Your search keyword '"Giovanni Marconi"' showing total 159 results

151. Novel Genomic Patterns of Metabolic Remodeling in Acute Myeloid Leukemia

Author

Gabriele Fontanarosa, Cristina Papayannidis, Italo Faria do Valle, Simona Soverini, Antonella Padella, Maria Chiara Abbenante, Anna Maria Ferrari, Marianna Garonzi, Annalisa Astolfi, Emanuela Ottaviani, Alberto Ferrarini, Elisa Zuffa, Giovanni Marconi, Elisa Zago, Eugenia Franchini, Giovanni Martinelli, Maria Chiara Fontana, Barbara Sinigaglia, Giorgia Simonetti, Elisa Dan, Michele Cavo, Massimo Delledonne, Daniel Remondini, Viviana Guadagnuolo, Ilaria Iacobucci, Samantha Bruno, Simonetti, Giorgia, Padella, Antonella, FARIA DO VALLE, Italo, Fontanarosa, Gabriele, Zago, Elisa, Garonzi, Marianna, Papayannidis, Cristina, Abbenante, Mariachiara, Marconi, Giovanni, Guadagnuolo, Viviana, Fontana, MARIA CHIARA, Bruno, Samantha, Ferrari, Anna, Zuffa, Elisa, Franchini, Eugenia, Astolfi, Annalisa, Dan, Elisa, Sinigaglia, Barbara, Iacobucci, Ilaria, Soverini, Simona, Cavo, Michele, Ottaviani, Emanuela, Ferrarini, Alberto, Delledonne, Massimo, Remondini, Daniel, and Martinelli, Giovanni

Subjects

Neuroblastoma RAS viral oncogene homolog, Genetics, Mutation, Acute leukemia, Immunology, Myeloid leukemia, Cell Biology, Hematology, Acute Myeloid Leukemia, Metabolism, Biology, medicine.disease, medicine.disease_cause, Biochemistry, Leukemia, Metabolic pathway, medicine, KRAS, Gene

Abstract

Metabolic remodeling of cancer is controlled by metabolic enzymes having oncogenic or tumor suppressor functions, along with oncogenes and tumor suppressors, which cooperate with the tissue environment to define specific metabolic profiles (Yuneva et al. Cell met 2012). Dysregulated metabolic pathways contribute to the pathogenesis of Acute Myeloid Leukemia (AML), as demonstrated for IDH1/2 mutations, which force the production of the oncometabolite 2-Hydroxyglutarate (Ward et al. Cancer Cell 2010) and can be selectively targeted (Wang et al. Science 2013). However, the genetic determinants of leukemia metabolic plasticity are largely unexplored. To identify metabolism-related pathogenic mechanisms in AML, we screened 886 AML cases for targeted genomic alterations and performed Whole Exome Sequencing of 143 leukemia samples (100 bp paired-end, HiSeq2000, Illumina), focusing our analysis on 37 AML cases (34 at diagnosis and 3 at relapse). Mutations were called by MuTect and GATK. Moreover, transcriptional analysis was performed on bone marrow cells from 59 AML cases (≥80% blasts) and 7 healthy controls (HTA2.0, Affymetrix). By mapping the mutated genes into functional categories, we identified a previously undescribed class of mutations targeting metabolism-related genes, that we define metabolic acute leukemia genes (MALGs). MALG was the most represented category after signaling pathways (76/915 genomic alterations) and 29/37 patients carried at least one MALG mutation. MALG mutations mostly targeted biosynthesis and catabolism of lipids and of CoA (ACP2, PANK2), bioenergetic pathways, metabolism of amino acids and nucleotides (NUDT18, IMPDH2). Notably, IMPDH2 is a target of MYC, a known regulator of cancer cell metabolism, and balances the nucleotide pool required for DNA replication (Liu et al, Plos one 2008). IMPDH2 was not only mutated but also upregulated at mRNA level in AML compared with controls (p=0.0001), suggesting an oncogenic function of the gene in AML, which is under investigation. Moreover, MYC transcriptional network was affected by additional mutations targeting genes regulating MYC activity (HUWE1, ZBTB17, TRRAP) and degradation (HEPACAM). Mutations in amino acid metabolism affected the synthesis/degradation of serine (PHGDH), glycine (SHMT2), proline (PRODH), tryptophan(CYP1B1) and glutamate (OPLAH), with a glutamate-related metabolic signature being also enriched in AML. These results may be highly relevant to AML therapy, since they may identify patients suitable to glutaminase inhibitor treatment, which is under development by pharmaceutical companies. An additional subset of patients displayed mutations in glucose-dependent bioenergetic pathways: glycolysis (GPI), oxidative phosphorylation (ND1, ND4, ND5, CYTB) and pentose phosphate pathway (H6PD, PGLS). These mutations were mutually exclusive with KRAS/NRAS alterations, which were detected in 8/37 samples. Indeed, oncogenic KRAS stimulates glucose uptake and channeling of glucose intermediates into pentose phosphate pathway (Ying et al. Cell 2012). Mutations in the bioenergetic pathways occurred across different cytogenetic groups and were associated with a poor outcome in terms of overall survival (p=0.016 Fig.1) in our AML cohort. Along with mutations in KRAS- and MYC-oncogenic pathways, which are known to control metabolic processes, we identified a novel functional category of mutated genes involved in metabolism (MALG) in AML. Our results may suggest different types of metabolic remodeling across leukemia subgroups. Mutations targeting a common downstream metabolic pathway are mutually exclusive in our cohort, as shown by KRAS and genes involved in glucose-dependent bioenergetic processes. Glucose metabolism predicts clinical outcome and chemotherapy response in AML (Chen et al. Blood 2014). Our data further suggest that the mutational screening of glucose-related MALGs may define a new subgroup of patients, which could not be identified by cytogenetic analysis. These findings may have implication for AML treatment, since metabolic alterations and genomic determinants of metabolic remodeling are promising targets for tailored therapies, as recently shown for glutaminase and IDH1/2 inhibitors. Acknowledgments: EHA Research Fellowship award, FP7 NGS-PTL project, ELN, AIL, AIRC, progetto Regione-Università 2010-12 Disclosures Soverini: Novartis, Briston-Myers Squibb, ARIAD: Consultancy. Cavo:JANSSEN, CELGENE, AMGEN: Consultancy. Martinelli:Novartis: Consultancy, Speakers Bureau; Pfizer: Consultancy; MSD: Consultancy; Ariad: Consultancy; BMS: Consultancy, Speakers Bureau; ROCHE: Consultancy; AMGEN: Consultancy.

152. Blinatumomab is safe and effective in relapsed and MRD-positive B-ALL CD1 9+patients: The Bologna Compassionate Program Experience

Author

Andrea Ghelli Luserna di Rorà, Antonella Padella, Sarah Parisi, Alessandra Santoro, Chiara Sartor, Anna Maria Ferrari, Claudio Cerchione, Stefania Paolini, Enrica Imbrogno, Maria Chiara Fontana, Maria Chiara Abbenante, Simona Soverini, Giorgia Simonetti, Silvia Lo Monaco, Cristina Papayannidis, Caterina De Benedittis, Giovanni Martinelli, Valentina Robustelli, and Giovanni Marconi

Subjects

Cancer Research, medicine.medical_specialty, Oncology, biology, business.industry, Internal medicine, Incidence (epidemiology), medicine, biology.protein, Blinatumomab, business, CD19, medicine.drug

Abstract

e18522 Background: Adult B-ALL patients still have a dismal prognosis, due to a high incidence of relapse even after allogenic SCT. Safety and efficacy of Blinatumomab, anti CD3-CD19 Bite antibody, has been demonstrated both in MRD pos patients and in relapsed/refractory (R/R) setting. To evaluate safety profile and efficacy of Blinatumomab, obtained through a compassionate use, in a cohort of 18 adult patients affected by MRD+ or R/R B-ALL treated at Bologna University. Methods: From March 2015 to December 2017, 18 patients received Blinatumomab at the standard dosage (9 mcg/d x 7 days, 28 mcg/d x 21 days) in 28-days courses. All the patients were hospitalized to receive the 1st course of therapy. The following courses, based on the good safety profile of the compound, were administered in outpatient setting. 18 patients (M/F = 10/8; median age 43, r. 18-73) have been treated. Ph chromosome was detected in 8/18 . 10 were MRD+ (5 Ph pos and 5 Ph neg); E2A-PBX1 and MLL-AF4 rearrangements were found in two patients. 8 patients had a R/R disease (3 Ph pos/5 Ph neg). Median WBC count before starting therapy with Blinatumomab was 5400/mmc (r. 500-76500). All patients had previously received many lines of therapy (median 4, r. 1-7). In 4 cases an alloTMO was already performed, and two patients had received two transplants. 12/18 patients were referred to us by other Institutions. All the patients received at least one course of Blinatumomab. Bone marrow evaluations, including cytogenetics, molecular biology and immunophenotyping analysis were performed at the beginning of every course of therapy in order to assess patients' disease status. MRD evaluation was assessed through BCR-ABL fusion transcript quantitative analysis in Ph pos ALL patients and Ig rearrangment in Ph neg patients. Monitoring of adverse events was periodically performed. 16/18 patients are evaluable for response, at least to one cycle. Results: 9/16 (56%) patients obtained a CR (7/9 MRD+ and 2/7 R/R). In 7/9 (78%) responders patients a molecular CR was reached, (in 6 patients after the first course, in one case after the second one). 5 responders proceeded to alloBMT and are actually alive in CR (median follow-up after transplant 240 days). In terms of toxicity, one patient developed a grade IV neurological event (mental confusion, tremor), which completely resolved after a transient drug withdrawal. Conclusions: Our results confirm the high rate of response and to Blinatumomab in a poor patients' population, and the good management profile of the compound.

153. Very Poor Outcome and Chemoresistance of Acute Myeloid Leukemia Patients with TP53 Mutations: Correlation with Complex Karyotype and Clinical Outcome

Author

Sarah Parisi, Beatrice Anna Zannetti, Elisa Zuffa, Carmen Baldazzi, Giorgia Simonetti, Claudia Venturi, Eugenia Franchini, Chiara Sartor, Giovanni Martinelli, Nicoletta Testoni, Abbenante maria Chiara, A. Ferrari, Michele Cavo, Emanuela Ottaviani, Cristina Papayannidis, Katia Mancuso, Stefania Paolini, Margherita Perricone, Francesca Volpato, Viviana Guadagnuolo, Alberto Conficoni, Antonella Padella, Valentina Robustelli, Giovanni Marconi, Ilaria Iacobucci, Papayannidis, Cristina, Ferrari, Anna, Paolini, Stefania, Baldazzi, Carmen, Sartor, Chiara, Abbenante, Mariachiara, Marconi, Giovanni, Parisi, Sarah, Volpato, Francesca, Iacobucci, Ilaria, Padella, Antonella, Guadagnuolo, Viviana, Perricone, Margherita, Robustelli, Valentina, Venturi, Claudia, Simonetti, Giorgia, Conficoni, Alberto, Mancuso, Katia, Zannetti, BEATRICE ANNA, Ottaviani, Emanuela, Zuffa, Elisa, Franchini, Eugenia, Testoni, Nicoletta, Cavo, Michele, and Martinelli, Giovanni

Subjects

Oncology, Mutation rate, medicine.medical_specialty, NPM1, education.field_of_study, Immunology, Population, outcome clinico, leucemia acuta mieloide, Aneuploidy, Karyotype, Cell Biology, Hematology, Biology, medicine.disease, Bioinformatics, Biochemistry, Internal medicine, Complex Karyotype, medicine, education, Trisomy, Survival analysis

Abstract

Background: AML is a heterogeneous disease. The karyotype provides important prognostic information that influences therapy and outcome. Identification of AML patients (pts) with poor prognosis such as those with complex karyotype (CK) has great interest and impact on therapeutic strategies. TP53 is the most frequently mutated gene in human tumours. TP53 mutation rate in AML was reported to be low (2.1%), but the incidence of TP53 mutations in AML with a complex aberrant karyotype is still debated. Aims: To investigate the frequency of TP53 mutations in adult AML pts, the types of mutations, the associations with recurrent cytogenetic abnormalities and their relationship with response to therapy, clinical outcome and finally their prognostic role. To this aim, we focused on a subgroup of TOT/886 AML pts treated at the Serˆgnoli Institute of Bologna between 2002 and 2013. Patients and Methods: 886 AML patients were analysed for morphology, immunophenotype, cytogenetic and for a panel of genetic alterations (FLT3, NPM1, DNMT3A, IDH1, IDH2 mutations, WT-1 expression, CBF fusion transcripts). Of these, 172 adult AML pts were also examined for TP53 mutations using several methods, including Sanger sequencing, Next-Generation Deep-Sequencing (Roche) and HiSeq 2000 (Illumina) platform. 40 samples were genotyped with Genome-Wide Human SNP 6.0 arrays or with CytoScan HD Array (Affymetrix) and analysed by Nexus Copy Numberª v7.5 (BioDiscovery). Results: Of the 886 AML patients, 172 pts were screened for TP53 mutations. Sanger sequencing analysis detected TP53 mutations in 29/172 AML patients with 36 different types of mutations; seven pts (4%) had 2 mutations. At diagnosis, the median age of TP53 mutated and wild type patients was 68 years (range 42-86), and 65 years (range 22-97) respectively. Median WBC count was 8955/mmc (range 580-74360/mmc) and 1240/mmc (range 400-238000/mmc). Conventional cytogenetics showed that: a) 52 pts (30,2%) had 3 or more chromosome abnormalities, i.e. complex karyotype; b) 71 (41,3%) presented with one or two cytogenetic abnormalities (other-AML); c) 34 pts (19,8%) had normal karyotype. Most of the TP53 mutated pts (23/29, 79.3%) had complex karyiotype, whereas only 6/29 mutated pts had “no complex Karyotype” (21% and 3% of the entire screened population, respectively). Overall, TP53 frequency was 44.2% in the complex karyotype group, suggesting a pathogenetic role of TP53 mutations in this subgroup of leukemias. As far as the types of TP53 alterations regards, the majority of mutations (32) were deleterious.. Copy Number Alterations (CNAs) analysis performed on 40 cases by Affymetrix SNP arrays showed the presence of several CNAs in all cases: they ranged from loss or gain of the full chromosome (chr) arm to focal deletions and gains targeting one or few genes involving macroscopic (>1.5 Mbps), submicroscopic genomic intervals (50 Kbps - 1.5 Mbps) and LOH (>5 Mbps) events. Of relevance, gains located on chr 8 were statistically associated with TP53 mutations (p = 0.001). In addition to the trisomy of the chr 8, others CNAs, located on chromosomes 5q, 3, 12, 17 are significantly associated (p = 0.05) with TP53 mutations. WES analysis was performed in 37 pts: 32 TP53 were wt while 5 pts were TP53 mutated. Interestingly, TP53 mutated patients had more incidence of complex karyotype, more aneuploidy state, more number of somatic mutations (median mutation rate 30/case vs 10/case, respectively). Regarding the clinical outcome, as previously reported (Grossmann V. et Al. Blood 2013), alterations of TP53 were significantly associated with poor outcome in terms of both overall survival (median survival: 4 and 31 months in TP53 mutated and wild type patients, respectively; p Figure 1: Overall Survival curve of 172 AML patients with (red) or without (blue) TP53 mutations (p< 0.0001). Conclusions: Our data demonstrated that TP53 mutations are more frequent at diagnosis in the subgroup of complex karyotype AML (16.86%) (p< 0.0001–Fisher's exact test). They are mostly deleterious mutations and are significantly correlated with worst prognosis, fail to respond to therapy and rapidly progress. We recommend TP53 mutation screening at least in AML pts carrying either complex karyotype or chr. 8 gain. Supported by: ELN, AIL, AIRC, PRIN, progetto Regione-Universitˆ 2010-12 (L. Bolondi), FP7 NGS-PTL project. Disclosures No relevant conflicts of interest to declare.

154. Alterations in Pathways Regulating Phosphatidil Inositol 3 Phosphate (PI3P) Produce Both Cell Proliferation and Therapy Resistance, and Define a Group of Patients with Poor Prognosis in Acute Myeloid Leukemia (AML)

Author

Sarah Parisi, Chiara Sartor, Marco Manfrini, Elena Tenti, Maria Teresa Bochicchio, Antonella Padella, Simona Soverini, Margherita Perricone, Giorgia Simonetti, Nicoletta Testoni, Emanuela Ottaviani, Valentina Robustelli, Giovanni Marconi, Andrea Ghelli Luserna di Rorà, Francesca Volpato, Viviana Guadagnuolo, Eugenia Franchini, Giovanni Martinelli, Maria Chiara Fontana, Anna Maria Ferrari, Stefania Paolini, Maria Chiara Abbenante, Carmen Baldazzi, Silvia Lo Monaco, Cristina Papayannidis, Marconi, Giovanni, Papayannidis, Cristina, Fontana, MARIA CHIARA, Padella, Antonella, Simonetti, Giorgia, Manfrini, Marco, Ferrari, Anna, Franchini, Eugenia, Paolini, Stefania, Parisi, Sarah, Sartor, Chiara, Abbenante, Mariachiara, LO MONACO, Silvia, Volpato, Francesca, Tenti, Elena, Guadagnuolo, Viviana, Perricone, Margherita, Bochicchio, MARIA TERESA, GHELLI LUSERNA DI RORÀ, Andrea, Baldazzi, Carmen, Robustelli, Valentina, Testoni, Nicoletta, Soverini, Simona, Ottaviani, Emanuela, and Martinelli, Giovanni

Subjects

Cell growth, business.industry, Immunology, AMPK, Myeloid leukemia, Cancer, Cell Biology, Hematology, Mitochondrion, acute myeloid leukemia, Phosphate, medicine.disease, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Cytoplasm, 030220 oncology & carcinogenesis, Cancer research, Medicine, Inositol, business, 030215 immunology

Abstract

Introduction PI3P is a key regulator of cell growth, and mediates cell proliferation via PI3K/AKT/mTOR in response to various growth signals. Abnormal activation of genes in its pathway is associated to oncogenic activity and poor Overall Survival (OS). PI3P is also a core activator of autophagy. Which role autophagy plays in cancer is not well established; it can function as a pro-apoptotic mechanism, or it can improve survive to stresses clearing damaged mitochondria and proteins accumulation, preventing apoptosis. Levels and activity of pro-apoptotic and anti-apoptotic proteins, particularly bcl-2 and p53, membrane signaling via mTOR, high levels of cAMP, a complex made by pink/park, promote a switch from apoptotic autophagy toward a mechanism that augment cell resiliency. Our study aims to define the role of PI3P pathways in AML, and to establish if autophagy could reduce the patients' chance to respond to induction, and to worsen OS. Methods We analyzed 208 consecutive newly diagnosed non M3 AML patients, screened for TP53, FLT3, NMP1, IDH1, IDH2, and DNMT3A mutations. Remission status was assessed with bone marrow biopsy. In all the patients, we perform Microarray-based Comparative Genomic Hybridization with Affymetrix SNP array 6.0 or Cytoscan HD; we perform Whole Exome Sequencing (WES)in 80/208 patients. Survival data were collected prospectively, with a median follow-up of 18 months. Survival analysis was performed with Kaplan Meyer method using log rank test. Univariate and multivariable regression and Cox Hazard Ratio(HR) model was performed. Correlation between variables was assessed with Fisher's exact test. Results We analyzed 4 pathways (Table 1); we selected genes in pathways basing on literature and GO data. Alterations in these pathways involved 103/209 patients (48%). PI3K/AKT/mTOR pathway alterations (both gains or losses) were shown to confer worst OS (p = .035, Figure 1a) when compared with unaltered patients; events in these pathways did not affect therapy response. Autophagy pathway alterations were shown to confer worst OS (p AMPK pathway alterations were shown to confer worst OS (p Autophagy switch pathway confer worst OS to patients(p Having at least an altered pathway is associated with worst prognosis (p WES in a sub-cohort of patients did not found any significant mutation in genes we analyzed. This data is consistent with literature. Conclusions Our work investigates for the first time the role of PI3P pathways and autophagy in AML. Surprisingly, it showed that both positive and negative alterations in these pathways are associated with poor prognosis. Significantly, alterations in cAMP and autophagy pathways were associated with therapy resistance. These results point out that both positive and negative regulation of autophagy could worsen patients OS; a diminished autophagy could be linked to a hyper-proliferative state via activation of AKT/mTOR but an augmented autophagy could give cell resiliency, favoring cytoplasm turnover, damaged mitochondria elimination, and neutralizing oxidative damages to proteins. A pan-PI3K inhibitor could target these mechanisms and improve chemo-sensitivity in high risk AML. Acknowledgment: ELN, AIL, AIRC, PRIN, Progetto Regione-Università 2010-12 (L. Bolondi), FP7 NGS-PTL project. Disclosures Guadagnuolo: CellPly S.r.l.: Employment. Soverini:Ariad: Consultancy; Bristol-Myers Squibb: Consultancy; Novartis: Consultancy. Martinelli:Novartis: Speakers Bureau; MSD: Consultancy; Ariad: Consultancy, Speakers Bureau; BMS: Speakers Bureau; Celgene: Consultancy, Speakers Bureau; Pfizer: Consultancy, Speakers Bureau; Genentech: Consultancy; Roche: Consultancy, Speakers Bureau; Amgen: Consultancy, Speakers Bureau.

155. Gemtuzumab-Ozogamicin Containing Regimens As Induction Therapy Give the Highest Complete Remission Rate and the Longest Overall Survival Compared with Other Induction Regimens in Patients with Newly Diagnosed Acute Myeloid Leukemia

Author

Maria Teresa Bochicchio, Anna Maria Ferrari, Giovanni Marconi, Maria Chiara Abbenante, Maria Chiara Fontana, Michele Malagola, Emanuela Ottaviani, Antonella Padella, Viviana Guadagnuolo, Claudia Venturi, Giorgia Simonetti, Anna Candoni, Sarah Parisi, Marco Manfrini, Renato Fanin, Simona Soverini, Stefania Paolini, Chiara Sartor, Michele Cavo, Nicoletta Testoni, Domenico Russo, Carmen Baldazzi, Cristina Papayannidis, Elisa Zuffa, Eugenia Franchini, Giovanni Martinelli, Papayannidis, Cristina, Candoni, Anna, Malagola, Michele, Marconi, Giovanni, Manfrini, Marco, Simonetti, Giorgia, Zuffa, Elisa, Abbenante, Mariachiara, Parisi, Sarah, Paolini, Stefania, Sartor, Chiara, Franchini, Eugenia, Ottaviani, Emanuela, Venturi, Claudia, Fontana, MARIA CHIARA, Padella, Antonella, Guadagnuolo, Viviana, Bochicchio, MARIA TERESA, Ferrari, Anna, Soverini, Simona, Testoni, Nicoletta, Baldazzi, Carmen, Fanin, Renato, Russo, Domenico, Cavo, Michele, and Martinelli, Giovanni

Subjects

medicine.medical_specialty, Pediatrics, education.field_of_study, Gemtuzumab Ozogamicin, Acute Myeloid Leukemia, business.industry, Gemtuzumab ozogamicin, Proportional hazards model, Incidence (epidemiology), Immunology, Population, Cell Biology, Hematology, Biochemistry, Fludarabine, Exact test, Regimen, Internal medicine, medicine, Cytarabine, business, education, medicine.drug

Abstract

Introduction. Conventional induction treatment in young non APL-Acute Myeloid Leukemia (AML) patients is still represented by the association of an antracycline and Cytarabine, which offers a complete remission (CR) rate not inferior to 60%. The addition of Gemtuzumab Ozogamicin (GO) as a third or fourth drug, already demonstrated to improve clinical outcome, in terms of CR rates. Aims of the study. We retrospectively evaluated and compared the efficacy of different induction schedules, in terms of CR rates and Overall Survival (OS), administered to two groups of AML patients. Group 1 (n=139) was treated with a GO containing course (MyFLAI or MyAIE schedules); Group 2 (n=270) received a non-GO based regimen including or not Fludarabine (FLAI, FLAN, FLAG, 3+7 or DAE). Patients and Methods. From 1997 to 2014,409 newly diagnosed AML patients were treated in 3 Italian Institutions. Their median age was 53 (range 19-74) and 52 (range 17-75) years, respectively. According to karyotype (performed in 392/409 patients), FLT3 (available for 244/409 patients), and NPM1 mutational status (available for 157/409 patients), based on the NCCN-2013 risk stratification criteria, 35.2% of the patients were considered at High Risk (HR) (31.6% and 36.4% in the two groups, respectively) and 7.6% at low risk (LR) (7.8% and 7.0%, respectively). Results. The complete remission (CR) rate after induction was 81.4% and 70.4% for Group 1 and 2, respectively (p=0.01). Deaths during induction (DDI), occurring in the first 50 days from 1st line therapy, were 4/139 (2.9%) in Group 1 and 22/270 (8.1%) in Group 2 (p=0.003). Patients treated with GO showed a better OS than patients of Group 2 (Figure 1); the 5-years OS in the two groups was 54.01% and 34.9%, respectively, and different according to age (54.0% and 34.9% respectively (p=0.0003) in patients Then, with a logistic univariate regression analysis.,we explored the impact of GO therapy in terms of CR rate. The use of GO was identified as a strong predictor of the achievement of a 1st CR (p=0.008). Moreover, a logistic multivariate regression analysis (risk and age) confirmed the role of the compound as a predictor of higher CR rate (p=0.013). We also performed a Cox Regression analysis, to investigate the impact of GO therapy, age and risk on OS: the use of GO was confirmed to be an independent predictor of better OS (p In a sub-analysis performed on HR patients, we observed a significantly better outcome in Group 1 than in Group 2 in terms of OS (p=0.0074, 5-year OS 47.7%; in group 2 OS 21.0% respectively, Figure 3) and EFS (p=0.001). However, there was no difference in terms of CR rate (p=ns). In particular, HR patients with adverse karyotype, may benefit from GO induction therapy in terms of OS (5-years OS 42.9% and 12.8% in Group 1 and 2, respectively, p=0.02); nevertheless FLT3 mutations negative impact canÕt be overcome by the drug administration (5-years OS 66.6% and 61.3% in Group 1 and 2, respectively). In SR AML, GO offered a better OS (p=0.036, 5-years OS 51.4% and 41.9% respectively). Comparing with Fisher's exact test the rate of increment in 5-years OS between Group1 and Group2 in HR and SR AML, we demonstrate that treatment with GO gave the higher benefit in HR AML (p=0.0005). Conclusions. These data showed that a four-drugs intensified induction therapy is a feasible approach in AML patients: adding GO at any induction regimen is an independent and strong predictor of better OS and higher CR rates. In our population, GO was not associated with a higher incidence of DDI. This approach, could be strongly recommended in SR and HR AML patients, due to karyotype abnormalities, in which showed an advantage in term of OS if compared with other standard regimens. On the contrary, we donÕt suggest the same schedule in FLT3 mutated patients, in which no benefits have been observed. Acknowledgments Work supported by ELN, AIL, AIRC, Progetto Regione-Universitˆ 2010-12 (L.Bolondi), FP7 NGS-PTL project. Figure 1. Figure 1. Figure 2. Figure 2. Figure 3. Figure 3. Disclosures Soverini: Novartis, Briston-Myers Squibb, ARIAD: Consultancy. Fanin:Novartis Farma: Speakers Bureau. Cavo:BMS: Honoraria; Millenium Pharmaceuticals: Honoraria; Jansenn: Consultancy, Honoraria; Sanofi: Consultancy, Honoraria; Onyx: Honoraria; Celgene: Consultancy, Honoraria; Novartis: Consultancy, Honoraria. Martinelli:Pfizer: Consultancy; BMS: Consultancy, Speakers Bureau; Novartis: Consultancy, Speakers Bureau; ROCHE: Consultancy; MSD: Consultancy; AMGEN: Consultancy; Ariad: Consultancy.

156. A Three-Genes Signature of Anti-Apoptotic Genes Showed Different Mechanisms in Preventing Apoptosis in Acute Myeloid Leukemia Cells and Could Provide an Useful Model to Establish the Proper BH3-Mimetich Drug or Combination

Author

Nanni, Jacopo, GIORGIA SIMONETTI, Marconi, Giovanni, Fontana, Maria Chiara, Bruno, Samantha, Papayannidis, Cristina, Padella, Antonella, Abbenante, Mariachiara, Lo Monaco, Silvia, Tenti, Elena, Sartor, Chiara, Parisi, Sarah, Martinelli, Giovanni, and Jacopo Nanni, Giorgia Simonetti, Giovanni Marconi, Maria Chiara Fontana, Samantha Bruno, Cristina Papayannidis, Antonella Padella, Mariachiara Abbenante, Silvia lo Monaco, Elena Tenti, Chiara Sartor, Sarah Parisi, Giovanni Martinelli

Subjects

Apoptosis, Acute Myeloid Leukemia

Published

2017

157. MHC-I Antigen Presentation Role in Immune Escape of Acute Myeloid Leukemia with High Burden of Genomic Aberration

Author

Marconi, Giovanni, Fontana, Maria Chiara, Fonzi, Eugenio, Papayannidis, Cristina, Abbenante, Mariachiara, Ottaviani, Emanuela, Testoni, Nicoletta, GIORGIA SIMONETTI, Padella, Antonella, Sartor, Chiara, Baldazzi, Carmen, Nanni, Jacopo, Bertamini, Luca, Di Rora, Andrea Ghelli Luserna, Robustelli, Valentina, Pazzaglia, Martina, Tenti, Elena, Parisi, Sarah, Martinelli, Giovanni, and Giovanni Marconi, Maria Chiara Fontana, Eugenio Fonzi, Cristina Papayannidis, Mariachiara Abbenante, Emanuela Ottaviani, Nicoletta Testoni, Giorgia Simonetti, Antonella Padella, Chiara Sartor, Carmen Baldazzi, Jacopo Nanni, Luca Bertamini, Andrea Ghelli Luserna Di Rora, Valentina Robustelli, Martina Pazzaglia, Elena Tenti, Sarah Parisi, Giovanni Martinelli

Subjects

Immune escape, Acute Myeloid Leukemia

158. Bromodomain Inhibition Is Effective Against Acute Myeloid Leukemia Cells Under Hypoxia and Induces Genome-Dependent Metabolic Perturbations

Author

GIORGIA SIMONETTI, Bruno, Samantha, Onofrillo, Carmine, Malferrari, Marco, Papayannidis, Cristina, Marconi, Giovanni, Cavo, Michele, Rapino, Stefania, Montanaro, Lorenzo, Martinelli, Giovanni, and Giorgia Simonetti, Samantha Bruno, Carmine Onofrillo, Marco Malferrari, Cristina Papayannidis, Giovanni Marconi, Michele Cavo, Stefania Rapino, Lorenzo Montanaro, Giovanni Martinelli

Subjects

Bromodomain, Acute Myeloid Leukemia

159. Blinatumomab Is Safe and Effective in Relapsed and MRD Positive B-ALL CD19+Patients: The Bologna Compassionate Program Experience

Author

CRISTINA PAPAYANNIDIS, Paolini, Stefania, Santoro, Alessandra, Robustelli, Valentina, Soverini, Simona, Benedittis, Caterina, Imbrogno, Enrica, Terragna, Carolina, Di Rora, Andrea Ghelli Luserna, Parisi, Sarah, Sartor, Chiara, Marconi, Giovanni, Lo Monaco, Silvia, Abbenante, Maria Chiara, Fontana, Maria Chiara, Padella, Antonella, Ferrari, Anna, Tenti, Elena, Simonetti, Giorgia, Frabetti, Federica, Volpato, Francesca, Baldazzi, Carmen, Martinelli, Giovanni, and Cristina Papayannidis, Stefania Paolini, Alessandra Santoro, Valentina Robustelli, Simona Soverini, Caterina De Benedittis, Enrica Imbrogno, Carolina Terragna, Andrea Ghelli Luserna Di Rora, Sarah Parisi, Chiara Sartor, Giovanni Marconi, Silvia Lo Monaco, Maria Chiara Abbenante, Maria Chiara Fontana, Antonella Padella, Anna Ferrari, Giorgia Simonetti, Elena Tenti, Federica Frabetti, Francesca Volpato, Carmen Baldazzi, Giovanni Martinelli

Subjects

Immunology, Cell Biology, Hematology, Biochemistry, Blinatumomab, Acute Lymphoblastic Leukemia

Abstract

Background: Adult B-ALL patients still have a dismal prognosis, due to a high incidence of relapse even after allogenic SCT. Safety and efficacy of Blinatumomab, an anti CD3-CD19 Bite antibody, has been demonstrated both in MRD positive patients and in relapsed/refractory (R/R) setting. Aim: To evaluate safety profile and efficacy of Blinatumomab, obtained through a compassionate use, in a cohort of 18 adult patients affected by MRD+ or R/R B-ALL treated at Bologna University. Design: From March 2015 to July 2016, 18 patients received Blinatumomab at the standard dosage (9 mcg/d x 7 days, 28 mcg/d x 21 days) in 28-days courses. All the patients were hospitalized to receive the first course of therapy. The following courses, based on the good safety profile of the compound, were administered in outpatient setting. Patients: 18 patients (M/F = 10/8; median age 43, range 18-73) have been treated. Philadelphia (Ph) chromosome was detected in 8/18 patients. 10 patients were MRD+ (5 Ph pos and 5 Ph neg); E2A-PBX1 and MLL-AF4 rearrangements were found in two patients. 8 patients had a R/R disease (3 Ph pos and 5 Ph neg). Median WBC count before starting therapy with Blinatumomab was 5400/mmc (range 500-76500). All the patients had previously received many lines of therapy (median 4, range 1-7). In 4 cases an alloTMO was already performed, and two patients had received two transplants. 12/18 patients were referred to us by other Italian Institutions. All the patients received at least one course of Blinatumomab. In one case three courses were administered; an elderly patient is actually receiving the fifth course. Globally, 32 courses of therapy have been administered (median 2, range 1-5). Bone marrow evaluations, including cytogenetics, molecular biology and immunophenotyping analysis were performed at the beginning of every course of therapy in order to assess patients' disease status. MRD evaluation was assessed through BCR-ABL fusion transcript quantitative analysis in Ph pos ALL patients and Ig rearrangment in Ph negative patients. Monitoring of adverse events was periodically performed. Results: 16/18 patients are evaluable for response, at least to one cycle (one patient died during the first course, one patient is still receiving the first course). 9/16 (56%) patients obtained a CR (7/9 MRD+ and 2/7 R/R). In 7/9 (78%) responders patients a molecular CR was reached, (in 6 patients after the first course, in one case after the second one). 5 responders proceeded to alloBMT and are actually alive in CR (median follow-up after transplant 240 days). In terms of toxicity, one patient developed a grade IV neurological event (mental confusion, tremor), which completely resolved after a transient drug withdrawal. Conclusions: Our results confirm the high rate of response and to Blinatumomab in a poor patients' population, and the good management profile of the compound. Acknowledgments: Work supported by ALN, AIL, AIRC, PRIN, Progetto Regione-Università 2010-12 (L. Bolondi), FP7 NGS-PTL project. Disclosures Soverini: Ariad: Consultancy; Bristol-Myers Squibb: Consultancy; Novartis: Consultancy.