@article{1492287, author = {Amruz Černá, Kateřina and Oppelt, Jan and Chochola, Václav and Musilová, Kateřina and Šeda, Václav and Pavlasová, Gabriela and Radová, Lenka and Arigoni, M. and Calogero, R.A. and Benes, V. and Trbušek, Martin and Brychtová, Yvona and Doubek, Michael and Mayer, Jiří and Pospíšilová, Šárka and Mráz, Marek}, article_location = {London}, article_number = {2}, doi = {http://dx.doi.org/10.1038/s41375-018-0230-x}, keywords = {TRANSCRIPTION FACTOR; TP53 MUTATION; EXPRESSION; RECEPTOR; LYMPHOMA; SURVIVAL; TRANSFORMATION; FLUDARABINE; PROGRESSION; REPRESSION}, language = {eng}, issn = {0887-6924}, journal = {Leukemia}, title = {MicroRNA miR-34a downregulates FOXP1 during DNA damage response to limit BCR signalling in chronic lymphocytic leukaemia B cells}, url = {https://www.nature.com/articles/s41375-018-0230-x}, volume = {33}, year = {2019} }
TY - JOUR ID - 1492287 AU - Amruz Černá, Kateřina - Oppelt, Jan - Chochola, Václav - Musilová, Kateřina - Šeda, Václav - Pavlasová, Gabriela - Radová, Lenka - Arigoni, M. - Calogero, R.A. - Benes, V. - Trbušek, Martin - Brychtová, Yvona - Doubek, Michael - Mayer, Jiří - Pospíšilová, Šárka - Mráz, Marek PY - 2019 TI - MicroRNA miR-34a downregulates FOXP1 during DNA damage response to limit BCR signalling in chronic lymphocytic leukaemia B cells JF - Leukemia VL - 33 IS - 2 SP - 403-414 EP - 403-414 PB - Nature Publishing Group SN - 08876924 KW - TRANSCRIPTION FACTOR KW - TP53 MUTATION KW - EXPRESSION KW - RECEPTOR KW - LYMPHOMA KW - SURVIVAL KW - TRANSFORMATION KW - FLUDARABINE KW - PROGRESSION KW - REPRESSION UR - https://www.nature.com/articles/s41375-018-0230-x L2 - https://www.nature.com/articles/s41375-018-0230-x N2 - The variable clinical course in chronic lymphocytic leukaemia (CLL) largely depends on p53 functionality and B-cell receptor (BCR) signalling propensity; however, it is unclear if there is any crosstalk between these pathways. We show that DNA damage response (DDR) activation leads to down-modulating the transcriptional factor FOXP1, which functions as a positive BCR signalling regulator and its high levels are associated with worse CLL prognosis. We identified microRNA (miRNA) miR-34a as the most prominently upregulated miRNA during DDR in CLL cells in vitro and in vivo during FCR therapy (fludarabine, cyclophosphamide, rituximab). MiR-34a induced by DDR activation and p53 stabilization potently represses FOXP1 expression by binding in its 3'-UTR. The low FOXP1 levels limit BCR signalling partially via derepressing BCR-inhibitory molecule CD22. We also show that low miR-34a levels can be used as a biomarker for worse response or shorter progression free survival in CLL patients treated with FCR chemoimmunotherapy, and shorter overall survival, irrespective of TP53 status. Additionally, we have developed a method for the absolute quantification of miR-34a copies and defined precise prognostic/predictive cutoffs. Overall, herein, we reveal for the first time that B cells limit their BCR signalling during DDR by down-modulating FOXP1 via DDR-p53/miR-34a axis. ER -
AMRUZ ČERNÁ, Kateřina, Jan OPPELT, Václav CHOCHOLA, Kateřina MUSILOVÁ, Václav ŠEDA, Gabriela PAVLASOVÁ, Lenka RADOVÁ, M. ARIGONI, R.A. CALOGERO, V. BENES, Martin TRBUŠEK, Yvona BRYCHTOVÁ, Michael DOUBEK, Jiří MAYER, Šárka POSPÍŠILOVÁ and Marek MRÁZ. MicroRNA miR-34a downregulates FOXP1 during DNA damage response to limit BCR signalling in chronic lymphocytic leukaemia B cells (MicroRNA miR-34a downregulates FOXP1 during DNA damage response to limit BCR signalling in chronic lymphocytic leukaemia B cells.). \textit{Leukemia}. London: Nature Publishing Group, 2019, vol.~33, No~2, p.~403-414. ISSN~0887-6924. Available from: https://dx.doi.org/10.1038/s41375-018-0230-x.
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