Your search keyword '"Turcq, Béatrice"' showing total 28 results

1. Integrating allele-specific PCR with CRISPR-Cas13a for sensitive KRAS mutation detection in pancreatic cancer

Author

Amintas, Samuel, Cullot, Grégoire, Boubaddi, Mehdi, Rébillard, Julie, Karembe, Laura, Turcq, Béatrice, Prouzet-Mauléon, Valérie, Bedel, Aurélie, Moreau-Gaudry, François, Cappellen, David, and Dabernat, Sandrine

Published

2024

2. In vivo vulnerabilities to GPX4 and HDAC inhibitors in drug-persistent versus drug-resistant BRAFV600E lung adenocarcinoma

Author

Nokin, Marie-Julie, Darbo, Elodie, Richard, Elodie, San José, Sonia, de Hita, Sergio, Prouzet-Mauleon, Valérie, Turcq, Béatrice, Gerardelli, Laura, Crake, Rebekah, Velasco, Valérie, Koopmansch, Benjamin, Lambert, Frederic, Xue, Jenny Y., Sang, Ben, Horne, Julie, Ziemons, Eric, Villanueva, Alberto, Blomme, Arnaud, Herfs, Michael, Cataldo, Didier, Calvayrac, Olivier, Porporato, Paolo, Nadal, Ernest, Lito, Piro, Jänne, Pasi A., Ricciuti, Biagio, Awad, Mark M., Ambrogio, Chiara, and Santamaría, David

Published

2024

3. Antimetabolic cooperativity with the clinically approved l-asparaginase and tyrosine kinase inhibitors to eradicate CML stem cells

Author

Trinh, Anne, Khamari, Raeeka, Fovez, Quentin, Mahon, François-Xavier, Turcq, Béatrice, Bouscary, Didier, Maboudou, Patrice, Joncquel, Marie, Coiteux, Valérie, Germain, Nicolas, Laine, William, Dekiouk, Salim, Jean-Pierre, Sandrine, Maguer-Satta, Veronique, Ghesquiere, Bart, Idziorek, Thierry, Quesnel, Bruno, Kluza, Jerome, and Marchetti, Philippe

Published

2022

4. CRISPR Base Editing to Create Potential Charcot–Marie–Tooth Disease Models with High Editing Efficiency: Human Induced Pluripotent Stem Cell Harboring SH3TC2 Variants.

Author

Loret, Camille, Pauset, Amandine, Faye, Pierre-Antoine, Prouzet-Mauleon, Valérie, Pyromali, Ioanna, Nizou, Angélique, Miressi, Federica, Sturtz, Franck, Favreau, Frédéric, Turcq, Béatrice, and Lia, Anne-Sophie

Subjects

INDUCED pluripotent stem cells, GENOME editing, SINGLE nucleotide polymorphisms, PLURIPOTENT stem cells, CRISPRS

Abstract

Human induced pluripotent stem cells (hiPSCs) represent a powerful tool to investigate neuropathological disorders in which the cells of interest are inaccessible, such as in the Charcot–Marie–Tooth disease (CMT), the most common inherited peripheral neuropathy. Developing appropriate cellular models becomes crucial in order to both study the disease's pathophysiology and test new therapeutic approaches. The generation of hiPS cellular models for disorders caused by a single nucleotide variation has been significantly improved following the development of CRISPR-based editing tools. In this study, we efficiently and quickly generated, by CRISPR editing, the two first hiPSCs cellular models carrying alterations involved in CMT4C, also called AR-CMTde-SH3TC2. This subtype of CMT is associated with alterations in the SH3TC2 gene and represents the most prevalent form of autosomal recessive demyelinating CMT. We aimed to develop models for two different SH3TC2 nonsense variants, c.211C>T, p.Gln71* and the most common AR-CMTde-SH3TC2 alteration, c.2860C>T, p.Arg954*. First, in order to determine the best CRISPR strategy to adopt on hiPSCs, we first tested a variety of sgRNAs combined with a selection of recent base editors using the conveniently cultivable and transfectable HEK-293T cell line. The chosen CRISPR base-editing strategy was then applied to hiPSCs derived from healthy individuals to generate isogenic CMT disease models with up to 93% editing efficiency. For point mutation generation, we first recommend to test your strategies on alternative cell line such as HEK-293T before hiPSCs to evaluate a variety of sgRNA-BE combinations, thus boosting the chance of achieving edited cellular clones with the hard-to-culture and to transfect hiPSCs. [ABSTRACT FROM AUTHOR]

Published

2024

5. A new mechanism of resistance to ABL1 tyrosine kinase inhibitors in a BCR-ABL1-positive cell line

Author

Airiau, Kelly, Turcq, Béatrice, Mahon, François-Xavier, and Belloc, Francis

Published

2017

6. Novel analytical methods to interpret large sequencing data from small sample sizes

Author

Lichou, Florence, Orazio, Sébastien, Dulucq, Stéphanie, Etienne, Gabriel, Longy, Michel, Hubert, Christophe, Groppi, Alexis, Monnereau, Alain, Mahon, François-Xavier, and Turcq, Béatrice

Published

2019

7. Specific High-Sensitivity Enzymatic Reporter UnLOCKing-Mediated Detection of Oncogenic BCR::ABL1 and EGFR Rearrangements

Author

Cullot, Grégoire, primary, Amintas, Samuel, additional, Karembé, Laura, additional, Prouzet-Mauléon, Valérie, additional, Rébillard, Julie, additional, Boureau, Lisa, additional, Cappellen, David, additional, Bedel, Aurélie, additional, Moreau-Gaudry, François, additional, Dulucq, Stéphanie, additional, Dabernat, Sandrine, additional, and Turcq, Béatrice, additional

Published

2023

8. Data from Evidence that Resistance to Nilotinib May Be Due to BCR-ABL, Pgp, or Src Kinase Overexpression

Author

Mahon, François-Xavier, primary, Hayette, Sandrine, primary, Lagarde, Valérie, primary, Belloc, Francis, primary, Turcq, Béatrice, primary, Nicolini, Franck, primary, Belanger, Coralie, primary, Manley, Paul W., primary, Leroy, Cédric, primary, Etienne, Gabriel, primary, Roche, Serge, primary, and Pasquet, Jean-Max, primary

Published

2023

9. Supplementary Table 1 from Evidence that Resistance to Nilotinib May Be Due to BCR-ABL, Pgp, or Src Kinase Overexpression

Author

Mahon, François-Xavier, primary, Hayette, Sandrine, primary, Lagarde, Valérie, primary, Belloc, Francis, primary, Turcq, Béatrice, primary, Nicolini, Franck, primary, Belanger, Coralie, primary, Manley, Paul W., primary, Leroy, Cédric, primary, Etienne, Gabriel, primary, Roche, Serge, primary, and Pasquet, Jean-Max, primary

Published

2023

10. Supplementary Figure 1 from Evidence that Resistance to Nilotinib May Be Due to BCR-ABL, Pgp, or Src Kinase Overexpression

Author

Mahon, François-Xavier, primary, Hayette, Sandrine, primary, Lagarde, Valérie, primary, Belloc, Francis, primary, Turcq, Béatrice, primary, Nicolini, Franck, primary, Belanger, Coralie, primary, Manley, Paul W., primary, Leroy, Cédric, primary, Etienne, Gabriel, primary, Roche, Serge, primary, and Pasquet, Jean-Max, primary

Published

2023

11. Loss of mutL homolog-1 (MLH1) expression promotes acquisition of oncogenic and inhibitor-resistant point mutations in tyrosine kinases

Author

Springuel, Lorraine, Losdyck, Elisabeth, Saussoy, Pascale, Turcq, Béatrice, Mahon, François-Xavier, Knoops, Laurent, and Renauld, Jean-Christophe

Published

2016

12. ANTIMETABOLIC COOPERATIVITY WITH THE CLINICALLY-APPROVED L-ASPARAGINASE AND TYROSINE KINASE INHIBITORS TO ERADICATE CML STEM CELLS

Author

Trinh, Anne, primary, Khamari, Raeeka, additional, Fovez, Quentin, additional, Mahon, François-Xavier, additional, Turcq, Béatrice, additional, Bouscary, Didier, additional, Maboudou, Patrice, additional, Joncquel, Marie, additional, Coiteux, Valérie, additional, Germain, Nicolas, additional, Laine, William, additional, Dekiouk, Salim, additional, Jean-Pierre, Sandrine, additional, Maguer-Satta, Veronique, additional, Ghesquiere, Bart, additional, Idziorek, Thierry, additional, Quesnel, Bruno, additional, Kluza, Jerome, additional, and Marchetti, Philippe, additional

Published

2021

13. 3e colloque de recherche fondamentale en oncologie pédiatrique

Author

Trézéguet, Véronique, Lesjean, Sarah, Veschambre, Philippe, Auguste, Patrick, Turcq, Béatrice, Ducassou, Stéphane, Merched, Aksam, Grosset, Christophe, Biothérapies des maladies génétiques et cancers, Université Bordeaux Segalen - Bordeaux 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Actions for OnCogenesis understanding and Target Identification in ONcology (ACTION), Institut Bergonié [Bordeaux], UNICANCER-UNICANCER-Université Bordeaux Segalen - Bordeaux 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre National de la Recherche Scientifique (CNRS), and CHU Bordeaux [Bordeaux]

Subjects

[SDV]Life Sciences [q-bio], [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC]

Abstract

International audience; Contexte scientifique: Malgré des avancées majeures en oncologie depuis vingt ans, 20 % des enfants et adolescents atteints d'un cancer en France décèdent de leur maladie et parmi ceux qui survivent, beaucoup gardent pendant toute leur vie des séquelles plus ou moins invalidantes consécutives à leur traitement. C'est pourquoi en 2017, les chercheurs, cliniciens, biologistes et étudiants français travaillant dans le domaine de la recherche fondamentale et translationnelle en oncologie pédiatrique se sont organisés en réseau sous le nom de REACT4KIDS (https:// react4kids.apps-dev.io/). Ce réseau a pour objectif principal de mieux coordonner les efforts des équipes de recherche françaises (une trentaine) travaillant sur les cancers de l'enfant afin de faire émerger de nouvelles pistes thérapeutiques. Chaque année, REACT4KIDS organise un colloque afin que ces équipes puissent se rencontrer, présenter leurs travaux, partager leurs données et mettre en place de nouvelles collaborations. Cette année, ce colloque scientifique était également tourné vers l'international, avec la venue de deux conférenciers étrangers de renommée mondiale, et vers la société, avec la participation de nombreuses associations de patients et le grand public. Après la tenue des deux premiers colloques en oncologie pédiatrique au centre Léon-Bérard à Lyon, la ville de Bordeaux a été choisie pour organiser la 3 e édition de cette manifestation.

Published

2020

14. A genome-scale CRISPR knock-out screen in chronic myeloid leukemia identifies novel drug resistance mechanisms along with intrinsic apoptosis and MAPK signaling

Author

Lewis, Matthieu, Prouzet-Mauléon, Valérie, Lichou, Florence, Richard, Elodie, Iggo, Richard, Turcq, Béatrice, Mahon, François-Xavier, Laboratory of Mammary and Leukaemic Oncogenesis, INSERM U1218, Université de Bordeaux, Institut National de la Santé et de la Recherche Médicale (INSERM), Centre National de la Recherche Scientifique (CNRS), and Turcq, Beatrice

Subjects

[SDV] Life Sciences [q-bio], [SDV]Life Sciences [q-bio], ComputingMilieux_MISCELLANEOUS

Abstract

International audience

Published

2020

15. Antimetabolic cooperativity with the clinically approved kidrolase and tyrosine kinase inhibitors to eradicate cml stem cells

Author

Trinh, Anne, primary, Khamari, Raeeka, additional, Fovez, Quentin, additional, Mahon, François-Xavier, additional, Turcq, Béatrice, additional, Bouscary, Didier, additional, Maboudou, Patrice, additional, Joncquel, Marie, additional, Coiteux, Valérie, additional, Germain, Nicolas, additional, Laine, William, additional, Dekiouk, Salim, additional, Ghesquiere, Bart, additional, Idziorek, Thierry, additional, Quesnel, Bruno, additional, Kluza, Jerome, additional, and Marchetti, Philippe, additional

Published

2020

16. Inhibition of DDR1 enhances in vivo chemosensitivity in KRAS-mutant lung adenocarcinoma

Author

Nokin, Marie-Julie, primary, Darbo, Elodie, additional, Travert, Camille, additional, Drogat, Benjamin, additional, Lacouture, Aurélie, additional, San José, Sonia, additional, Cabrera, Nuria, additional, Turcq, Béatrice, additional, Prouzet-Mauleon, Valérie, additional, Falcone, Mattia, additional, Villanueva, Alberto, additional, Wang, Haiyun, additional, Herfs, Michael, additional, Mosteiro, Miguel, additional, Jänne, Pasi A., additional, Pujol, Jean-Louis, additional, Maraver, Antonio, additional, Barbacid, Mariano, additional, Nadal, Ernest, additional, Santamaría, David, additional, and Ambrogio, Chiara, additional

Published

2020

17. In vivovulnerabilities to GPX4 and HDAC inhibitors in drug-persistent versus drug-resistant BRAFV600Elung adenocarcinoma

Author

Nokin, Marie-Julie, Darbo, Elodie, Richard, Elodie, San José, Sonia, de Hita, Sergio, Prouzet-Mauleon, Valérie, Turcq, Béatrice, Gerardelli, Laura, Crake, Rebekah, Velasco, Valérie, Koopmansch, Benjamin, Lambert, Frederic, Xue, Jenny Y., Sang, Ben, Horne, Julie, Ziemons, Eric, Villanueva, Alberto, Blomme, Arnaud, Herfs, Michael, Cataldo, Didier, Calvayrac, Olivier, Porporato, Paolo, Nadal, Ernest, Lito, Piro, Jänne, Pasi A., Ricciuti, Biagio, Awad, Mark M., Ambrogio, Chiara, and Santamaría, David

Abstract

The current targeted therapy for BRAFV600E-mutant lung cancer consists of a dual blockade of RAF/MEK kinases often combining dabrafenib/trametinib (D/T). This regimen extends survival when compared to single-agent treatments, but disease progression is unavoidable. By using whole-genome CRISPR screening and RNA sequencing, we characterize the vulnerabilities of both persister and D/T-resistant cellular models. Oxidative stress together with concomitant induction of antioxidant responses is boosted by D/T treatment. However, the nature of the oxidative damage, the choice of redox detoxification systems, and the resulting therapeutic vulnerabilities display stage-specific differences. Persister cells suffer from lipid peroxidation and are sensitive to ferroptosis upon GPX4 inhibition in vivo. Biomarkers of lipid peroxidation are detected in clinical samples following D/T treatment. Acquired alterations leading to mitogen-activated protein kinase (MAPK) reactivation enhance cystine transport to boost GPX4-independent antioxidant responses. Similarly to BRAFV600E-mutant melanoma, histone deacetylase (HDAC) inhibitors decrease D/T-resistant cell viability and extend therapeutic response in vivo.

Published

2024

18. Additional file 7: of Novel analytical methods to interpret large sequencing data from small sample sizes

Author

Lichou, Florence, Orazio, Sébastien, Dulucq, Stéphanie, Etienne, Gabriel, Longy, Michel, Hubert, Christophe, Groppi, Alexis, Monnereau, Alain, François-Xavier Mahon, and Turcq, Béatrice

Abstract

File S7. Detailed manual and annotated script. (DOCX 49 kb)

Published

2019

19. Midostaurin resistance in FLT3-ITD acute myeloblastic leukemia: Fonctional genomic screening by Crispr-Cas9

Author

Fernandez, Solène, Lewis, Matthieu, Guitart, Amélie, Massara*, Layal, Fabres, Clémentine, Villacreces, Arnaud, Desplat, Vanessa, Turcq, Béatrice, Dumas, Pierre‐yves, Pasquet, Jean-Max, Vigon, Isabelle, and Vigon, Isabelle

Subjects

[SDV.MHEP.HEM] Life Sciences [q-bio]/Human health and pathology/Hematology, [SDV] Life Sciences [q-bio], [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, [SDV.CAN] Life Sciences [q-bio]/Cancer, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, ComputingMilieux_MISCELLANEOUS

Published

2019

20. The Expression of Myeloproliferative Neoplasm-Associated Calreticulin Variants Depends on the Functionality of ER-Associated Degradation

Author

Mansier, Olivier, primary, Prouzet-Mauléon, Valérie, additional, Jégou, Gwénaële, additional, Barroso, Kim, additional, Raymundo, Diana Pelizzari, additional, Chauveau, Aurélie, additional, Dumas, Pierre-Yves, additional, Lagarde, Valérie, additional, Turcq, Béatrice, additional, Pasquet, Jean-Max, additional, Viallard, Jean-François, additional, James, Chloé, additional, Praloran, Vincent, additional, Voutetakis, Konstantinos, additional, Chatziioannou, Aristotelis, additional, Mahon, François-Xavier, additional, Chevet, Eric, additional, and Lippert, Eric, additional

Published

2019

21. CRISPR-Cas9 genome editing induces megabase-scale chromosomal truncations

Author

Cullot, Grégoire, primary, Boutin, Julian, additional, Toutain, Jérôme, additional, Prat, Florence, additional, Pennamen, Perrine, additional, Rooryck, Caroline, additional, Teichmann, Martin, additional, Rousseau, Emilie, additional, Lamrissi-Garcia, Isabelle, additional, Guyonnet-Duperat, Véronique, additional, Bibeyran, Alice, additional, Lalanne, Magalie, additional, Prouzet-Mauléon, Valérie, additional, Turcq, Béatrice, additional, Ged, Cécile, additional, Blouin, Jean-Marc, additional, Richard, Emmanuel, additional, Dabernat, Sandrine, additional, Moreau-Gaudry, François, additional, and Bedel, Aurélie, additional

Published

2019

22. Dasatinib-Loaded Erythrocytes Trigger Apoptosis in Untreated Chronic Myelogenous Leukemic Cells

Author

Airiau, Kelly, Turcq, Béatrice, Bouchet, Stéphane, Laharanne, Elodie, Vial, Jean-Philippe, Etienne, Gabriel, Mahon, François-Xavier, Belloc, Francis, Université de Bordeaux (UB), Actions for OnCogenesis understanding and Target Identification in ONcology (ACTION), Institut Bergonié [Bordeaux], UNICANCER-UNICANCER-Université Bordeaux Segalen - Bordeaux 2-Institut National de la Santé et de la Recherche Médicale (INSERM), CHU Bordeaux [Bordeaux], UNICANCER, and Turcq, Beatrice

Subjects

[SDV.MHEP.HEM] Life Sciences [q-bio]/Human health and pathology/Hematology, [SDV.CAN] Life Sciences [q-bio]/Cancer, [SDV.SP.PHARMA] Life Sciences [q-bio]/Pharmaceutical sciences/Pharmacology, hemic and lymphatic diseases, [SDV.SP.PHARMA]Life Sciences [q-bio]/Pharmaceutical sciences/Pharmacology, [SDV.CAN]Life Sciences [q-bio]/Cancer, [SDV.MHEP.HEM]Life Sciences [q-bio]/Human health and pathology/Hematology

Abstract

International audience; Dasatinib is an ABL1 tyrosine kinase inhibitor (TKI) with a short in vivo plasmatic half-life but with good efficiency, which is not fully understood. We investigated the possibility that circulating erythrocytes store and then provide dasatinib to target cells. In vitro coincubation of dasatinib-treated cells with naïve leukemic cells followed by analysis of kinase inhibition, apoptosis induction, fluorescent molecule exchanges, and dasatinib dosage were performed. Cells incubated with clinically relevant concentrations of dasatinib for a short time retained, after a washout procedure, an intracellular pool of dasatinib which was transferable to naïve BCR-ABL1 expressing cells and induced their apoptosis. This was verified in total blood where the huge cellular volume of erythrocytes constituted a large reservoir of dasatinib able to induce apoptosis in naïve BCR-ABL1 cell lines and primitive chronic myeloid leukemia (CML) CD34+ cells. This dasatinib transfer necessitated a contact between donor and acceptor cells. A component exchange occurred during this contact, carrying dasatinib and other TKIs such as nilotinib or the fluorescent sunitinib. An active pool of dasatinib could be buried inside the circulating erythrocytes, out of reach of detoxifying mechanisms, but still available for target cells and thus extending the acute effect of the plasmatic pool of the drug.

Published

2018

23. Killer immunoglobulin‐like receptor genotypes and chronic myeloid leukemia outcomes after imatinib cessation for treatment‐free remission.

Author

Dumas, Pierre‐Yves, Bérard, Emilie, Bréal, Claire, Dulucq, Stéphanie, Réa, Delphine, Nicolini, Franck, Forcade, Edouard, Dufossée, Melody, Pasquet, Jean‐Max, Turcq, Béatrice, Bidet, Audrey, Milpied, Noel, Déchanet‐Merville, Julie, Lafarge, Xavier, Etienne, Gabriel, and Mahon, François‐Xavier

Subjects

CHRONIC myeloid leukemia, INNATE lymphoid cells, GENOTYPES, HEMATOLOGIC malignancies, KILLER cells

Abstract

Background: Natural Killer (NK) cells are innate lymphoid cells that can be cytotoxic toward a large panel of solid tumors and hematological malignancies including chronic myeloid leukemia (CML). Such a cytotoxicity depends on various receptors. Killer immunoglobulin‐like receptors (KIR) belong to these receptors and are involved in maturation process, then in the activation abilities of NK cells. Methods: We investigated the prognostic impact of the KIR2DL5B genotype in 240 CML patients included in two clinical trials investigating tyrosine kinase inhibitors (TKI) discontinuation: STIM and STIM2. Results: After adjustment for standard risk factors in CML, we found that the inhibitory receptor KIR2DL5B‐positive genotype was independently related to a delayed second deep molecular remission (HR 0.54, 95% CI [0.32‐0.91], P = 0.02) after TKI rechallenge but not to time to first deep molecular remission or treatment‐free remission rates. Conclusion: These results suggest that KIR2DL5B could carry a role in lymphocyte‐mediated control of leukemic residual disease control in patient with CML relapse. [ABSTRACT FROM AUTHOR]

Published

2019

24. Loss of mutL homolog-1 (MLH1) expression promotes acquisition of oncogenic and inhibitor-resistant point mutations in tyrosine kinases.

Author

UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/DDUV/MEXP - Médecine expérimentale, UCL - SSS/IREC/SLUC - Pôle St.-Luc, UCL - (SLuc) Service de biologie hématologique, UCL - (SLuc) Service d'hématologie, Springuel, Lorraine, Losdyck, Elisabeth, Saussoy, Pascale, Turcq, Béatrice, Mahon, François-Xavier, Knoops, Laurent, Renauld, Jean-Christophe, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/DDUV/MEXP - Médecine expérimentale, UCL - SSS/IREC/SLUC - Pôle St.-Luc, UCL - (SLuc) Service de biologie hématologique, UCL - (SLuc) Service d'hématologie, Springuel, Lorraine, Losdyck, Elisabeth, Saussoy, Pascale, Turcq, Béatrice, Mahon, François-Xavier, Knoops, Laurent, and Renauld, Jean-Christophe

Abstract

Genomic instability drives cancer progression by promoting genetic abnormalities that allow for the multi-step clonal selection of cells with growth advantages. We previously reported that the IL-9-dependent TS1 cell line sequentially acquired activating substitutions in JAK1 and JAK3 upon successive selections for growth factor independent and JAK inhibitor-resistant cells, suggestive of a defect in mutation avoidance mechanisms. In the first part of this paper, we discovered that the gene encoding mutL homolog-1 (MLH1), a key component of the DNA mismatch repair system, is silenced by promoter methylation in TS1 cells. By means of stable ectopic expression and RNA interference methods, we showed that the high frequencies of growth factor-independent and inhibitor-resistant cells with activating JAK mutations can be attributed to the absence of MLH1 expression. In the second part of this paper, we confirm the clinical relevance of our findings by showing that chronic myeloid leukemia relapses upon ABL-targeted therapy correlated with a lower expression of MLH1 messenger RNA. Interestingly, the mutational profile observed in our TS1 model, characterized by a strong predominance of T:A>C:G transitions, was identical to the one described in the literature for primitive cells derived from chronic myeloid leukemia patients. Taken together, our observations demonstrate for the first time a causal relationship between MLH1-deficiency and incidence of oncogenic point mutations in tyrosine kinases driving cell transformation and acquired resistance to kinase-targeted cancer therapies.

Published

2016

25. Identification of Imatinib-Sensitizing Genes in Chronic Myeloid Leukemia with a Genome-Scale Crispr Knock-out Screen

Author

Lewis, Matthieu, Prouzet-Mauleon, Valerie, Richard, Elodie, Turcq, Beatrice, Iggo, Richard, and Mahon, Francois-xavier

Published

2016

26. [3rd colloquium on fundamental research in paediatric oncology].

Author

Trézéguet V, Lesjean S, Veschambre P, Auguste P, Turcq B, Ducassou S, Merched A, and Grosset CF

Subjects

Adolescent, Bone Neoplasms, Brain Neoplasms, Child, France, Humans, Leukemia, Liver Neoplasms, Biomedical Research, Medical Oncology, Pediatrics

Published

2020

27. A genome-scale CRISPR knock-out screen in chronic myeloid leukemia identifies novel drug resistance mechanisms along with intrinsic apoptosis and MAPK signaling.

Author

Lewis M, Prouzet-Mauléon V, Lichou F, Richard E, Iggo R, Turcq B, and Mahon FX

Abstract

Understanding resistance mechanisms in cancer is of utmost importance for the discovery of novel "druggable" targets. Efficient genetic screening, now even more possible with CRISPR-Cas9 gene-editing technology, next-generation sequencing and bioinformatics, is an important tool for deciphering novel cellular processes, such as resistance to treatment in cancer. Imatinib specifically eliminates chronic myeloid leukemia (CML) cells by targeting and blocking the kinase activity of BCR-ABL1; however, resistance to treatment exists. In order to discover BCR-ABL1 independent mechanisms of imatinib resistance, we utilized the genome-scale CRISPR knock-out library to screen for imatinib-sensitizing genes in vitro on K562 cells. We revealed genes that seem essential for imatinib-induced cell death, such as proapoptotic genes (BIM, BAX) or MAPK inhibitor SPRED2. Specifically, reestablishing apoptosis in BIM knock-out (KO) cells with BH3 mimetics, or inhibiting MAPK signaling in SPRED2 KO cells with MEK inhibitors restores sensitivity to imatinib. In this work, we discovered previously identified pathways and novel pathways that modulate response to imatinib in CML cell lines, such as the implication of the Mediator complex, mRNA processing and protein ubiquitinylation. Targeting these specific genetic lesions with combinational therapy can overcome resistance phenotypes and paves the road for the use of precision oncology., (© 2020 The Authors. Cancer Medicine published by John Wiley & Sons Ltd.)

Published

2020

28. Dasatinib-Loaded Erythrocytes Trigger Apoptosis in Untreated Chronic Myelogenous Leukemic Cells: A Cellular Reservoir Participating in Dasatinib Efficiency.

Author

Airiau K, Turcq B, Bouchet S, Laharanne E, Vial JP, Etienne G, Mahon FX, and Belloc F

Abstract

Dasatinib is an ABL1 tyrosine kinase inhibitor (TKI) with a short in vivo plasmatic half-life but with good efficiency, which is not fully understood. We investigated the possibility that circulating erythrocytes store and then provide dasatinib to target cells. In vitro coincubation of dasatinib-treated cells with naïve leukemic cells followed by analysis of kinase inhibition, apoptosis induction, fluorescent molecule exchanges, and dasatinib dosage were performed. Cells incubated with clinically relevant concentrations of dasatinib for a short time retained, after a washout procedure, an intracellular pool of dasatinib which was transferable to naïve BCR-ABL1 expressing cells and induced their apoptosis. This was verified in total blood where the huge cellular volume of erythrocytes constituted a large reservoir of dasatinib able to induce apoptosis in naïve BCR-ABL1 cell lines and primitive chronic myeloid leukemia (CML) CD34+ cells. This dasatinib transfer necessitated a contact between donor and acceptor cells. A component exchange occurred during this contact, carrying dasatinib and other TKIs such as nilotinib or the fluorescent sunitinib. An active pool of dasatinib could be buried inside the circulating erythrocytes, out of reach of detoxifying mechanisms, but still available for target cells and thus extending the acute effect of the plasmatic pool of the drug., (Copyright © 2018 the Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the European Hematology Association.)

Published

2018