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10. Synergistic drug combinations preventdrug resistance in anaplastic large cell lymphomapreclinical models

Author

Sharma, G, Arosio, G, Villa, M, Mauri, M, Zappa, M, Magistroni, V, Ceccon, M, Redaelli, S, Crespiatico, I, Fontana, D, Mastini, C, Garbin, A, Lovisa, F, Mussolin, L, Piazza, R, Gambacorti Passerini, C, Mologni, L, Sharma, G, Arosio, G, Villa, M, Mauri, M, Zappa, M, Magistroni, V, Ceccon, M, Redaelli, S, Crespiatico, I, Fontana, D, Mastini, C, Garbin, A, Lovisa, F, Mussolin, L, Piazza, R, Gambacorti Passerini, C, and Mologni, L

Subjects
drug combinations, anaplastic large cell lymphoma
Published
2021

13. Synergistic drug combinations prevent resistance in ALK+ anaplastic large cell lymphoma

Author

Arosio, G, Sharma, G, Villa, M, Mauri, M, Crespiatico, I, Fontana, D, Manfroni, C, Mastini, C, Zappa, M, Magistroni, V, Ceccon, M, Redaelli, S, Massimino, L, Garbin, A, Lovisa, F, Mussolin, L, Piazza, R, Gambacorti Passerini, C, Mologni, L, Sharma, GG, Arosio, G, Sharma, G, Villa, M, Mauri, M, Crespiatico, I, Fontana, D, Manfroni, C, Mastini, C, Zappa, M, Magistroni, V, Ceccon, M, Redaelli, S, Massimino, L, Garbin, A, Lovisa, F, Mussolin, L, Piazza, R, Gambacorti Passerini, C, Mologni, L, and Sharma, GG

Abstract

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.

Published
2021

17. Use of narrative medicine to identify key factors for effective doctor–patient relationships in severe asthma

Author

Cappuccio, A., Napolitano, S., Menzella, F., Pellegrini, G., Policreti, A., Pelaia, G., Porpiglia, P. A., Marini, M. G., Antonelli, A., Arezzo, C., Baglioni, S., Boni, E., Bragantini, A., Bruzzese, D., Caldarelli, V., Caminati, M., Caminiti, L., Carraro, C., Ceccon, M. A., Bianchi, F. C., Cirisano, A., Cogo, R., Conte, E., D(')Auria, E., Daniele, S., De Brasi, D., De Castro, G., De Luca, S., Detoraki, C., Di Palmo, E., Fenu, G., Ferrara, A., Ferrigno, G., Fusi, A., Gaccione, A., Gandino, M., Guarnieri, G., Guerrieri, A., Iacoacci, C., Lacedonia, D., Schiavo, M. L., Longo, R., Magazz(`u), C., Marzo, G., Mastroberardino, M., Mattioli, G. P., Monaco, L., Montera, C., Morelli, M., Nicolini, A., Omodeo, P., Palmiero, G., Pannofino, A., Papa, A., Patria, F., Pini, L., Polti, S., Pontillo, A., Poppa, M., Poto, S., Quercia, O., Raie, A., Ronzoni, V., Rosati, Y., Russo, A., Salzillo, A., Santoro, M., Savoia, F., Simonazzi, A., Sposato, B., Tourtchenko, V., Tripodi, S., Vatrella, A., and Veronelli, E.

Subjects
Pulmonary and Respiratory Medicine, Severe asthma, medicine.medical_specialty, media_common.quotation_subject, Medical education and training, Empathy, Grounded theory, 03 medical and health sciences, 0302 clinical medicine, Promotion (rank), Qualitative research, Medicine, Narrative, Original Research Article, 030212 general & internal medicine, education, Asthma, media_common, lcsh:RC705-779, Narrative medicine, education.field_of_study, business.industry, lcsh:Diseases of the respiratory system, medicine.disease, 030228 respiratory system, Family medicine, business
Abstract

Background: In this project the authors use a narrative medicine (NM) approach to assess the promotion of trust in the relationship between physicians and their asthma patients. Methods: Following a NM educational course for physicians, a research was carried out in which at least 5 written narratives (parallel charts) for each participating physician were collected and qualitatively analysed according to Bury’s classification and the Grounded Theory. Results: The results of this study were of speculative and clinical interest. In particular, 66 participants wrote 314 narratives (246 on adult and 68 on paediatric patients). As a result of applying the NM approach, when the relationships remained problematic, many physicians wrote with a moral style about their adult (67%), and paediatric patients (33%) - especially in cases of asthmatic children’s or adolescents’ overprotective or absent families (40%) -. On the contrary, physicians who were able to listen to their patients with empathy (35%) made more shared decisions with patients, even with those they initially had a bad relationship. The used words of welcome, interest and acceptance were promoting patients’ trust that lead to restoring their activities in 45% of cases, according to physicians self-reporting. Conclusions: These approaches of NM are useful in daily clinical practice, with the goal of improving the quality of life (QOL) of patients with severe asthma, even in cases in which the doctor-patient relationship isn’t initially good.

Published
2019
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21. Erratum: Treatment efficacy and resistance mechanisms using the second-generation ALK inhibitor AP26113 in human NPM-ALK-positive anaplastic large cell lymphoma (Molecular Cancer Research (2015) 13 (775-783))

Author

Ceccon M., Ceccon, M, Mologni, L, Giudici, G, Piazza, R, Pirola, A, Fontana, D, Ceccon M., Mologni L., Giudici G., Piazza R., Pirola A., Fontana D., Ceccon M., Ceccon, M, Mologni, L, Giudici, G, Piazza, R, Pirola, A, Fontana, D, Ceccon M., Mologni L., Giudici G., Piazza R., Pirola A., and Fontana D.

Published
2015

22. Lorlatinib treatment elicits multiple on- and off-target mechanisms of resistance in ALK-driven cancer

Author

Redaelli, S, Ceccon, M, Zappa, M, Geeta, G, Mastini, C, Mauri, M, Nigoghossian, M, Massimino, L, Cordani, N, Farina, F, Piazza, R, Gambacorti-Passerini, C, Mologni, L, Redaelli, Sara, Ceccon, Monica, Zappa, Marina, Sharma, Geeta G, Mastini, Cristina, Mauri, Mario, Nigoghossian, Marion, Massimino, Luca, Cordani, Nicoletta, Farina, Francesca, Piazza, Rocco, Gambacorti-Passerini, Carlo, Mologni, Luca, Redaelli, S, Ceccon, M, Zappa, M, Geeta, G, Mastini, C, Mauri, M, Nigoghossian, M, Massimino, L, Cordani, N, Farina, F, Piazza, R, Gambacorti-Passerini, C, Mologni, L, Redaelli, Sara, Ceccon, Monica, Zappa, Marina, Sharma, Geeta G, Mastini, Cristina, Mauri, Mario, Nigoghossian, Marion, Massimino, Luca, Cordani, Nicoletta, Farina, Francesca, Piazza, Rocco, Gambacorti-Passerini, Carlo, and Mologni, Luca

Abstract

Targeted therapy changed the standard of care in ALK-dependent tumors. However, resistance remains a major challenge. Lorlatinib is a third-generation ALK inhibitor that inhibits most ALK mutants resistant to current ALK inhibitors. In this study, we utilize lorlatinib-resistant anaplastic large cell lymphoma (ALCL), non–small cell lung cancer (NSCLC), and neuroblastoma cell lines in vitro and in vivo to investigate the acquisition of resistance and its underlying mechanisms. ALCL cells acquired compound ALK mutations G1202R/G1269A and C1156F/L1198F in vitro at high drug concentrations. ALCL xenografts selected in vivo showed recurrent N1178H (5/10 mice) and G1269A (4/10 mice) mutations. Interestingly, intracellular localization of NPM/ALKN1178H skewed toward the cytoplasm in human cells, possibly mimicking overexpression. RNA sequencing of resistant cells showed significant alteration of PI3K/AKT and RAS/MAPK pathways. Functional validation by small-molecule inhibitors confirmed the involvement of these pathways in resistance to lorlatinib. NSCLC cells exposed in vitro to lorlatinib acquired hyperactivation of EGFR, which was blocked by erlotinib to restore sensitivity to lorlatinib. In neuroblastoma, whole-exome sequencing and proteomic profiling of lorlatinib-resistant cells revealed a truncating NF1 mutation and hyperactivation of EGFR and ErbB4. These data provide an extensive characterization of resistance mechanisms that may arise in different ALK-positive cancers following lorlatinib treatment. Significance: High-throughput genomic, transcriptomic, and proteomic profiling reveals various mechanisms by which multiple tumor types acquire resistance to the third-generation ALK inhibitor lorlatinib.

Published
2018

23. Mitochondrial Hyperactivation and Enhanced ROS Production are Involved in Toxicity Induced by Oncogenic Kinases Over-Signaling

Author

Ceccon, M, Mauri, M, Massimino, L, Giudici, G, Piazza, R, Gambacorti-Passerini, C, Mologni, L, Ceccon, Monica, Mauri, Mario, Massimino, Luca, Giudici, Giovanni, Piazza, Rocco, Gambacorti-Passerini, Carlo, Mologni, Luca, Ceccon, M, Mauri, M, Massimino, L, Giudici, G, Piazza, R, Gambacorti-Passerini, C, Mologni, L, Ceccon, Monica, Mauri, Mario, Massimino, Luca, Giudici, Giovanni, Piazza, Rocco, Gambacorti-Passerini, Carlo, and Mologni, Luca

Abstract

Targeted therapy is an effective, rational, and safe approach to solid and hematological tumors treatment. Unfortunately, a significant fraction of patients treated with tyrosine kinase inhibitors (TKI) relapses mainly because of gene amplification, mutations, or other bypass mechanisms. Recently a growing number of papers showed how, in some cases, resistance due to oncogene overexpression may be associated with drug addiction: cells able to proliferate in the presence of high TKI doses become also TKI dependent, undergoing cellular stress, and apoptosis/death upon drug withdrawal. Notably, if a sub-cellular population survives TKI discontinuation it is also partially re-sensitized to the same drug. Thus, it is possible that a subset of patients relapsing upon TKI treatment may benefit from a discontinuous therapeutic schedule. We focused on two different hematologic malignancies, chronic myeloid leukemia (CML) and anaplastic large cell lymphoma (ALCL), both successfully treatable with TKIs. The two models utilized (LAMA and SUP-M2) differed in having oncogene overexpression as the sole cause of drug resistance (CML), or additionally carrying kinase domain mutations (ALCL). In both cases drug withdrawal caused a sudden overload of oncogenic signal, enhanced mitochondria activity, induced the release of a high amount of reactive oxygen species (ROS), and caused genotoxic stress and massive cell death. In LAMA cells (CML) we could rescue the cells from death by partially blocking downstream oncogenic signaling or lowering ROS detrimental effect by adding reduced glutathione

Published
2018

24. Abstract 902: In vitro andin vivocharacterization of resistance to lorlatinib treatment in ALK mutated cancers

Author

Geeta, G, Redaelli, S, Ceccon, M, Zappa, M, Gambacorti-Passerini, C, Mologni, L, GEETA, GEETA, Geeta, G, Redaelli, S, Ceccon, M, Zappa, M, Gambacorti-Passerini, C, Mologni, L, and GEETA, GEETA

Abstract

The development of targeted therapy has significantly improved the treatment of Anaplastic Lymphoma Kinase (ALK) dependent neoplasias such as Anaplastic Large Cell Lymphoma (ALCL) and Non-Small Cell Lung Cancer (NSCLC). Despite the efficacy of ALK inhibitor crizotinib, acquired resistance is a major challenge. Lorlatinib is a second generation inhibitor with improved activity and selectivity against ALK. To investigate resistance mechanisms that may arise on lorlatinib therapy, we selected in vitro and in vivo lorlatinib resistant tumor cells. In vivo, 10 mice carrying subcutaneous Karpas299 xenografts received vehicle or lorlatinib at increasing doses, starting at 0.1 mg/kg BID. As expected, tumor size was significantly reduced in lorlatinib group compared to controls. After initial partial responses, tumors relapsed and mice were shifted to an increased dose (0.25 mg/kg). Tumors relapsed again and mice were randomized into three groups, to achieve a maximum dose of 0.5, 1 or 2 mg/kg. In all cases tumors regrew after an initial response, indicating acquired resistance to lorlatinib. Upon mice sacrifice, tumors were collected and characterized. All ex vivo cell lines were resistant to lorlatinib as assessed by proliferation assay and 2/10 showed moderate drug addiction. However, in several cases, ALK phosphorylation did not fully correlate with the observed high drug resistance, suggesting the involvement of ALK-independent mechanisms. ALK kinase domain sequencing revealed N1178H mutation in 5/10 mice, alone or in combination with other mutations and L1196M substitution in 2/10 cases. Since both mutants have been described as sensitive or moderately resistant to lorlatinib in murine BaF3 cells, further characterization of these cell lines was performed. ALK N1178H mutant was found to be predominantly localized in the cytoplasm, possibly mimicking overexpression, in human cells. Whole-exome and mRNA sequencing of cells carrying the L1196M substitution showed signific

Published
2018

25. Mechanisms of resistance to the second-generation ALK inhibitor AP26113 in human NPM-ALK-positive anaplastic large cell lymphoma cells

Author

Ceccon, M, Mologni, L, Giudici, G, Piazza, R, Pirola, A, Fontana, D, Gambacorti-Passerini, C, Ceccon, M, Mologni, L, Giudici, G, Piazza, R, Pirola, A, Fontana, D, and Gambacorti-Passerini, C

Subjects
drug resistance
Abstract

ALK is a tyrosine kinase receptor involved in a broad range of solid and haematological tumors. It has been shown that about 70-80% of ALK+ Anaplastic Large Cell Lymphoma (ALCL) cases, an aggressive Non Hodgkin T-cell lymphoma, are characterized by the traslocation t(2;5), originating the functional, aberrant oncogenic fusion protein NPM-ALK. Crizotinib was the first clinically relevant ALK inhibitor, now approved for the treatment of late stage and metastatic cases of lung cancer. Several patients soon developed Crizotinib resistance, mainly due to the appearance of new point mutations located in ALK kinase domain. Currently, other ALK inhibitors are available and already in clinical trial, hopefully representing the second line therapy able to overcome Crizotinib resistance. In this work we focused our attention on the more potent phase I/II dual ALK/EGFR inhibitor AP26113 (Ariad Pharm.), able to overcome the Crizotinib-resistant gatekeeper mutation L1196M. Two NPM-ALK+ human cell lines, KARPAS-299 and SUP-M2, were grown in four independent flasks in the presence of increasing doses of AP26113, so that eight cell lines able to grow in the presence of high AP26113 doses were selected. All cell lines show an AP26113 50% inhibitory concentration (IC50) value substantially higher than the one observed in parental cells, with a 130 to 1000-fold increase. All KARPAS-299 populations resistant to AP26113 show NPM-ALK overexpression, due to oncogene amplification, as the main cause of resistance, while SUP-M2 cells proliferating in the presence of the drug harbour several point mutations spanning the entire ALK kinase domain. In particular, we identified the following aminoacid substitutions: L1122V, , L1196M, S1206C and a double F1174V+L1198F mutation. The knowledge of the possible appearance of new clinically relevant mechanisms of drug resistance is a useful tool for the management of new TKI resistant cases

Published
2014

27. Synergistic Activity of ALK and mTOR Inhibitors for the Treatment of NPM-ALK Positive Lymphoma

Author

Redaelli, S, Ceccon, M, Pirola, A, Peronaci, M, Gambacorti-Passerini, C, Mologni, L, Redaelli, S, Ceccon, M, Pirola, A, Peronaci, M, Gambacorti-Passerini, C, and Mologni, L

Subjects
drug resistance, ALK, kinase, Immunology, Cell Biology, Hematology, Biochemistry
Abstract

ALK-positive Anaplastic Large Cell Lymphoma (ALCL) is a subset of Non-Hodgkin Lymphoma that positively took advantage of crizotinib development, a selective ALK inhibitor. Crizotinib is able to block ALK kinase activity which is fundamental for cancer cell survival. Constitutively active ALK kinase triggers the activation of several pro-proliferative and pro-survival downstream pathways, such as PI3K/AKT/mTOR. Despite the positive impact of targeted therapy on ALCL treatment, resistant clones tend to be selected during therapy. Strategies to overcome resistance include the design of more potent and selective drugs and the use of combined therapy approaches that allow for the simultaneous targeting of more than one node essential for cancer cells survival. Following this strategy, we decided to investigate the effects of combined ALK/mTOR inhibition. We first observed a synergistic effect of the combination of ALK inhibitors (crizotinib, alectinib or PF-3922) with an mTOR inhibitor (temsirolimus) in proliferation assays. Interestingly, the synergistic effect was observed only in ALK+ cell lines (Karpas 299, SUDH-L1 and SUPM2), while no synergism was observed in ALK- cell line (U937) as well as in normal lymphocytes. The Combination Index (CI) ranged from 0.16 to 0.45 indicating a synergistic/strong synergistic effect, accordingly to Chou classification. (Chou, 2006) (Table 1). The positive cooperation resulted in an increased inhibition of mTOR effectors p70S6K, 4EBP1 and eIF4B compared to single agent treatment as observed in immunoblot analysis performed on Karpas 299 treated for 4 hours. At the cell cycle level, the use of the drugs in combination induced a sharp block in G0/G1 phase, as observed by propidium iodide analysis performed on Karpas 299 at 48-72 and 96 hours. Long term exposure of ALK+ cells to either alectinib or temsirolimus, led to the establishment of resistant cell lines, while the exposure to the combination prevented the selection of resistant clones. Interestingly, the cell line resistant to alectinib showed a marked increase of ALK both at mRNA and protein level. In vivo, nude mice were injected with Karpas 299 cells. As the tumor masses reached 150mm3, mice were randomized and treated for 12 days with the combination of PF-3922 (0.5 mg/kg, administered per os twice a day) and temsirolimus (i.p., 1 mg/kg every other day) or with the single agents. The combined treatment induced a faster regression of the tumor masses compared to the single agents-treated mice. Moreover, responses were sustained for a longer period of time, upon treatment stop. (Figure 1) In conclusion, our data suggest that the combination of ALK and mTOR inhibitors could be a valuable therapeutic option for patients affected by ALK+ ALCL. Table 1. combination indexes from proliferation experiments. Synergism levels calculated accordingly to Chou, Pharmacological reviews, 2006 Crizotinib - Temsirolimus Cell lines Ratio Combination Index (CI) Average CI Synergism level EC50 EC75 EC90 NPM-ALK+ Karpas 299 1:1 0.42 0.35 0.33 0.37 Synergism SUDHL1 3:1 0.49 0.45 0.42 0.45 Synergism SUPM2 1:1 0.59 0.33 0.29 0.40 Synergism NPM-ALK- U937 1:1 >10 >10 >10 >10 Antagonism HD Lymphocytes 1:1 >10 >10 >10 >10 Antagonism Alectinib - Temsirolimus Cell lines Ratio Combination Index (CI) Average CI Synergism level EC50 EC75 EC90 NPM-ALK+ Karpas 299 1:3 0.56 0.29 0.15 0.33 Synergism SUDHL1 1:3 0.53 0.45 0.38 0.45 Synergism SUPM2 1:10 0.65 0.18 0.06 0.3 Strong synergism NPM-ALK- U937 1:3 1.5 >10 >10 >10 Antagonism HD Lymphocytes 1:3 1.2 2.7 7.2 3.7 Antagonism PF06463922 - Temsirolimus Cell lines Ratio Combination Index (CI) Average CI Synergism level EC50 EC75 EC90 NPM-ALK+ Karpas 299 1:10 0.30 0.15 0.15 0.20 Strong synergism SUDHL1 1:30 0.57 0.41 0.29 0.42 Synergism SUPM2 1:3 0.30 0.12 0.06 0.16 Strong synergism NPM-ALK- U937 1:10 3.2 5.39 >10 >10 Antagonism HD Lymphocytes 1:3 1.4 8.8 >10 >10 Antagonism Figure 1. in vivo experiment for the evaluation of the combines treatment. Tumors volume measurements ±SEM are presented Figure 1. in vivo experiment for the evaluation of the combines treatment. Tumors volume measurements ±SEM are presented Disclosures No relevant conflicts of interest to declare.

Published
2015
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28. Synergistic activity of ALK and mTOR inhibitors for the treatment of NPM-ALK positive lymphoma

Author

Redaelli, S, Ceccon, M, Antolini, L, Rigolio, R, Pirola, A, Peronaci, M, GAMBACORTI PASSERINI, C, Mologni, L, REDAELLI, SARA, CECCON, MONICA, ANTOLINI, LAURA, RIGOLIO, ROBERTA, PIROLA, ALESSANDRA, PERONACI, MARCO, GAMBACORTI PASSERINI, CARLO, MOLOGNI, LUCA, Redaelli, S, Ceccon, M, Antolini, L, Rigolio, R, Pirola, A, Peronaci, M, GAMBACORTI PASSERINI, C, Mologni, L, REDAELLI, SARA, CECCON, MONICA, ANTOLINI, LAURA, RIGOLIO, ROBERTA, PIROLA, ALESSANDRA, PERONACI, MARCO, GAMBACORTI PASSERINI, CARLO, and MOLOGNI, LUCA

Abstract

ALK-positive Anaplastic Large Cell Lymphoma (ALCL) represents a subset of Non-Hodgkin Lymphoma whose treatment benefited from crizotinib development, a dual ALK/MET inhibitor. Crizotinib blocks ALK-triggered pathways such as PI3K/AKT/ mTOR, indispensable for survival of ALK-driven tumors. Despite the positive impact of targeted treatment in ALCL, resistant clones are often selected during therapy. Strategies to overcome resistance include the design of second generation drugs and the use of combined therapies that simultaneously target multiple nodes essential for cells survival. We investigated the effects of combined ALK/mTOR inhibition. We observed a specific synergistic effect of combining ALK inhibitors with an mTOR inhibitor (temsirolimus), in ALK+ lymphoma cells. The positive cooperation resulted in an increased inhibition of mTOR effectors, compared to single treatments, a block in G0/G1 phase and induction of apoptosis. The combination was able to prevent the selection of resistant clones, while longterm exposure to single agents led to the establishment of resistant cell lines, with either ALK inhibitor or temsirolimus. In vivo, mice injected with Karpas 299 cells and treated with low dose combination showed complete regression of tumors, while only partial inhibition was obtained in single agents-treated mice. Upon treatment stop the combination was able to significantly delay tumor relapses. Re-challenge of relapsed tumors at a higher dose led to full regression of xenografts in the combination group, but not in mice treated with lorlatinib alone. In conclusion, our data suggest that the combination of ALK and mTOR inhibitors could be a valuable therapeutic option for ALK+ ALCL patients.

Published
2016

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

Author

Redaelli, S, Perini, P, Ceccon, M, Piazza, R, Rigolio, R, Mauri, M, Boschelli, F, Giannoudis, A, GAMBACORTI PASSERINI, C, REDAELLI, SARA, PERINI, PIETRO, CECCON, MONICA, PIAZZA, ROCCO GIOVANNI, RIGOLIO, ROBERTA, MAURI, MARIO, GAMBACORTI PASSERINI, CARLO, Redaelli, S, Perini, P, Ceccon, M, Piazza, R, Rigolio, R, Mauri, M, Boschelli, F, Giannoudis, A, GAMBACORTI PASSERINI, C, REDAELLI, SARA, PERINI, PIETRO, CECCON, MONICA, PIAZZA, ROCCO GIOVANNI, RIGOLIO, ROBERTA, MAURI, MARIO, 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.

Published
2015

31. NPM/ALK mutants resistant to ASP3026 display variable sensitivity to alternative ALK inhibitors but succumb to the novel compound PF-06463922

Author

Mologni, L, Ceccon, M, Pirola, A, Chiriano, G, Piazza, R, Scapozza, L, GAMBACORTI PASSERINI, C, MOLOGNI, LUCA, CECCON, MONICA, PIROLA, ALESSANDRA, PIAZZA, ROCCO GIOVANNI, GAMBACORTI PASSERINI, CARLO, Mologni, L, Ceccon, M, Pirola, A, Chiriano, G, Piazza, R, Scapozza, L, GAMBACORTI PASSERINI, C, MOLOGNI, LUCA, CECCON, MONICA, PIROLA, ALESSANDRA, PIAZZA, ROCCO GIOVANNI, and GAMBACORTI PASSERINI, CARLO

Abstract

ALK is involved in the onset of several tumors. Crizotinib (XalkoriTM), a potent ALK inhibitor, represents the current front-line treatment for ALK+ NSCLC and shows great clinical efficacy. However, resistant disease often develops after initial response. ASP3026 is a novel second-generation ALK inhibitor with activity on crizotinib-resistant ALK-L1196M gatekeeper mutant. As resistance is likely to be a relevant hurdle for any drug, we sought to determine the resistance profile of ASP3026 in the context of NPM/ALK+ ALCL. We selected six ASP3026-resistant cell lines by culturing human ALCL cells in the presence of increasing concentrations of drug. The established resistant cell lines carry several point mutations in the ALK kinase domain (G1128S, C1156F, I1171N/T, F1174I, N1178H, E1210K and C1156F/D1203N were the most frequent) that are shown to confer resistance to ASP3026 in the Ba/F3 cell model. All mutants were profiled for cross-resistance against a panel of clinically relevant inhibitors including ceritinib, alectinib, crizotinib, AP26113 and PF-06463922. Finally, a genetically heterogeneous ASP3026-resistant cell line was exposed to second-line treatment simulations with all inhibitors. The population evolved according to relative sensitivity of its mutant subclones to the various drugs. Compound PF-06463922 did not allow the outgrowth of any resistant clone, at non-toxic doses.

Published
2015

32. Treatment efficacy and resistance mechanisms using the second-generation ALK inhibitor AP26113 in human NPM-ALK-positive anaplastic large cell lymphoma

Author

Ceccon, M, Mologni, L, Giudici, G, Piazza, R, Pirola, A, Fontana, D, GAMBACORTI PASSERINI, C, CECCON, MONICA, MOLOGNI, LUCA, PIAZZA, ROCCO GIOVANNI, PIROLA, ALESSANDRA, FONTANA, DILETTA, GAMBACORTI PASSERINI, CARLO, Ceccon, M, Mologni, L, Giudici, G, Piazza, R, Pirola, A, Fontana, D, GAMBACORTI PASSERINI, C, CECCON, MONICA, MOLOGNI, LUCA, PIAZZA, ROCCO GIOVANNI, PIROLA, ALESSANDRA, FONTANA, DILETTA, and GAMBACORTI PASSERINI, CARLO

Abstract

ALK is a tyrosine kinase receptor involved in a broad range of solid and hematologic tumors. Among 70% to 80% of ALK+ anaplastic large cell lymphomas (ALCL) are caused by the aberrant oncogenic fusion protein NPM-ALK. Crizotinib was the first clinically relevant ALK inhibitor, now approved for the treatment of late-stage and metastatic cases of lung cancer. However, patients frequently develop drug resistance to Crizotinib, mainly due to the appearance of point mutations located in the ALK kinase domain. Fortunately, other inhibitors are available and in clinical trial, suggesting the potential for second-line therapies to overcome Crizotinib resistance. This study focuses on the ongoing phase I/II trial small-molecule tyrosine kinase inhibitor (TKI) AP26113, by Ariad Pharmaceuticals, which targets both ALK and EGFR. Two NPM-ALK+ human cell lines, KARPAS-299 and SUP-M2, were grown in the presence of increasing concentrations of AP26113, and eight lines were selected that demonstrated resistance. All lines show IC50 values higher (130 to 1,000-fold) than the parental line. Mechanistically, KARPAS-299 populations resistant to AP26113 show NPM-ALK overexpression, whereas SUP-M2-resistant cells harbor several point mutations spanning the entire ALK kinase domain. In particular, amino acid substitutions: L1196M, S1206C, the double F1174V+L1198F and L1122V+L1196M mutations were identified. The knowledge of the possible appearance of new clinically relevant mechanisms of drug resistance is a useful tool for the management of new TKI-resistant cases. Implications: This work defines reliable ALCL model systems of AP26113 resistance and provides a valuable tool in the management of all cases of relapse upon NPM-ALK-targeted therapy. Mol Cancer Res; 13(4); 775-83.

Published
2015

33. Abstract 2920: Excess of cytoplasmic NPM-ALK driven oncogenic signaling is toxic and promotes cellular apoptosis and drug dependency

Author

Ceccon, M, Boggio Merlo, M, Mologni, L, Varesio, L, Poggio, T, Menotti, M, Bombelli, S, Rigolio, R, Manazza, A, Ambrogio, C, Giudici, G, Casati, C, Compagno, M, Turner, S, Gambacorti Passerini, C, Chiarle, R, Voena, C, Boggio Merlo, ME, CASATI, COSTANZA, Ceccon, M, Boggio Merlo, M, Mologni, L, Varesio, L, Poggio, T, Menotti, M, Bombelli, S, Rigolio, R, Manazza, A, Ambrogio, C, Giudici, G, Casati, C, Compagno, M, Turner, S, Gambacorti Passerini, C, Chiarle, R, Voena, C, Boggio Merlo, ME, and CASATI, COSTANZA

Published
2015

34. Activity of second-generation ALK inhibitors against crizotinib-resistant mutants in an NPM-ALK model compared to EML4-ALK

Author

Fontana, D, Ceccon, M, GAMBACORTI PASSERINI, C, Mologni, L, FONTANA, DILETTA, CECCON, MONICA, GAMBACORTI PASSERINI, CARLO, MOLOGNI, LUCA, Fontana, D, Ceccon, M, GAMBACORTI PASSERINI, C, Mologni, L, FONTANA, DILETTA, CECCON, MONICA, GAMBACORTI PASSERINI, CARLO, and MOLOGNI, LUCA

Abstract

Anaplastic lymphoma kinase (ALK) is a tyrosine kinase receptor involved in both solid and hematological tumors. About 80% of ALK-positive anaplastic large-cell lymphoma (ALCL) cases are characterized by the t(2;5)(p23;q35) translocation, encoding for the aberrant fusion protein nucleophosmin (NPM)-ALK, whereas 5% of non-small-cell lung cancer (NSCLC) patients carry the inv(2)(p21;p23) rearrangement, encoding for the echinoderm microtubule-associated protein-like 4 (EML4)-ALK fusion. The ALK/c-MET/ROS inhibitor crizotinib successfully improved the treatment of ALK-driven diseases. However, several cases of resistance appeared in NSCLC patients, and ALK amino acid substitutions were identified as a leading cause of resistance to crizotinib. Second-generation ALK inhibitors have been developed in order to overcome crizotinib resistance. In this work, we profiled in vitro the activity of crizotinib, AP26113, ASP3026, alectinib, and ceritinib against six mutated forms of ALK associated with clinical resistance to crizotinib (C1156Y, L1196M, L1152R, G1202R, G1269A, and S1206Y) and provide a classification of mutants according to their level of sensitivity/resistance to the drugs. Since the biological activity of ALK mutations extends beyond the specific type of fusion, both NPM-ALK- and EML4-ALK-positive cellular models were used. Our data revealed that most mutants may be targeted by using different inhibitors. One relevant exception is represented by the G1202R substitution, which was highly resistant to all drugs (>10-fold increased IC50 compared to wild type) and may represent the most challenging mutation to overcome. These results provide a prediction of cross-resistance of known crizotinib-resistant mutations against all second-generation tyrosine kinase inhibitors (TKIs) clinically available, and therefore could be a useful tool to help clinicians in the management of crizotinib-resistance cases.

Published
2015

35. Reversal of microRNA-150 silencing disadvantages crizotinib-resistant NPM-ALK(+) cell growth

Author

Hoareau Aveilla, C, Valentin, T, Daugrois, C, Quelen, C, Mitou, G, Quentin, S, Jia, J, Spicuglia, S, Ferrier, P, Ceccon, M, Giuriato, S, GAMBACORTI PASSERINI, C, Brousset, P, Lamant, L, Meggetto, F, Meggetto, F., CECCON, MONICA, GAMBACORTI PASSERINI, CARLO, Hoareau Aveilla, C, Valentin, T, Daugrois, C, Quelen, C, Mitou, G, Quentin, S, Jia, J, Spicuglia, S, Ferrier, P, Ceccon, M, Giuriato, S, GAMBACORTI PASSERINI, C, Brousset, P, Lamant, L, Meggetto, F, Meggetto, F., CECCON, MONICA, and GAMBACORTI PASSERINI, CARLO

Abstract

The regulatory microRNA miR-150 is involved in the development of hemopathies and is downregulated in T-lymphomas, such as anaplastic large-cell lymphoma (ALCL) tumors. ALCL is defined by the presence or absence of translocations that activate the anaplastic lymphoma kinase (ALK), with nucleophosmin-ALK (NPM-ALK) fusions being the most common. Here, we compared samples of primary NPM-ALK(+) and NPM-ALK(-) ALCL to investigate the role of miR-150 downstream of NPM-ALK. Methylation of the MIR150 gene was substantially elevated in NPM-ALK(+) biopsies and correlated with reduced miR-150 expression. In NPM-ALK(+) cell lines, DNA hypermethylation-mediated miR-150 repression required ALK-dependent pathways, as ALK inhibition restored miR-150 expression. Moreover, epigenetic silencing of miR-150 was due to the activation of STAT3, a major downstream substrate of NPM-ALK, in cooperation with DNA methyltransferase 1 (DNMT1). Accordingly, miR-150 repression was turned off following treatment with the DNMT inhibitor, decitabine. In murine NPM-ALK(+) xenograft models, miR-150 upregulation induced antineoplastic activity. Treatment of crizotinib-resistant NPM-ALK(+) KARPAS-299-CR06 cells with decitabine or ectopic miR-150 expression reduced viability and growth. Altogether, our results suggest that hypomethylating drugs, alone or in combination with other agents, may benefit ALK(+) patients harboring tumors resistant to crizotinib and other anti-ALK tyrosine kinase inhibitors (TKIs). Moreover, these results support further work on miR-150 in these and other ALK(+) malignancies.

Published
2015

36. Excess of NPM-ALK oncogenic signaling promotes cellular apoptosis and drug dependency

Author

Ceccon, M, primary, Merlo, M E Boggio, additional, Mologni, L, additional, Poggio, T, additional, Varesio, L M, additional, Menotti, M, additional, Bombelli, S, additional, Rigolio, R, additional, Manazza, A D, additional, Di Giacomo, F, additional, Ambrogio, C, additional, Giudici, G, additional, Casati, C, additional, Mastini, C, additional, Compagno, M, additional, Turner, S D, additional, Gambacorti-Passerini, C, additional, Chiarle, R, additional, and Voena, C, additional

Published
2015
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41. In Vitro and in Vivo Characterization of Bosutinib as Substrate of the Pglycoprotein Efflux Transporter

Author

Redaelli, S, Perini, P, Ceccon, M, Piazza, R, Rigolio, R, Boschelli, F, Giannoudis, A, GAMBACORTI PASSERINI, C, REDAELLI, SARA, PERINI, PIETRO, CECCON, MONICA, PIAZZA, ROCCO GIOVANNI, RIGOLIO, ROBERTA, GAMBACORTI PASSERINI, CARLO, Redaelli, S, Perini, P, Ceccon, M, Piazza, R, Rigolio, R, Boschelli, F, Giannoudis, A, GAMBACORTI PASSERINI, C, REDAELLI, SARA, PERINI, PIETRO, CECCON, MONICA, PIAZZA, ROCCO GIOVANNI, RIGOLIO, ROBERTA, and GAMBACORTI PASSERINI, CARLO

Published
2014

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

Author

GAMBACORTI PASSERINI, C, Farina, F, Stasia, A, Redaelli, S, Ceccon, M, Mologni, L, Messa, M, Guerra, L, Giudici, G, Sala, E, Mussolin, L, Deeren, D, King, M, Steurer, M, Ordemann, R, Cohen, A, Grube, M, Bernard, L, Chiriano, G, Antolini, L, Piazza, R, GAMBACORTI PASSERINI, CARLO, REDAELLI, SARA, CECCON, MONICA, MOLOGNI, LUCA, MESSA, MARIA CRISTINA, ANTOLINI, LAURA, PIAZZA, ROCCO GIOVANNI, GAMBACORTI PASSERINI, C, Farina, F, Stasia, A, Redaelli, S, Ceccon, M, Mologni, L, Messa, M, Guerra, L, Giudici, G, Sala, E, Mussolin, L, Deeren, D, King, M, Steurer, M, Ordemann, R, Cohen, A, Grube, M, Bernard, L, Chiriano, G, Antolini, L, Piazza, R, GAMBACORTI PASSERINI, CARLO, REDAELLI, SARA, CECCON, MONICA, MOLOGNI, LUCA, MESSA, MARIA CRISTINA, ANTOLINI, LAURA, and PIAZZA, ROCCO GIOVANNI

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 latest 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. ALK 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.

Published
2014

44. Crizotinib-resistan NPM-ALK mutants confer differential sensitivity to unrelated alk inhibitors

Author

MOLOGNI, LUCA, Ceccon, M, GAMBACORTI PASSERINI, CARLO, CECCON, MONICA, MOLOGNI, LUCA, Ceccon, M, GAMBACORTI PASSERINI, CARLO, and CECCON, MONICA

Abstract

The dual ALK/MET inhibitor Crizotinib was recently approved for the treatment of metastatic and late stage ALK+ NSCLC, and is currently in clinical trial for other ALK‐related diseases. As predicted after other TKIs clinical experience, the first mutations that confer resistance to Crizotinib have been described in Non Small Cell Lung Cancer (NSCLC) and in one Inflammatory Myofibroblastic Tumor (IMT) patients. Here we focused our attention on Anaplastic Large Cell Lymphoma (ALCL), where the oncogenic fusion protein NPM-ALK, responsible for 70-80% of cases, represents an ideal Crizotinib target. We selected and characterized two human NPM-ALK+ ALCL cell lines, KARPAS299 and SUP-M2, able to survive and proliferate at different Crizotinib concentrations. Sequencing of ALK kinase domain revealed that a single mutation became predominant at high Crizotinib doses in each cell line, namely L1196Q and I1171N in Karpas299 and SUP-M2 cells, respectively. These mutations also conferred resistance to Crizotinib in Ba/F3 cells expressing human NPM‐ALK. The resistant cell populations, as well as mutated Ba/F3 cells, were characterized for sensitivity to two additional ALK inhibitors: the dual ALK/EGFR inhibitor AP26113 and NVPTAE684. While L1196Q-positive cell lines were sensitive to both inhibitors, cells carrying I1171N substitution showed cross-resistance to all ALK inhibitors tested. This study provides potential relevant information for the management of ALCL patients that may relapse after Crizotinib treatment.

Published
2013

45. Crizotinib-Resistant NPM-ALK Mutants Confer Differential Sensitivity to Unrelated Alk Inhibitors

Author

Ceccon, M, Mologni, L, Bisson, W, Scapozza, L, GAMBACORTI PASSERINI, C, CECCON, MONICA, MOLOGNI, LUCA, GAMBACORTI PASSERINI, CARLO, Ceccon, M, Mologni, L, Bisson, W, Scapozza, L, GAMBACORTI PASSERINI, C, CECCON, MONICA, MOLOGNI, LUCA, and GAMBACORTI PASSERINI, CARLO

Abstract

The dual ALK/MET inhibitor crizotinib was recently approved for the treatment of metastatic and late-stage ALK+ NSCLC, and is currently in clinical trial for other ALK-related diseases. As predicted after other tyrosine kinase inhibitors' clinical experience, the first mutations that confer resistance to crizotinib have been described in patients with non-small cell lung cancer (NSCLC) and in one patient inflammatory myofibroblastic tumor (IMT). Here, we focused our attention on the anaplastic large cell lymphoma (ALCL), where the oncogenic fusion protein NPM-ALK, responsible for 70% to 80% of cases, represents an ideal crizotinib target. We selected and characterized 2 human NPM-ALK+ ALCL cell lines, KARPAS-299 and SUP-M2, able to survive and proliferate at different crizotinib concentrations. Sequencing of ALK kinase domain revealed that a single mutation became predominant at high crizotinib doses in each cell line, namely L1196Q and I1171N in Karpas-299 and SUP-M2 cells, respectively. These mutations also conferred resistance to crizotinib in Ba/F3 cells expressing human NPM-ALK. The resistant cell populations, as well as mutated Ba/F3 cells, were characterized for sensitivity to two additional ALK inhibitors: the dual ALK/EGFR inhibitor AP26113 and NVP-TAE684. While L1196Q-positive cell lines were sensitive to both inhibitors, cells carrying I1171N substitution showed cross-resistance to all ALK inhibitors tested. This study provides potentially relevant information for the management of patients with ALCL that may relapse after crizotinib treatment

Published
2013

46. Three novel patients derived BCR/ABL mutants show different sensitivity to second and third generation tyrosine kinase inhibitors

Author

Redaelli, S, Mologni, L, Rostagno, R, Piazza, R, Magistroni, V, Ceccon, M, Viltadi, M, Flynn, D, GAMBACORTI PASSERINI, C, REDAELLI, SARA, MOLOGNI, LUCA, ROSTAGNO, ROBERTA, PIAZZA, ROCCO GIOVANNI, MAGISTRONI, VERA, CECCON, MONICA, VILTADI, MICHELA, GAMBACORTI PASSERINI, CARLO, Redaelli, S, Mologni, L, Rostagno, R, Piazza, R, Magistroni, V, Ceccon, M, Viltadi, M, Flynn, D, GAMBACORTI PASSERINI, C, REDAELLI, SARA, MOLOGNI, LUCA, ROSTAGNO, ROBERTA, PIAZZA, ROCCO GIOVANNI, MAGISTRONI, VERA, CECCON, MONICA, VILTADI, MICHELA, and GAMBACORTI PASSERINI, CARLO

Abstract

BCR/ABL (Breakpoint Cluster Region protein/Abelson tyrosine-protein kinase 1) kinase domain (KD) mutations represent the most frequently described mechanism of resistance to the treatment with tyrosine kinase inhibitors (TKI) in patients with chronic myeloid leukemia (CML). Mutations may impair TKI activity by directly or indirectly impairing the drug binding to the protein. We report the discovery of three new BCR/ABL mutations, L248R, T315V, and F317R identified in two patients with CML (L248R and T315V) and in one patient with Ph1 acute lymphoblastic leukemia (ALL) (F317R). Mutations were screened against second-generation (bosutinib, nilotinib, and dasatinib), as well as third-generation TKIs (ponatinib/AP-24534 and DCC-2036). Furthermore, the activity profile of ponatinib and DCC-2036 against a panel of 24 clinically relevant BCR/ABL mutants is presented and compared to the other TKIs. The IC50 values for each TKI against the mutants and the IC50 increase over wild type BCR/ABL (relative resistance, RR) were calculated to define four resistance levels: sensitive (RR 2), moderately resistant (2 < RR 4), resistant (4 < RR 10), or highly resistant (RR > 10). L248R and T315V showed high resistance to imatinib, bosutinib, dasatinib, and nilotinib, intermediate resistance to ponatinib, but were sensitive to DCC-2036. Interestingly, F317R showed a moderate resistance to imatinib and nilotinib, but is resistant/highly resistant to dasatinib, bosutinib, ponatinib, and DCC-2036. The availability of drugs activity profiles may become a useful tool for clinicians dealing with the treatment of drug-resistant CML patients

Published
2012

47. Colorectal tumors are effectively eradicated by combined inhibition of {beta}-catenin, KRAS, and the oncogenic transcription factor ITF2

Author

Mologni, L, Dekhil, H, Ceccon, M, Purgante, S, Lan, C, Cleris, L, Magistroni, V, Formelli, F, GAMBACORTI PASSERINI, C, MOLOGNI, LUCA, CECCON, MONICA, PURGANTE, STEFANIA, MAGISTRONI, VERA, GAMBACORTI PASSERINI, CARLO, Mologni, L, Dekhil, H, Ceccon, M, Purgante, S, Lan, C, Cleris, L, Magistroni, V, Formelli, F, GAMBACORTI PASSERINI, C, MOLOGNI, LUCA, CECCON, MONICA, PURGANTE, STEFANIA, MAGISTRONI, VERA, and GAMBACORTI PASSERINI, CARLO

Abstract

Colorectal carcinomas (CRC) harbor well-defined genetic abnormalities, including aberrant activation of beta-catenin (beta-cat) and KRAS, but independent targeting of these molecules seems to have limited therapeutic effect. In this study, we report therapeutic effects of combined targeting of different oncogenes in CRC. Inducible short hairpin RNA (shRNA)-mediated silencing of beta-cat, ITF2, or KRAS decreased proliferation by 88%, 72%, and 45%, respectively, with no significant apoptosis in any case. In contrast, combined blockade of beta-cat and ITF2 inhibited proliferation by 99% with massive apoptosis. Similar effects occurred after combined shRNA against beta-cat and KRAS. In vivo, single oncogene blockade inhibited the growth of established tumors by up to 30%, whereas dual beta-cat and ITF2 targeting caused 93% inhibition. Similar tumor growth suppression was achieved by double beta-cat/KRAS shRNA in vivo. Our findings illustrate an effective therapeutic principle in CRC based on a combination targeting strategy that includes the ITF2 oncogene, which represents a novel therapeutic target. Cancer Res; 70(18); 7253-63. (C)2010 AACR.

Published
2010

48. Resistance Profile of the BCR/ABL Inhibitor Bosutinib Using a High Throughput random Mutagenesis Assay

Author

Piazza, R, Redaelli, S, Ceccon, M, Mogavero, A, Marega, M, Mologni, L, Boschelli, F, Pogliani, E, GAMBACORTI PASSERINI, C, PIAZZA, ROCCO GIOVANNI, REDAELLI, SARA, CECCON, MONICA, MOLOGNI, LUCA, POGLIANI, ENRICO MARIA, GAMBACORTI PASSERINI, CARLO, Piazza, R, Redaelli, S, Ceccon, M, Mogavero, A, Marega, M, Mologni, L, Boschelli, F, Pogliani, E, GAMBACORTI PASSERINI, C, PIAZZA, ROCCO GIOVANNI, REDAELLI, SARA, CECCON, MONICA, MOLOGNI, LUCA, POGLIANI, ENRICO MARIA, and GAMBACORTI PASSERINI, CARLO

Published
2009

49. A DominantABCC8-Related Hyperinsulinism: Familial Case ReportMoreiraet al.ABCC8-Related Hyperinsulinism

Author

Moreira, M. C., primary, Piazzon, F. B., additional, Carvalho, M. D. F., additional, Quaio, C. R. D. C., additional, Dutra, A. B., additional, Ceccon, M. E., additional, Della-Manna, T., additional, Tannuri, U., additional, Lee, J. H., additional, Zerbini, M. C. N., additional, Bellanne-Chantelot, C., additional, Lonlay, P., additional, Bertola, D. R., additional, and Kim, C. A., additional

Published
2013
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