Your search keyword '"REDAELLI, SARA"' showing total 17 results

1. Novel targeted therapeutics for MEN2.

Author

Redaelli, Sara, Plaza-Menacho, Ivan, and Mologni, Luca

Subjects

*MULTIPLE endocrine neoplasia, *GENE transfection, *PROTO-oncogenes, *KINASE inhibitors, *CELLULAR signal transduction, *THERAPEUTICS

Abstract

The rearranged during transfection (RET) proto-oncogene was recognized as the multiple endocrine neoplasia type 2 (MEN2) causing gene in 1993. Since then, much effort has been put into a clear understanding of its oncogenic signaling, its biochemical function and ways to block its aberrant activation in MEN2 and related cancers. Several small molecules have been designed, developed or redirected as RET inhibitors for the treatment of MEN2 and sporadic MTC. However, current drugs are mostly active against several other kinases, as they were not originally developed for RET. This limits efficacy and poses safety issues. Therefore, there is still much to do to improve targeted MEN2 treatments. New, more potent and selective molecules, or combinatorial strategies may lead to more effective therapies in the near future. Here, we review the rationale for RET targeting in MEN2, the use of currently available drugs and novel preclinical and clinical RET inhibitor candidates. [ABSTRACT FROM AUTHOR]

Published

2018

2. In vitro and in vivo identification of ABCB1 as an efflux transporter of bosutinib.

Author

Redaelli, Sara, Perini, Pietro, Ceccon, Monica, Piazza, Rocco, Rigolio, Roberta, Mauri, Mario, Boschelli, Frank, Giannoudis, Athina, and Gambacorti-Passerini, Carlo

Subjects

*LEUKEMIA treatment, *MYELOID leukemia, *PROTEIN-tyrosine kinases, *DRUG resistance, *CELL proliferation, *VERAPAMIL

Abstract

Background: Bosutinib is a recently approved ABL inhibitor. In spite of the well-documented effectiveness of BCR-ABL inhibitors in treating chronic myeloid leukemia, development of resistance is a continuous clinical challenge. Transporters that facilitate drug uptake and efflux have been proposed as one potential source of resistance to tyrosine kinase inhibitor treatment. Our aim was to determine which carriers are responsible for bosutinib transport. Methods: K562S cells overexpressing the drug transporters ABCB1, ABCG2, and SLC22A1 were generated, characterized and used in proliferation assay and intracellular uptake and retention assay (IUR). In vivo experiments were performed in nude mice injected with K562S, K562DOX cells (overexpressing ABCB1), and K562DOX silenced for ABCB1 (K562DOX/sh P-GP). Results: The IUR assay using C-14 bosutinib showed that only ABCB1 was responsible for active bosutinib transport. K562DOX cells showed the lowest intracellular level of bosutinib, while K562DOX cells treated with the ABCB1 inhibitor verapamil showed intracellular bosutinib levels comparable with parental K562S. Proliferation assays demonstrated that K562DOX are resistant to bosutinib treatment while verapamil is able to restore the sensitivity to the drug. Nude mice injected with K562DOX and treated with bosutinib showed very limited response and quickly relapsed after stopping treatment while K562S as well as K562DOX/sh P-GP remained tumor-free. Conclusions: Our data suggest that the analysis of ABCB1 expression levels might help determine treatment options for patients exhibiting resistance to bosutinib. [ABSTRACT FROM AUTHOR]

Published

2015

3. In vitro and in vivo identification of ABCB1 as an efflux transporter of bosutinib

Author

Redaelli, Sara, Perini, Pietro, Ceccon, Monica, Piazza, Rocco, Rigolio, Roberta, Mauri, Mario, Boschelli, Frank, Giannoudis, Athina, and Gambacorti-Passerini, Carlo

Abstract

Background: Bosutinib is a recently approved ABL inhibitor. In spite of the well-documented effectiveness of BCR-ABL inhibitors in treating chronic myeloid leukemia, development of resistance is a continuous clinical challenge. Transporters that facilitate drug uptake and efflux have been proposed as one potential source of resistance to tyrosine kinase inhibitor treatment. Our aim was to determine which carriers are responsible for bosutinib transport. Methods: K562S cells overexpressing the drug transporters ABCB1, ABCG2, and SLC22A1 were generated, characterized and used in proliferation assay and intracellular uptake and retention assay (IUR). In vivo experiments were performed in nude mice injected with K562S, K562DOX cells (overexpressing ABCB1), and K562DOX silenced for ABCB1 (K562DOX/sh P-GP). Results: The IUR assay using C-14 bosutinib showed that only ABCB1 was responsible for active bosutinib transport. K562DOX cells showed the lowest intracellular level of bosutinib, while K562DOX cells treated with the ABCB1 inhibitor verapamil showed intracellular bosutinib levels comparable with parental K562S. Proliferation assays demonstrated that K562DOX are resistant to bosutinib treatment while verapamil is able to restore the sensitivity to the drug. Nude mice injected with K562DOX and treated with bosutinib showed very limited response and quickly relapsed after stopping treatment while K562S as well as K562DOX/sh P-GP remained tumor-free. Conclusions: Our data suggest that the analysis of ABCB1 expression levels might help determine treatment options for patients exhibiting resistance to bosutinib. [ABSTRACT FROM AUTHOR]

Published

2015

4. Ponatinib is a potent inhibitor of wild-type and drug-resistant gatekeeper mutant RET kinase.

Author

Mologni, Luca, Redaelli, Sara, Morandi, Andrea, Plaza-Menacho, Ivan, and Gambacorti-Passerini, Carlo

Subjects

*KINASE inhibitors, *ORAL medicine, *DRUG resistance, *DRUG approval, *GENETIC mutation

Abstract

Highlights: [•] We show potent inhibition of RET kinase by ponatinib, including gatekeeper-mutant RET. [•] Ponatinib is more potent than FDA-approved vandetanib against RET and overcomes vandetanib-resistant mutant RET. [•] We conclude from our study that ponatinib should be considered as a potential therapeutic option for MEN2 patients. [Copyright &y& Elsevier]

Published

2013

5. Regional Blood Acidification Enhances Extracorporeal Carbon Dioxide Removal: A 48-hour Animal Study.

Author

Zanella, Alberto, Mangili, Paolo, Redaelli, Sara, Scaravilli, Vittorio, Giani, Marco, Ferlicca, Daniela, Scaccabarozzi, Diletta, Pirrone, Federica, Albertini, Mariangela, Patroniti, Nicolò, and Pesenti, Antonio

Abstract

BACKGROUND: Extracorporeal carbon dioxide removal has been proposed to achieve protective ventilation in patients at risk for ventilator-induced lung injury. In an acute study, the authors previously described an extracorporeal carbon dioxide removal technique enhanced by regional extracorporeal blood acidification. The current study evaluates efficacy and feasibility of such technology applied for 48 h. METHODS: Ten pigs were connected to a low-flow veno-venous extracorporeal circuit (blood flow rate, 0.25 l/min) including a membrane lung. Blood acidification was achieved in eight pigs by continuous infusion of 2.5 mEq/min of lactic acid at the membrane lung inlet. The acid infusion was interrupted for 1 h at the 24 and 48 h. Two control pigs did not receive acidification. At baseline and every 8 h thereafter, the authors measured blood lactate, gases, chemistry, and the amount of carbon dioxide removed by the membrane lung (VCO2ML). The authors also measured erythrocyte metabolites and selected cytokines. Histological and metalloproteinases analyses were performed on selected organs. RESULTS: Blood acidification consistently increased VCO2ML by 62 to 78%, from 79 ± 13 to 128 ± 22 ml/min at baseline, from 60 ± 8 to 101 ± 16 ml/min at 24 h, and from 54 ± 6 to 96 ± 16 ml/min at 48 h. During regional acidification, arterial pH decreased slightly (average reduction, 0.04), whereas arterial lactate remained lower than 4 mEq/l. No sign of organ and erythrocyte damage was recorded. CONCLUSION: Infusion of lactic acid at the membrane lung inlet consistently increased VCO2ML providing a safe removal of carbon dioxide from only 250 ml/min extracorporeal blood flow in amounts equivalent to 50% production of an adult man. [ABSTRACT FROM AUTHOR]

Published

2014

6. Dual Kinase Targeting in Leukemia.

Author

Mologni, Luca, Marzaro, Giovanni, Redaelli, Sara, and Zambon, Alfonso

Subjects

*THERAPEUTIC use of antineoplastic agents, *CHRONIC myeloid leukemia, *PROTEIN kinase inhibitors, *ACUTE myeloid leukemia, *MOLECULAR structure, *HISTONE deacetylase, *LYMPHOMAS, *CHEMICAL inhibitors

Abstract

Simple Summary: A new option to treat cancer is based on the use of so-called multi-targeting drugs. This strategy can replace the standard treatment based on the co-administration of several drugs. An increased and uncontrolled activity of kinases (enzymes devoted to the regulation of several cell pathways) is often seen in hematological malignancies. The development of multi-kinase inhibitors is having a great impact on the treatment of this kind of cancer. Here, we review the most recent findings on this novel class of drugs. Pharmacological cancer therapy is often based on the concurrent inhibition of different survival pathways to improve treatment outcomes and to reduce the risk of relapses. While this strategy is traditionally pursued only through the co-administration of several drugs, the recent development of multi-targeting drugs (i.e., compounds intrinsically able to simultaneously target several macromolecules involved in cancer onset) has had a dramatic impact on cancer treatment. This review focuses on the most recent developments in dual-kinase inhibitors used in acute myeloid leukemia (AML), chronic myelogenous leukemia (CML), and lymphoid tumors, giving details on preclinical studies as well as ongoing clinical trials. A brief overview of dual-targeting inhibitors (kinase/histone deacetylase (HDAC) and kinase/tubulin polymerization inhibitors) applied to leukemia is also given. Finally, the very recently developed Proteolysis Targeting Chimeras (PROTAC)-based kinase inhibitors are presented. [ABSTRACT FROM AUTHOR]

Published

2021

7. Recurrent ETNK1 mutations in atypical chronic myeloid leukemia.

Author

Gambacorti-Passerini, Carlo B., Donadoni, Carla, Parmiani, Andrea, Pirola, Alessandra, Redaelli, Sara, Signore, Giovanni, Piazza, Vincenzo, Malcovati, Luca, Fontana, Diletta, Spinelli, Roberta, Magistroni, Vera, Gaipa, Giuseppe, Peronaci, Marco, Morotti, Alessandro, Panuzzo, Cristina, Saglio, Giuseppe, Usala, Emilio, Dong-Wook Kim, Rea, Delphine, and Zervakis, Konstantinos

Subjects

*GENETIC mutation, *CHRONIC myeloid leukemia, *SOMATIC mutation, *PHOSPHOCHOLINE derivatives, *MYELODYSPLASTIC syndromes

Abstract

Despite the recent identification of recurrent SETBP1 mutations in atypical chronic myeloid leukemia (aCML), a complete description of the somatic lesions responsible for the onset of this disorder is still lacking. To find additional somatic abnormalities in aCML, we performed whole-exome sequencing on 15 aCML cases. In 2 cases (13.3%), we identified somatic missense mutations in the ETNK1 gene. Targeted resequencing on 515 hematological clonal disorders revealed the presence of ETNK1 variants in 6 (8.8%) of 68 aCML and 2 (2.6%) of 77 chronic myelomonocytic leukemia samples. These mutations clustered in a small region of the kinase domain, encoding for H243Y and N244S (1/8 H243Y; 7/8 N244S). They were all heterozygous and present in the dominant clone. The intracellular phosphoethanolamine/phosphocholine ratio was, on average, 5.2-fold lower in ETNK1-mutated samples (P < .05). Similar results were obtained using myeloid TF1 cells transduced with ETNK1 wild type, ETNK1-N244S, and ETNK1-H243Y, where the intracellular phosphoethanolamine/phosphocholine ratio was significantly lower in ETNK1-N244S (0.76 ± 0.07) and ETNK1-H243Y (0.37 ± 0.02) than in ETNK1-WT (1.37 ± 0.32; P = .01 and P = .0008, respectively), suggesting that ETNK1 mutations may inhibit the catalytic activity of the enzyme. In summary, our study shows for the first time the evidence of recurrent somatic ETNK1 mutations in the context of myeloproliferative/myelodysplastic disorders. [ABSTRACT FROM AUTHOR]

Published

2015

8. Extracorporeal carbon dioxide removal through ventilation of acidified dialysate: An experimental study.

Author

Zanella, Alberto, Mangili, Paolo, Giani, Marco, Redaelli, Sara, Scaravilli, Vittorio, Castagna, Luigi, Sosio, Simone, Pirrone, Federica, Albertini, Mariangela, Patroniti, Nicolò, and Pesenti, Antonio

Subjects

*EXTRACORPOREAL carbon dioxide removal, *DIALYSIS (Chemistry), *ARTIFICIAL respiration, *LACTIC acid, *ACIDIFICATION, *BLOOD flow

Abstract

Background: Extracorporeal (EC) carbon dioxide (CO2) removal (ECCO2R) may be a powerful alternative to ventilation, possibly avoiding the need for mechanical ventilation and endotracheal intubation. We previously reported how an infusion of lactic acid before a membrane lung (ML) effectively enhances ECCO2R. We evaluated an innovative ECCO2R technique based on ventilation of acidified dialysate. Methods: Four swine were sedated, mechanically ventilated, and connected to a venovenous dialysis circuit (blood flow, 250 ml/min). The dialysate was recirculated in a closed loop circuit including a ML (gas flow, 10 liters/min) and then returned to the dialyzer. In each animal, 4 different dialysis flows (DF) of 200, 400, 600, and 800 ml/min were evaluated with and without lactic acid infusion (2.5 mEq/min); the sequence was completed 3 times. At the end of each step, we measured the volume of CO2R by the ML (Vco 2ML) and collected blood and dialysate samples for gas analyses. Results: Acid infusion substantially increased Vco 2ML, from 33 ± 6 ml/min to 86 ± 7 ml/min. Different DFs had little effect on Vco 2ML, which was only slightly reduced at DF 200 ml/min. The partial pressure of CO2 of blood passing through the dialysis filter changed from 60.9 ± 3.6 to 37.1 ± 4.8 mm Hg without acidification and to 32.5 ± 5.3 mm Hg with acidification, corresponding to a pH increase of 0.18 ± 0.03 and 0.03 ± 0.04 units, respectively. Conclusions: Ventilation of acidified dialysate efficiently increased ECCO2R of an amount corresponding to 35% to 45% of the total CO2 production of an adult man from a blood flow as low as 250 ml/min. [ABSTRACT FROM AUTHOR]

Published

2014

9. Crizotinib in Advanced, Chemoresistant Anaplastic Lymphoma Kinase--Positive Lymphoma Patients.

Author

Gambacorti Passerini, Carlo, Farina, Francesca, Stasia, Alessandra, Redaelli, Sara, Ceccon, Monica, Mologni, Luca, Messa, Cristina, Guerra, Luca, Giudici, Giovanni, Sala, Elena, Mussolin, Lara, Deeren, Dries, King, Michael H., Steurer, Michael, Ordemann, Rainer, Cohen, Amos M., Grube, Matthias, Bernard, Lea, Chiriano, Gianpaolo, and Antolini, Laura

Subjects

*LYMPHOMAS, *ANAPLASTIC lymphoma kinase, *CANCER chemotherapy, *ANTINEOPLASTIC agents, *CANCER research

Abstract

Anaplastic lymphoma kinase (ALK)-positive lymphomas respond to chemotherapy, but relapses, which bear a poor prognosis, occur. Crizotinib inhibits ALK in vitro and in vivo and was administered as monotherapy to 11 ALK+ lymphoma patients who were resistant/refractory to cytotoxic therapy. The overall response rate was 10 of 11 (90.9%; 95% confidence interval [CI] = 58.7% to 99.8%). Disease status at the lates follow-up is as follows: four patients are in complete response (CR) (months >21, >30, >35, >40) under continuous crizotinib administration; 4 patients had progression of disease (months 1, 2, 2, 2); 1 patient obtained CR on crizotinib, received an allogeneic bone marrow transplant, and is in CR; 2 patients (treated before and/or after allogeneic bone marrow transplant) obtained and are still in CR but they have stopped crizotinib. Overall and progression-free survival rates at 2 years are 72.7% (95% CI = 39.1% to 94.0%) and 63.7% (95% CI = 30.8% to 89.1%), respectively. AL mutations conferring resistance to crizotinib in vitro could be identified in relapsed patients. Crizotinib exerted a potent antitumor activity with durable responses in advanced, heavily pretreated ALK+ lymphoma patients, with a benign safety profile. [ABSTRACT FROM AUTHOR]

Published

2014

10. CEQer: A Graphical Tool for Copy Number and Allelic Imbalance Detection from Whole-Exome Sequencing Data.

Author

Piazza, Rocco, Magistroni, Vera, Pirola, Alessandra, Redaelli, Sara, Spinelli, Roberta, Redaelli, Serena, Galbiati, Marta, Valletta, Simona, Giudici, Giovanni, Cazzaniga, Giovanni, and Gambacorti-Passerini, Carlo

Subjects

*DNA copy number variations, *ALLELES, *NUCLEOTIDE sequence, *COMPARATIVE genomic hybridization, *LOSS of heterozygosity, *HEURISTIC, *DATA analysis

Abstract

Copy number alterations (CNA) are common events occurring in leukaemias and solid tumors. Comparative Genome Hybridization (CGH) is actually the gold standard technique to analyze CNAs; however, CGH analysis requires dedicated instruments and is able to perform only low resolution Loss of Heterozygosity (LOH) analyses. Here we present CEQer (Comparative Exome Quantification analyzer), a new graphical, event-driven tool for CNA/allelic-imbalance (AI) coupled analysis of exome sequencing data. By using case-control matched exome data, CEQer performs a comparative digital exonic quantification to generate CNA data and couples this information with exome-wide LOH and allelic imbalance detection. This data is used to build mixed statistical/heuristic models allowing the identification of CNA/AI events. To test our tool, we initially used in silico generated data, then we performed whole-exome sequencing from 20 leukemic specimens and corresponding matched controls and we analyzed the results using CEQer. Taken globally, these analyses showed that the combined use of comparative digital exon quantification and LOH/AI allows generating very accurate CNA data. Therefore, we propose CEQer as an efficient, robust and user-friendly graphical tool for the identification of CNA/AI in the context of whole-exome sequencing data. [ABSTRACT FROM AUTHOR]

Published

2013

11. Rapid recognition of drug-resistance/sensitivity in leukemic cells by Fourier transform infrared microspectroscopy and unsupervised hierarchical cluster analysis.

Author

Bellisola, Giuseppe, Cinque, Gianfelice, Vezzalini, Marzia, Moratti, Elisabetta, Silvestri, Giovannino, Redaelli, Sara, Passerini, Carlo Gambacorti, Wehbe, Katia, and Sorio, Claudio

Subjects

*LEUKEMIA, *DRUG resistance, *FOURIER transform infrared spectroscopy, *PROTEIN-tyrosine kinases, *SYNCHROTRON radiation, *IMMUNOCHEMISTRY

Abstract

We tested the ability of Fourier Transform (FT) InfraRed (IR) microspectroscopy (microFTIR) in combination with unsupervised Hierarchical Cluster Analysis (HCA) in identifying drug-resistance/sensitivity in leukemic cells exposed to tyrosine kinase inhibitors (TKIs). Experiments were carried out in a well-established mouse model of human Chronic Myelogenous Leukemia (CML). Mouse-derived pro-B Ba/F3 cells transfected with and stably expressing the human p210BCR-ABL drug-sensitive wild-type BCR-ABL or the V299L or T315I p210BCR-ABL drug-resistant BCR-ABL mutants were exposed to imatinib-mesylate (IMA) or dasatinib (DAS). MicroFTIR was carried out at the Diamond IR beamline MIRIAM where the mid-IR absorbance spectra of individual Ba/F3 cells were acquired using the high brilliance IR synchrotron radiation (SR) via aperture of 15 × 15 μm2 in sizes. A conventional IR source (globar) was used to compare average spectra over 15 cells or more. IR signatures of drug actions were identified by supervised analyses in the spectra of TKI-sensitive cells. Unsupervised HCA applied to selected intervals of wavenumber allowed us to classify the IR patterns of viable (drug-resistant) and apoptotic (drug-sensitive) cells with an accuracy of ＞95%. The results from microFTIR + HCA analysis were cross-validated with those obtained via immunochemical methods, i.e. immunoblotting and flow cytometry (FC) that resulted directly and significantly correlated. We conclude that this combined microFTIR + HCA method potentially represents a rapid, convenient and robust screening approach to study the impact of drugs in leukemic cells as well as in peripheral blasts from patients in clinical trials with new anti-leukemic drugs. [ABSTRACT FROM AUTHOR]

Published

2013

12. Recurrent SETBP1 mutations in atypical chronic myeloid leukemia.

Author

Piazza, Rocco, Valletta, Simona, Winkelmann, Nils, Redaelli, Sara, Spinelli, Roberta, Pirola, Alessandra, Antolini, Laura, Mologni, Luca, Donadoni, Carla, Papaemmanuil, Elli, Schnittger, Susanne, Kim, Dong-Wook, Boultwood, Jacqueline, Rossi, Fabio, Gaipa, Giuseppe, De Martini, Greta P, di Celle, Paola Francia, Jang, Hyun Gyung, Fantin, Valeria, and Bignell, Graham R

Subjects

*CHRONIC myeloid leukemia, *DISEASE relapse, *GENETIC mutation, *AMINO acid sequence, *CANCER cells, *CELL lines, *GENE fusion, *GENE expression

Abstract

Atypical chronic myeloid leukemia (aCML) shares clinical and laboratory features with CML, but it lacks the BCR-ABL1 fusion. We performed exome sequencing of eight aCMLs and identified somatic alterations of SETBP1 (encoding a p.Gly870Ser alteration) in two cases. Targeted resequencing of 70 aCMLs, 574 diverse hematological malignancies and 344 cancer cell lines identified SETBP1 mutations in 24 cases, including 17 of 70 aCMLs (24.3%; 95% confidence interval (CI) = 16-35%). Most mutations (92%) were located between codons 858 and 871 and were identical to changes seen in individuals with Schinzel-Giedion syndrome. Individuals with mutations had higher white blood cell counts (P = 0.008) and worse prognosis (P = 0.01). The p.Gly870Ser alteration abrogated a site for ubiquitination, and cells exogenously expressing this mutant exhibited higher amounts of SETBP1 and SET protein, lower PP2A activity and higher proliferation rates relative to those expressing the wild-type protein. In summary, mutated SETBP1 represents a newly discovered oncogene present in aCML and closely related diseases. [ABSTRACT FROM AUTHOR]

Published

2013

13. ERG Deregulation Induces PIM1 Over-Expression and Aneuploidy in Prostate Epithelial Cells.

Author

Magistroni, Vera, Mologni, Luca, Sanselicio, Stefano, Reid, James Frances, Redaelli, Sara, Piazza, Rocco, Viltadi, Michela, Bovo, Giorgio, Strada, Guido, Grasso, Marco, Gariboldi, Manuela, and Gambacorti-Passerini, Carlo

Subjects

*EPITHELIAL cells, *GENETIC regulation, *ANEUPLOIDY, *TRANSCRIPTION factors, *GENE expression, *KINASES, *CHROMATIN

Abstract

The ERG gene belongs to the ETS family of transcription factors and has been found to be involved in atypical chromosomal rearrangements in several cancers. To gain insight into the oncogenic activity of ERG, we compared the gene expression profile of NIH-3T3 cells stably expressing the coding regions of the three main ERG oncogenic fusions: TMPRSS2/ERG (tERG), EWS/ERG and FUS/ERG. We found that all three ERG fusions significantly up-regulate PIM1 expression in the NIH-3T3 cell line. PIM1 is a serine/threonine kinase frequently over-expressed in cancers of haematological and epithelial origin. We show here that tERG expression induces PIM1 in the non-malignant prostate cell line RWPE-1, strengthening the relation between tERG and PIM1 up-regulation in the initial stages of prostate carcinogenesis. Silencing of tERG reversed PIM1 induction. A significant association between ERG and PIM1 expression in clinical prostate carcinoma specimens was found, suggesting that such a mechanism may be relevant in vivo. Chromatin Immunoprecipitation experiments showed that tERG directly binds to PIM1 promoter in the RWPE-1 prostate cell line, suggesting that tERG could be a direct regulator of PIM1 expression. The up-regulation of PIM1 induced by tERG over-expression significantly modified Cyclin B1 levels and increased the percentage of aneuploid cells in the RWPE-1 cell line after taxane-based treatment. Here we provide the first evidence for an ERG-mediated PIM1 up-regulation in prostate cells in vitro and in vivo, suggesting a direct effect of ERG transcriptional activity in the alteration of genetic stability. [ABSTRACT FROM AUTHOR]

Published

2011

14. Bcr-Abl stabilizes β-catenin in chronic myeloid leukemia through its tyrosine phosphorylation.

Author

Coluccia, Addolorata Maria Luce, Vacca, Angelo, Duñach, Mireia, Mologni, Luca, Redaelli, Sara, Bustos, Victor H., Benati, Daniela, Pinna, Lorenzo A., and Gambacorti-Passerini, Carlo

Subjects

*CHRONIC myeloid leukemia, *PHOSPHORYLATION, *PROTEIN-tyrosine phosphatase, *PROTEIN-tyrosine kinases, *LEUKEMIA etiology, *RNA

Abstract

Self-renewal of Bcr-Abl+ chronic myeloid leukemia (CML) cells is sustained by a nuclear activated serine/threonine-(S/T) unphosphorylated β-catenin. Although β-catenin can be tyrosine (Y)-phosphorylated, the occurrence and biological relevance of this covalent modification in Bcr-Abl-associated leukemogenesis is unknown. Here we show that Bcr-Abl levels control the degree of β-catenin protein stabilization by affecting its Y/S/T-phospho content in CML cells. Bcr-Abl physically interacts with β-catenin, and its oncogenic tyrosine kinase activity is required to phosphorylate β-catenin at Y86 and Y654 residues. This Y-phospho β-catenin binds to the TCF4 transcription factor, thus representing a transcriptionally active pool. Imatinib, a Bcr-Abl antagonist, impairs the β-catenin/TCF-related transcription causing a rapid cytosolic retention of Y-unphosphorylated β-catenin, which presents an increased binding affinity for the Axin/GSK3β complex. Although Bcr-Abl does not affect GSK3β autophosphorylation, it prevents, through its effect on β-catenin Y phosphorylation, Axin/GSK3β binding to β-catenin and its subsequent S/T phosphorylation. Silencing of β-catenin by small interfering RNA inhibited proliferation and clonogenicity of Bcr-Abl+ CML cells, in synergism with Imatinib. These findings indicate the Bcr-Abl triggered Y phosphorylation of β-catenin as a new mechanism responsible for its protein stabilization and nuclear signalling activation in CML. [ABSTRACT FROM AUTHOR]

Published

2007

15. Expression, purification, and inhibition of human RET tyrosine kinase

Author

Mologni, Luca, Sala, Elisa, Riva, Barbara, Cesaro, Luca, Cazzaniga, Sara, Redaelli, Sara, Marin, Oriano, Pasquato, Nicola, Donella-Deana, Arianna, and Gambacorti-Passerini, Carlo

Subjects

*PROTEIN-tyrosine kinases, *CHROMATOGRAPHIC analysis, *ENZYME-linked immunosorbent assay, *THYROID gland

Abstract

Abstract: Tyrosine kinases are emerging as frequent targets of primary oncogenic events and therefore represent an optimal focus of therapeutical intervention. Genetic alterations that cause dysregulated activation of the RET tyrosine kinase are responsible for a significant fraction of thyroid carcinomas. In an effort towards therapeutic RET inactivation, we have developed a method for expression and purification of recombinant RET catalytic domain for structural purposes and for use in the screening of potential inhibitors of RET kinase activity. His-tagged RET kinase domain was purified from Sf9 insect cell lysate using a two-step chromatographic protocol and characterised. Purified recombinant RET phosphorylated itself and exogenous substrates at physiological pH. A specific peptide substrate, derived from RET activation loop, was identified and experimentally validated. These reagents were used to develop a rapid ELISA-based kinase assay for screening potential inhibitors. Novel RET inhibitors were identified using this assay. [Copyright &y& Elsevier]

Published

2005

16. Synergistic Drug Combinations Prevent Resistance in ALK+ Anaplastic Large Cell Lymphoma.

Author

Arosio, Giulia, Sharma, Geeta G., Villa, Matteo, Mauri, Mario, Crespiatico, Ilaria, Fontana, Diletta, Manfroni, Chiara, Mastini, Cristina, Zappa, Marina, Magistroni, Vera, Ceccon, Monica, Redaelli, Sara, Massimino, Luca, Garbin, Anna, Lovisa, Federica, Mussolin, Lara, Piazza, Rocco, Gambacorti-Passerini, Carlo, and Mologni, Luca

Subjects

*PROTEIN metabolism, *THERAPEUTIC use of antineoplastic agents, *IN vitro studies, *IN vivo studies, *ANIMAL experimentation, *DRUG resistance, *CELL physiology, *APOPTOSIS, *PIPERIDINE, *DECITABINE, *CELLULAR signal transduction, *DRUG synergism, *CELL lines, *T-cell lymphoma, *ENZYME inhibitors, *MICE

Abstract

Simple Summary: Despite success of targeted therapy, cancer cells very often find a way to survive treatment; this eventually causes a tumor to relapse. In a particular type of lymphoma carrying a specific chromosomal rearrangement named anaplastic large-cell lymphoma (ALCL), selective drugs targeting the cause of the disease can induce spectacular remission of chemotherapy-resistant cancer. However, the lymphoma relapses again in about half of the cases, leaving no therapeutic options. We studied the possibility to combine two simultaneous treatments in order to prevent the relapse, starting from the hypothesis that acquiring resistance to two drugs at the same time is statistically very unlikely. We demonstrate that treating lymphoma cells with drug combinations has superior efficacy in comparison with single drug treatments, both in cell cultures and in mice. Anaplastic lymphoma kinase-positive (ALK+) anaplastic large-cell lymphoma (ALCL) is a subtype of non-Hodgkin lymphoma characterized by expression of the oncogenic NPM/ALK fusion protein. When resistant or relapsed to front-line chemotherapy, ALK+ ALCL prognosis is very poor. In these patients, the ALK inhibitor crizotinib achieves high response rates, however 30–40% of them develop further resistance to crizotinib monotherapy, indicating that new therapeutic approaches are needed in this population. We here investigated the efficacy of upfront rational drug combinations to prevent the rise of resistant ALCL, in vitro and in vivo. Different combinations of crizotinib with CHOP chemotherapy, decitabine and trametinib, or with second-generation ALK inhibitors, were investigated. We found that in most cases combined treatments completely suppressed the emergence of resistant cells and were more effective than single drugs in the long-term control of lymphoma cells expansion, by inducing deeper inhibition of oncogenic signaling and higher rates of apoptosis. Combinations showed strong synergism in different ALK-dependent cell lines and better tumor growth inhibition in mice. We propose that drug combinations that include an ALK inhibitor should be considered for first-line treatments in ALK+ ALCL. [ABSTRACT FROM AUTHOR]

Published

2021

17. Crizotinib in advanced, chemoresistant anaplastic lymphoma kinase-positive lymphoma patients.

Author

Gambacorti Passerini, Carlo, Farina, Francesca, Stasia, Alessandra, Redaelli, Sara, Ceccon, Monica, Mologni, Luca, Messa, Cristina, Guerra, Luca, Giudici, Giovanni, Sala, Elena, Mussolin, Lara, Deeren, Dries, King, Michael H, Steurer, Michael, Ordemann, Rainer, Cohen, Amos M, Grube, Matthias, Bernard, Lea, Chiriano, Gianpaolo, and Antolini, Laura

Published

2014