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2. Predicting the date of budbreak of grapevine grown in the « Serra Gaucha » region

Author

F. Mandelli, M. Antonio Berlato, J. Tonietto, and H. Bergamaschi

Subjects
grapevine, budbreak, modelling, Agriculture, Botany, QK1-989
Abstract

Predicting the date of budbreak allows a more organized and rational pruning, defining lire time for winter phythosanitary treatments and, if necessary, the application of products to improve homogeneous sprouting and to increase the percentage of budbreak. The objective of the work was to validate the predicting date of grapevine budbreak model developed by Pouget, in France, for the conditions of Bento Gonçalves, state of Rio Grande do Sul, Brazil. To achieve this purpose, daily meteorological data of air minimum and maximum températures (°C), from 1984 to 1999, were taken from the agroclimatological station located near the experiment. The phenological data of 20 grapevine cultivars were obtained from the Embrapa Grape and Wine Germoplasm Active Bank. The phenological évaluations for each cultivar were performed on six grapevines conducted in a high vertical trellis and pnined in a bounded double Guyot. For each year, winter pruning and cultural practices were done in the same date for ail cultivars. This methodology is based on the effects of température on the sprouting velocity, on the relationships between the sum of températures and the number of days up to sprouting, and between the precocity coefficient of sprouting and the sum of température. To obtain these relationships, the same cultivars used by Pouget were taken into account, being the June lst the date considered for the beginning of the sum of temperature. Results show that the methodology of Pouget may be applied either for the "Serra Gaucha" conditions, with the possibility to predict the date of sprouting with two or three weeks earlier, depending on the cultivar and on the year, which permit the grower a better winter pruning planning.

Published
2003
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3. CAROTENOID INTERCONVERSION IN LIGHT-DARK CULTURES OF THE DINOFLAGELLATE AMPHIDINIUM KLEBSII(1)

Author

E F, Mandelli

Abstract

The carotenoid pigments of Amphidinium klebsii cultures grown in LD 12:12 light regimes were determined in cells harvested during the log phase growth in the dark and light photoperiods. The analysis of the individual pigments revealed the presence of an endogenous redox carotenoid system involving the epoxide carotenoid diadinoxanthin and an unidentified carotenoid with the properties of a dihydroxy xanthophyll.

Published
2016

4. CAROTENOID PIGMENTS OF THE DINOFLAGELLATE GLENODINIUM FOLIACEUM STEIN(1) (2)

Author

E F, Mandelli

Abstract

The marine dinoflagellate, Glenoclinium foliaceum Stein, has been shown to contain fucoxanthin, instead of peridinin, as the major xanthophyll. In addition, 2 carotenes-β-carotene and a compound with spectral properties reminiscent of isomerized y-carotene-and 2 xanthophylls-diadinoxanthin and an unidentified compound-were also isolated. These results support an earlier work that indicated the possible presence of fucoxanthin in some members of the Pyrrophyta.

Published
2016

5. Therapy of essential thrombocythemia with alpha-interferon: Results and prospects

Author

E. Morra, A. Gagliardi, A. Castello, Carlo Bernasconi, A. Vitale, M. Lazzarino, Paolo Bernasconi, F. Mandelli, C. Torromeo, D. Inverardi, and V. L. Burgio

Subjects
business.industry, Essential thrombocythemia, Alpha interferon, Hematology, General Medicine, Pharmacology, medicine.disease, Recombinant Proteins, Leukemogenic, Hematologic Response, Interferon Type I, Immunology, Megakaryocytosis, Humans, Cytotoxic T cell, Medicine, Thrombopoiesis, Cytotoxicity, business, Thrombocythemia, Essential
Abstract

Conventional treatment of symptomatic essential thrombocythemia (ET) consists of long-term administration of myelosuppressive cytotoxic agents which, although efficacious in most cases, are associated with leukemogenic potential. Alpha-interferon (IFN) exerts a dose-dependent inhibitory influence on thrombopoiesis through a direct antiproliferative effect on megakaryocytic precursors. Therefore, it may provide a biologic, potentially non-mutagenic alternative to conventional cytotoxic treatments. At daily doses ranging from 1 to 5 M.U., alpha-IFN is efficacious in inducing a hematologic response in most patients with ET. Response to IFN is a gradual process. The median time to hematologic response varies from 1 to 3 months and a significant proportion of patients reach and maintain normal platelet counts with low doses (1–3 M.U./d). Normalization of marrow megakaryocytosis requires longer treatment (9–12 months). Also patients resistant to cytotoxic drugs may respond to alpha-IFN, suggesting a lack of cross-resistance between the two treatment modalities. Side-effects, although not severe, represents a limit to the administration of adequate doses of IFN in about 25% of cases. Once hematologic response has been obtained, both low-dose IFN and cytotoxic drugs are effective as maintenance. The full potentialities of alpha-IFN in ET in combination with cytotoxic drugs or with other cytokines need to be further investigated.

Published
2009

6. GIMEMA ALL 0183: a multicentric study on adult acute Iymphoblastic lecukaemia in Italy

Author

F. Mandelli

Subjects
Response rate (survey), medicine.medical_specialty, Multivariate analysis, business.industry, Incidence (epidemiology), Complete remission, Hematology, Disease, Surgery, medicine.anatomical_structure, Induction Death, Internal medicine, medicine, Methotrexate, Bone marrow, business, medicine.drug
Abstract

Summary In 1983 a multicentre trial for adult patients with ALL (excluding the B-phenotype) was initi,ated to evaluate: (a) complete remission (CR) rate and length in a protocol with a mild induction and an intensive consolidation therapy; (b) the efficacy of a mild versus an intensive post consolidation treatment in prolonging disease-free survival; (c) CNS relapse rate on a protocol substituting intrathecal chemotherapy and intermediate dose i.v. methotrexate (MTX) and cytosine arabinoside (ARA-C) for cranial radiotherapy. 358 patients entered the protocol between January 1983 and April 1987: 284 (79.3%) attained complete remission, 26 (7.3%) died during induction and 48 (13.4%) had resistant disease. Median overall survival was 21.7 months, with a projection that 29.4% of the patients will survive more than 55 months. The median duration of complete remission was 19.2 months: 21.9% of responders are projected to remain in continuing complete response for more than 50.6 months. Among the 284 responding patients, 154 (54.2%) relapsed (95 while on therapy, 59 off-therapy): major sites of relapse were bone marrow (103). CNS alone (23), or both (11). 14 patients died while in CR. Only 12 patients (2.2%) were lost to follow-up, while therapy was interrupted in 7 (2%) because of side effects and in 12 (3.3%) because of the patient's refusal. By multivariate analysis increasing age and presence of infection at diagnosis were associated with a lower remission rate: risk of relapse was greater in LL subtypes and in patients with higher WBC at diagnosis; survival was inversely correlated to age. The high response rate was not achieved at expense of an increased risk of induction death. The low incidence of isolated CNS relapse (8.0% of responding patients) suggests that CNS prophylaxis as used in this study is effective. No statistically significant difference in survival and relapse rate emerged between the two arms of post consolidation therapy. Moreover, the protocol therapy was well tolerated, required minimal supportive care, which could be provided even in small centres, and compliance proved acceptance for patients and staff.

Published
2008

7. Accuracy of physician assessment of treatment preferences and health status in elderly patients with higher-risk myelodysplastic syndromes

Author

F. Mandelli, Emanuele Angelucci, Giuseppe A. Palumbo, Stefano Molica, Giovanni Caocci, Rosangela Invernizzi, F. Efficace, Alessandra Ricco, Grazia Sanpaolo, Uwe Platzbecker, Marianna Criscuolo, Pasquale Niscola, Massimo Breccia, G. La Nasa, Michael Lübbert, Francesco Buccisano, Khanh Thi-Thuy Nguyen, Gianluca Gaidano, Huiyong Zhang, Susanna Fenu, Odile Beyne-Rauzy, Maria Teresa Voso, Francesco Cottone, Gregory A. Abel, and Reinhard Stauder

Subjects
Adult, Male, Cancer Research, medicine.medical_specialty, Poor prognosis, Concordance, Health Status, Decision Making, Myelodysplastic syndromes, Quality of life (healthcare), Risk Factors, Physicians, Surveys and Questionnaires, medicine, Physician perception, Humans, Patient participation, Cancer, Aged, Aged, 80 and over, Physician-Patient Relations, business.industry, Geriatric assessment, Patient Preference, Decision making, Health status, Hematology, Oncology, Middle Aged, medicine.disease, Patient preference, Settore MED/15 - MALATTIE DEL SANGUE, Family medicine, Physical therapy, Quality of Life, Female, Perception, Patient Participation, business
Abstract

Higher-risk myelodysplastic syndromes (MDS) are rarely curable and have a poor prognosis. We investigated the accuracy of physicians’ perception of patients’ health status and the patients’ preferences for involvement in treatment decisions. We examined 280 newly diagnosed higher-risk elderly MDS patients paired with their physicians. Survey tools included the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire-Core 30 (EORTC QLQ-C30) and the Control Preference Scale. Overall concordance was 49% for physician perception of patient preferences for involvement in treatment decisions. In 36.4% of comparisons there were minor differences and in 14.6% there were major differences. In 44.7% of the patients preferring a passive role, physicians perceived them as preferring an active or collaborative role. Absence of the patient's request for prognostic information ( P = 0.001) and judging the patient as having a poor health status ( P = 0.036) were factors independently associated with the physicians’ attitude toward a lower degree of patient involvement in clinical decisions. Agreement on health status was found in 27.5% of cases. Physicians most frequently tended to overestimate health status of patients who reported low-level health status. The value of decision aid-tools in the challenging setting of higher-risk MDS should be investigated to further promote patient-centered care.

Published
2015

8. Alpha-2b recombinant interferon (Intron) in Hodgkin's lymphoma: Therapeutic perspective

Author

P. Mazza, S. Tura, M. Bocchia, P. L. Zinzani, F. Gherlinzoni, F. Mandelli, M. P. Anselmo, G. Papa, M. Antimi, P. G. Gobbi, A. Porcellini, V. Rizzoli, L. Resegotti, A. Levis, L. Deriu, A. Chierichini, F. Ciccone, R. Fanin, G. Castoldi, G. L. Scapoli, V. Liso, T. Chisesi, L. Rancan, and B. Amurri

Subjects
Adult, Male, medicine.medical_specialty, medicine.medical_treatment, Phases of clinical research, Interferon alpha-2, Gastroenterology, law.invention, Randomized controlled trial, law, Internal medicine, Humans, Medicine, business.industry, Interferon-alpha, Combination chemotherapy, Hematology, General Medicine, Hodgkin's lymphoma, medicine.disease, Hodgkin Disease, Recombinant Proteins, Surgery, Clinical trial, Radiation therapy, ABVD, Toxicity, Drug Evaluation, Female, business, medicine.drug
Abstract

In an ongoing phase II study we are evaluating the role of alpha-2b recombinant interferon in Hodgkin's disease; the study design includes patients with high-risk parameters who are treated by combination chemotherapy MOPP, ABVD, MOPP + ABVD or equivalent combinations. At the end of the therapeutic program which could include also radiotherapy, patients will be randomly assigned to receive alpha-2b interferon at 3 MU/day over 3 months and then 3 MU/three times/week over 9 months or no further treatment. Up to September 1989, 107 patients were randomized; evaluable patients with a minimum follow-up of 3 months are 95, 56 in the arm of interferon and 39 in the arm of no further treatment. The results are preliminary and differences could not be disclosed between the two arms concerning either the relapse rate or the incidence of infections. Tolerance and toxicity due to alpha-2b interferon in patients with Hodgkin's disease could be defined as acceptably good considering that mild and reversible hematological toxicity was experienced in 12 (21%) patients; objective clinical toxicity was recorded in 4 (7%) patients although 7 (12%) patients refused to continue the treatment. Definite conclusions will be drawn when 100 patients per arm become evaluable.

Published
2009

11. Phase III Comparative Trial Uisng CHOP vs CIOP in the Treatment of Advanced Intermediate-Grade Non-Hodgkin's Lymphoma

Author

P. L. Zinzani, M. Martelli, S. Storti, M. Musso, M. Cantonetti, G. Leone, A. Cajozzo, G. Papa, E. Iannitto, A. Perrotti, M. Bendandi, F. Gherlinzoni, P. Gentilini, G. Rossi, E. Aitini, F. Mandelli, and S. Tura

Subjects
Adult, Male, Cancer Research, medicine.medical_specialty, Vincristine, Heart Diseases, Cyclophosphamide, CHOP, Gastroenterology, hemic and lymphatic diseases, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, CHOP REGIMEN, CIOP REGIMEN, IDARUBICIN, INTERMEDIATE-GRADE NON-HODGKINS LYMPHOMA, COMPLETE RESPONSE, medicine, Humans, Idarubicin, Aged, business.industry, Lymphoma, Non-Hodgkin, Hematology, Middle Aged, medicine.disease, Survival Analysis, Surgery, Lymphoma, Non-Hodgkin's lymphoma, Clinical trial, Regimen, Oncology, Doxorubicin, Prednisone, Female, business, medicine.drug
Abstract

Until now, literature data support the fact that the CHOP regimen represents the standard first line treatment for patients with advanced intermediate-grade non-Hodgkin's lymphoma. Recently, idarubicin has been introduced in clinical trials because of its favourable preclinical profile: it is more active than daunorubicin and doxorubicin against a number of experimental tumour systems and is significantly less cardiotoxic in animal models. From March 1991 to June 1993, 115 previously untreated patients with stage II to IV intermediate-grade non-Hodgkin's lymphoma, according to the Kiel classification, were enrolled in a phase III comparative trial. The objectives of the study were to compare the efficacy and safety of using idarubicin instead of doxorubicin in the polychemotherapeutic regimen CHOP (cyclophosphamide, doxorubicin, vincristine, and dexamethasone). Of the 115 patients registered for the trial, 103 were evaluable: 52 received CH (doxorubicin)OP and 51 received CI(Idarubicin)OP. Known prognostic factors were equally distributed among the two groups. There were no significant differences between the 2 groups in the rates of partial and complete response. The overall response rate was 87%, with complete response in 62%: 63% in the CHOP group, and 59% in the CIOP group. At 30 months (median 20 months), 86% of all CR patients were alive without disease in the CHOP group and 85% in the CIOP group. Patients treated with CHOP experienced severe alopecia more frequently (P = .004). Only three patients in the CIOP group showed cardiac adverse events (1 moderate and 2 mild), while in the CHOP group 4 mild, 2 moderate and 1 severe were recorded. LVEF monitoring was carried out in 31 patients of the CHOP group and in 27 of the CIOP group. A median drop of 8.3% of the LVEF was observed in patients treated with CHOP regimen as compared to 4.8% in patients with CIOP regimen (P = .0001). In this trial, the "idarubicin arm" (CIOP regimen) was found to have an equivalent therapeutic efficacy and, slightly, reduced clinical toxicity in comparison to the standard doxorubicin-containing CHOP regimen in patients with intermediate-grade non-Hodgkin's lymphoma.

Published
1995

12. Peg-Interferon a-2b in Essential Thrombocythaemia: phase II study for determination of the minimum effective, safe and tolerated dose, preliminary data

Author

L. GUGLIOTTA, D. RUSSO, S. BULGARELLI, N. VIANELLI, S. CAGLIO, S. SACCHI, S. RUPOLI, F. PASSAMONTI, A. BUCALOSSI, E. DE BIASI, R. CACCIOLA, E. CACCIOLA, A. CANDONI, L. VALDR, R. CIANCIA, L. BARULLI, V. AGOSTINI, G. FINAZZI, R. LATAGLIATA, A. TABILIO, L. MARCOMIGNI, M. MIGLINO, G. PALAZZO, A. MOLINARI, A. GROSSI, M. G. MAZZUCCONI, M. GOBBI, M. MARTELLI, A. ZACCARIA, P. MAZZA, M. BOCCADORO, R. GIUSTOLISI, F. LAURIA, M. LAZZARINO, P. LEONI, B. ROTOLI, F. MANDELLI, G. FINCATO, M. BACCARANI, MARTINELLI, VINCENZO, L., Gugliotta, D., Russo, S., Bulgarelli, N., Vianelli, S., Caglio, Martinelli, Vincenzo, S., Sacchi, S., Rupoli, F., Passamonti, A., Bucalossi, E., DE BIASI, R., Cacciola, E., Cacciola, A., Candoni, L., Valdr, R., Ciancia, L., Barulli, V., Agostini, G., Finazzi, R., Latagliata, A., Tabilio, L., Marcomigni, M., Miglino, G., Palazzo, A., Molinari, A., Grossi, M. G., Mazzucconi, M., Gobbi, M., Martelli, A., Zaccaria, P., Mazza, M., Boccadoro, R., Giustolisi, F., Lauria, M., Lazzarino, P., Leoni, B., Rotoli, F., Mandelli, G., Fincato, and M., Baccarani

Abstract

HAEMATHOLOGICA, VOL 86 (SUPPL) N.RO 10

Published
2001

13. A controlled trial of recombinant human erythropoietin after bone marrow transplantation

Author

AA Fauser, M.A. Boogaerts, S Slavin, F. Mandelli, AM Carella, N. C. Gorin, Augustin Ferrant, Hartmut Link, J Reiffers, and S. Burdach

Subjects
medicine.medical_specialty, Chemotherapy, Hematology, Randomization, business.industry, medicine.medical_treatment, Immunology, Cell Biology, Placebo, Gastroenterology, Biochemistry, Surgery, medicine.anatomical_structure, Erythropoietin, Multicenter trial, Internal medicine, medicine, Erythropoiesis, Bone marrow, business, medicine.drug
Abstract

Recombinant human erythropoietin (rHuEPO) stimulates erythropoietic bone marrow cells and increases erythrocyte production. This prospective study was designed to evaluate the effects of rHuEPO on regeneration of erythropoiesis after allogeneic or autologous bone marrow transplantation (BMT). Seventeen centers participated in this randomized, double-blind, placebo-controlled multicenter trial. The randomization was performed centrally for each center and stratified according to allogeneic or autologous BMT and major ABO-blood group incompatibility. One hundred and six patients received rHuEPO after allogeneic BMT and 109 patients received placebo. After autologous BMT, 57 patients were treated with rHuEPO and 57 with placebo. Patients received either 150 IU/kg/day C127 mouse-cell-derived rHuEPO or placebo as continuous intravenous infusion. Therapy started after bone marrow infusion and lasted until independence from erythrocyte transfusions for 7 consecutive days with stable hemoglobin levels greater than or equal to 9 g/100 mL or until day 41. After allogeneic BMT, the reticulocyte counts were significantly higher with rHuEPO from day 21 to day 42 after BMT. The median time (95% confidence intervals) to erythrocyte transfusion independence was 19 days (range, 16.3 to 21.6) with rHuEPO and 27 days (range, 22.3 to > 42) with placebo (P < .003). The mean (+/-SD) numbers of erythrocyte transfusions until day 20 after BMT were 6.6 +/- 4.8 with rHuEPO and 6.0 +/- 3.8 with placebo. However, from day 21 to day 41, the rHuEPO-treated patients received 1.4 +/- 2.5 (median, 0) transfusions and the control group received 2.7 +/- 4.0 (median, 2) transfusions (P = .004). In the follow-up period from day 42 up to day 100, 2.4 +/- 5.6 transfusions were required with rHuEPO and 4.5 +/- 9.6 were required with placebo (P =.075). A multivariate analysis (ANOVA) showed that acute graft-versus-host disease (GVHD), major ABO-blood group incompatibility, age greater than 35 years, and hemorrhage significantly increased the number of transfusions. However, after day 20, rHuEPO significantly reduced the number of erythrocyte transfusions in these patient groups, as well as reducing incompatibility in the major ABO-blood group. For the whole study period, rHuEPO reduced the transfusion requirements in GVHD III and IV from 18.4 +/- 8.6 to 8.5 +/- 6.8 U (P = .05). After autologous BMT, there was no difference in the time to independence from erythrocyte transfusions and in the regeneration of reticulocytes. Marrow purging strongly increased the requirement for transfusions as well as the time to transfusion independence. rHuEPO had no relevant effect on regeneration of thrombopoiesis after allogeneic or autologous BMT. Overall, no major differences in side effects or complications between rHuEPO-treated and placebo-treated patients occurred. After allogeneic BMT, rHuEPO significantly accelerates the reconstitution of erythropoiesis and reduces the number of erythrocyte transfusions after day 20. The strongest effect occurs in patients with acute GVHD. After autologous BMT, rHuEPO has no clinically relevant effect on regeneration of erythropoiesis. (C) 1994 by The American Society of Hematology.

Published
1994

14. Hair Dye Use and Other Risk Factors for Leukemia and Pre-leukemia: A Case-Control Study

Author

F. Mandelli, Moyses Szklo, Giuseppe Visani, Alfonso Mele, G Castelli, Paolo Pasquini, and Stazi Ma

Subjects
medicine.medical_specialty, Myeloid, Epidemiology, business.industry, Anemia, Preleukemia, Myeloid leukemia, medicine.disease, Leukemia, Myelogenous, medicine.anatomical_structure, hemic and lymphatic diseases, Acute lymphocytic leukemia, Internal medicine, Immunology, medicine, Refractory anemia with excess of blasts, business
Abstract

A case-control study was carried out to examine the relation of three subtypes of leukemia cells and refractory anemia with excess of blasts to selected behavioral and environmental factors. Cases aged 15 years or older were recruited in three hospitals located in Rome, Bologna, and Pavia, respectively. Outpatients who were either normal or had nonneoplastic hematologic disorders and were seen in the same hospitals as the cases were enrolled as controls. Two hundred fifty-two patients with acute myeloid leukemia, 100 with acute lymphocytic leukemia, 111 with refractory anemia with excess of blasts, 156 with chronic myeloid leukemia, and 1,161 controls were included in the study. Refractory anemia with excess of blasts and chronic myeloid leukemia were included because they are regarded as forms of pre-leukemia. Odds ratio estimates were generally imprecise, but associations were suggested between specific case subtypes and exposure to dark hair dye, selected occupations (shoemaker, painter, electrician, child care), residence in houses built with tuff, and smoking. Although the exploratory nature of the study and its limited statistical power preclude firm conclusions, its results are consistent with those of previous studies, and are in general biologically plausible.

Published
1994

15. A layer correlation technique for pion energy calibration at the 2004 ATLAS Combined Beam Test

Author

Abat, E. Abdallah, J.M. Addy, T.N. Adragna, P. Aharrouche, M. Ahmad, A. Akesson, T.P.A. Aleksa, M. Alexa, C. Anderson, K. Andreazza, A. Anghinolfi, F. Antonaki, A. Arabidze, G. Arik, E. Atkinson, T. Baines, J. Baker, O.K. Banfi, D. Baron, S. Barr, A.J. Beccherle, R. Beck, H.P. Belhorma, B. Bell, P.J. Benchekroun, D. Benjamin, D.P. Benslama, K. Bergeaas Kuutmann, E. Bernabeu, J. Bertelsen, H. Binet, S. Biscarat, C. Boldea, V. Bondarenko, V.G. Boonekamp, M. Bosman, M. Bourdarios, C. Broklova, Z. Burckhart Chromek, D. Bychkov, V. Callahan, J. Calvet, D. Canneri, M. Capéans Garrido, M. Caprini, M. Cardiel Sas, L. Carli, T. Carminati, L. Carvalho, J. Cascella, M. Castillo, M.V. Catinaccio, A. Cauz, D. Cavalli, D. Cavalli Sforza, M. Cavasinni, V. Cetin, S.A. Chen, H. Cherkaoui, R. Chevalier, L. Chevallier, F. Chouridou, S. Ciobotaru, M. Citterio, M. Clark, A. Cleland, B. Cobal, M. Cogneras, E. Conde Muino, P. Consonni, M. Constantinescu, S. Cornelissen, T. Correard, S. Corso Radu, A. Costa, G. Costa, M.J. Costanzo, D. Cuneo, S. Cwetanski, P. Da Silva, D. Dam, M. Dameri, M. Danielsson, H.O. Dannheim, D. Darbo, G. Davidek, T. De, K. Defay, P.O. Dekhissi, B. Del Peso, J. Del Prete, T. Delmastro, M. Derue, F. Di Ciaccio, L. Di Girolamo, B. Dita, S. Dittus, F. Djama, F. Djobava, T. Dobos, D. Dobson, M. Dolgoshein, B.A. Dotti, A. Drake, G. Drasal, Z. Dressnandt, N. Driouchi, C. Drohan, J. Ebenstein, W.L. Eerola, P. Efthymiopoulos, I. Egorov, K. Eifert, T.F. Einsweiler, K. El Kacimi, M. Elsing, M. Emelyanov, D. Escobar, C. Etienvre, A.I. Fabich, A. Facius, K. Fakhr-Edine, A.I. Fanti, M. Farbin, A. Farthouat, P. Fassouliotis, D. Fayard, L. Febbraro, R. Fedin, O.L. Fenyuk, A. Fergusson, D. Ferrari, P. Ferrari, R. Ferreira, B.C. Ferrer, A. Ferrere, D. Filippini, G. Flick, T. Fournier, D. Francavilla, P. Francis, D. Froeschl, R. Froidevaux, D. Fullana, E. Gadomski, S. Gagliardi, G. Gagnon, P. Gallas, M. Gallop, B.J. Gameiro, S. Gan, K.K. Garcia, R. Garcia, C. Gavrilenko, I.L. Gemme, C. Gerlach, P. Ghodbane, N. Giakoumopoulou, V. Giangiobbe, V. Giokaris, N. Glonti, G. Goettfert, T. Golling, T. Gollub, N. Gomes, A. Gomez, M.D. Gonzalez-Sevilla, S. Goodrick, M.J. Gorfine, G. Gorini, B. Goujdami, D. Grahn, K.-J. Grenier, P. Grigalashvili, N. Grishkevich, Y. Grosse-Knetter, J. Gruwe, M. Guicheney, C. Gupta, A. Haeberli, C. Haertel, R. Hajduk, Z. Hakobyan, H. Hance, M. Hansen, J.D. Hansen, P.H. Hara, K. Harvey Jr., A. Hawkings, R.J. Heinemann, F.E.W. Henriques Correia, A. Henss, T. Hervas, L. Higon, E. Hill, J.C. Hoffman, J. Hostachy, J.Y. Hruska, I. Hubaut, F. Huegging, F. Hulsbergen, W. Hurwitz, M. Iconomidou-Fayard, L. Jansen, E. Jen-La Plante, I. Johansson, P.D.C. Jon-And, K. Joos, M. Jorgensen, S. Joseph, J. Kaczmarska, A. Kado, M. Karyukhin, A. Kataoka, M. Kayumov, F. Kazarov, A. Keener, P.T. Kekelidze, G.D. Kerschen, N. Kersten, S. Khomich, A. Khoriauli, G. Khramov, E. Khristachev, A. Khubua, J. Kittelmann, T.H. Klingenberg, R. Klinkby, E.B. Kodys, P. Koffas, T. Kolos, S. Konovalov, S.P. Konstantinidis, N. Kopikov, S. Korolkov, I. Kostyukhin, V. Kovalenko, S. Kowalski, T.Z. Krüger, K. Kramarenko, V. Kudin, L.G. Kulchitsky, Y. Lacasta, C. Lafaye, R. Laforge, B. Lampl, W. Lanni, F. Laplace, S. Lari, T. Le Bihan, A.-C. Lechowski, M. Ledroit-Guillon, F. Lehmann, G. Leitner, R. Lelas, D. Lester, C.G. Liang, Z. Lichard, P. Liebig, W. Lipniacka, A. Lokajicek, M. Louchard, L. Lourerio, K.F. Lucotte, A. Luehring, F. Lund-Jensen, B. Lundberg, B. Ma, H. Mackeprang, R. Maio, A. Maleev, V.P. Malek, F. Mandelli, L. Maneira, J. Mangin-Brinet, M. Manousakis, A. Mapelli, L. Marques, C. Garcia, S.M. Martin, F. Mathes, M. Mazzanti, M. McFarlane, K.W. McPherson, R. Mchedlidze, G. Mehlhase, S. Meirosu, C. Meng, Z. Meroni, C. Mialkovski, V. Mikulec, B. Milstead, D. Minashvili, I. Mindur, B. Mitsou, V.A. Moed, S. Monnier, E. Moorhead, G. Morettini, P. Morozov, S.V. Mosidze, M. Mouraviev, S.V. Moyse, E.W.J. Munar, A. Myagkov, A. Nadtochi, A.V. Nakamura, K. Nechaeva, P. Negri, A. Nemecek, S. Nessi, M. Nesterov, S.Y. Newcomer, F.M. Nikitine, I. Nikolaev, K. Nikolic-Audit, I. Ogren, H. Oh, S.H. Oleshko, S.B. Olszowska, J. Onofre, A. Padilla Aranda, C. Paganis, S. Pallin, D. Pantea, D. Paolone, V. Parodi, F. Parsons, J. Parzhitskiy, S. Pasqualucci, E. Passmored, S.M. Pater, J. Patrichev, S. Peez, M. Perez Reale, V. Perini, L. Peshekhonov, V.D. Petersen, J. Petersen, T.C. Petti, R. Phillips, P.W. Pina, J. Pinto, B. Podlyski, F. Poggioli, L. Poppleton, A. Poveda, J. Pralavorio, P. Pribyl, L. Price, M.J. Prieur, D. Puigdengoles, C. Puzo, P. Røhne, O. Ragusa, F. Rajagopalan, S. Reeves, K. Reisinger, I. Rembser, C. Bruckmande Renstrom, P.A. Reznicek, P. Ridel, M. Risso, P. Riu, I. Robinson, D. Roda, C. Roe, S. Rohne, O. Romaniouk, A. Rousseau, D. Rozanov, A. Ruiz, A. Rusakovich, N. Rust, D. Ryabov, Y.F. Ryjov, V. Salto, O. Salvachua, B. Salzburger, A. Sandaker, H. Santamarina Rios, C. Santi, L. Santoni, C. Saraiva, J.G. Sarri, F. Sauvage, G. Says, L.P. Schaefer, M. Schegelsky, V.A. Schiavi, C. Schieck, J. Schlager, G. Schlereth, J. Schmitt, C. Schultes, J. Schwemling, P. Schwindling, J. Seixas, J.M. Seliverstov, D.M. Serin, L. Sfyrla, A. Shalanda, N. Shaw, C. Shin, T. Shmeleva, A. Silva, J. Simion, S. Simonyan, M. Sloper, J.E. Smirnov, S.Yu. Smirnova, L. Solans, C. Solodkov, A. Solovianov, O. Soloviev, I. Sosnovtsev, V.V. Spaǹo, F. Speckmayer, P. Stancu, S. Stanek, R. Starchenko, E. Straessner, A. Suchkov, S.I. Suk, M. Szczygiel, R. Tarrade, F. Tartarelli, F. Tas, P. Tayalati, Y. Tegenfeldt, F. Teuscher, R. Thioye, M. Tikhomirov, V.O. Timmermans, C.J.W.P. Tisserant, S. Toczek, B. Tremblet, L. Troncon, C. Tsiareshka, P. Tyndel, M. Karagoez Unel, M. Unal, G. Unel, G. Usai, G. Van Berg, R. Valero, A. Valkar, S. Valls, J.A. Vandelli, W. Vannucci, F. Vartapetian, A. Vassilakopoulos, V.I. Vasilyeva, L. Vazeille, F. Vernocchi, F. Vetter-Cole, Y. Vichou, I. Vinogradov, V. Virzi, J. Vivarelli, I. De Vivie, J.B. Volpi, M. Vu Anh, T. Wang, C. Warren, M. Weber, J. Weber, M. Weidberg, A.R. Weingarten, J. Wells, P.S. Werner, P. Wheeler, S. Wiessmann, M. Wilkens, H. Williams, H.H. Wingerter-Seez, I. Yasu, Y. Zaitsev, A. Zenin, A. Zenis, T. Zenonos, Z. Zhang, H. Zhelezko, A. Zhou, N.

Subjects
Physics::Instrumentation and Detectors, High Energy Physics::Experiment
Abstract

A new method for calibrating the hadron response of a segmented calorimeter is developed and successfully applied to beam test data. It is based on a principal component analysis of energy deposits in the calorimeter layers, exploiting longitudinal shower development information to improve the measured energy resolution. Corrections for invisible hadronic energy and energy lost in dead material in front of and between the calorimeters of the ATLAS experiment were calculated with simulated Geant4 Monte Carlo events and used to reconstruct the energy of pions impinging on the calorimeters during the 2004 Barrel Combined Beam Test at the CERN H8 area. For pion beams with energies between 20GeV and 180GeV, the particle energy is reconstructed within 3% and the energy resolution is improved by between 11% and 25% compared to the resolution at the electromagnetic scale. © 2011 CERN for the benefit of the ATLAS collaboration, published under license by IOP Publishing Ltd and SISSA.

Published
2011

16. Photon reconstruction in the ATLAS Inner Detector and Liquid Argon Barrel Calorimeter at the 2004 Combined Test Beam

Author

Abat, E. Abdallah, J. M. Addy, T. N. Adragna, P. and Aharrouche, M. Ahmad, A. Akesson, T. P. A. Aleksa, M. and Alexa, C. Anderson, K. Andreazza, A. Anghinolfi, F. and Antonaki, A. Arabidze, G. Arik, E. Atkinson, T. Baines, J. Baker, O. K. Banfi, D. Baron, S. Barr, A. J. and Beccherle, R. Beck, H. P. Belhorma, B. Bell, P. J. and Benchekroun, D. Benjamin, D. P. Benslama, K. Kuutmann, E. Bergeaas Bernabeu, J. Bertelsen, H. Binet, S. Biscarat, C. Boldea, V. Bondarenko, V. G. Boonekamp, M. Bosman, M. and Bourdarios, C. Broklova, Z. Chromek, D. Burckhart and Bychkov, V. Callahan, J. Calvet, D. Canneri, M. Garrido, M. Capeans Caprini, M. Sas, L. Cardiel Carli, T. and Carminati, L. Carvalho, J. Cascella, M. Castillo, M. V. and Catinaccio, A. Cauz, D. Cavalli, D. Sforza, M. Cavalli and Cavasinni, V. Cetin, S. A. Chen, H. Cherkaoui, R. and Chevalier, L. Chevallier, F. Chouridou, S. Ciobotaru, M. and Citterio, M. Clark, A. Cleland, B. Cobal, M. Cogneras, E. Muino, P. Conde Consonni, M. Constantinescu, S. and Cornelissen, T. Correard, S. Radu, A. Corso Costa, G. and Costa, M. J. Costanzo, D. Cuneo, S. Cwetanski, P. Da Silva, D. Dam, M. Dameri, M. Danielsson, H. O. Dannheim, D. Darbo, G. Davidek, T. De, K. Defay, P. O. and Dekhissi, B. Del Peso, J. Del Prete, T. Delmastro, M. and Derue, F. Di Ciaccio, L. Di Girolamo, B. Dita, S. and Dittus, F. Djama, F. Djobava, T. Dobos, D. Dobson, M. and Dolgoshein, B. A. Dotti, A. Drake, G. Drasal, Z. and Dressnandt, N. Driouchi, C. Drohan, J. Ebenstein, W. L. and Eerola, P. Efthymiopoulos, I. Egorov, K. Eifert, T. F. and Einsweiler, K. El Kacimi, M. Elsing, M. Emelyanov, D. and Escobar, C. Etienvre, A. I. Fabich, A. Facius, K. and Fakhr-Edine, A. I. Fanti, M. Farbin, A. Farthouat, P. and Fassouliotis, D. Fayard, L. Febbraro, R. Fedin, O. L. and Fenyuk, A. Fergusson, D. Ferrari, P. Ferrari, R. and Ferreira, B. C. Ferrer, A. Ferrere, D. Filippini, G. and Flick, T. Fournier, D. Francavilla, P. Francis, D. and Froeschl, R. Froidevaux, D. Fullana, E. Gadomski, S. and Gagliardi, G. Gagnon, P. Gallas, M. Gallop, B. J. and Gameiro, S. Gan, K. K. Garcia, R. Garcia, C. Gavrilenko, I. L. Gemme, C. Gerlach, P. Ghodbane, N. Giakoumopoulou, V. Giangiobbe, V. Giokaris, N. Glonti, G. Goettfert, T. and Golling, T. Gollub, N. Gomes, A. Gomez, M. D. and Gonzalez-Sevilla, S. Goodrick, M. J. Gorfine, G. Gorini, B. and Goujdami, D. Grahn, K-J. Grenier, P. Grigalashvili, N. and Grishkevich, Y. Grosse-Knetter, J. Gruwe, M. Guicheney, C. Gupta, A. Haeberli, C. Haertel, R. Hajduk, Z. and Hakobyan, H. Hance, M. Hansen, J. D. Hansen, P. H. Hara, K. Harvey, Jr., A. Hawkings, R. J. Heinemann, F. E. W. and Correia, A. Henriques Henss, T. Hervas, L. Higon, E. and Hill, J. C. Hoffman, J. Hostachy, J. Y. Hruska, I. and Hubaut, F. Huegging, F. Hulsbergen, W. Hurwitz, M. and Iconomidou-Fayard, L. Jansen, E. Jen-La Plante, I. and Johansson, P. D. C. Jon-And, K. Joos, M. Jorgensen, S. and Joseph, J. Kaczmarska, A. Kado, M. Karyukhin, A. and Kataoka, M. Kayumov, F. Kazarov, A. Keener, P. T. and Kekelidze, G. D. Kerschen, N. Kersten, S. Khomich, A. and Khoriauli, G. Khramov, E. Khristachev, A. Khubua, J. and Kittelmann, T. H. Klingenberg, R. Klinkby, E. B. Kodys, P. and Koffas, T. Kolos, S. Konovalov, S. P. Konstantinidis, N. and Kopikov, S. Korolkov, I. Kostyukhin, V. Kovalenko, S. and Kowalski, T. Z. Krueger, K. Kramarenko, V. Kudin, L. G. and Kulchitsky, Y. Lacasta, C. Lafaye, R. Laforge, B. and Lampl, W. Lanni, F. Laplace, S. Lari, T. Le Bihan, A-C. and Lechowski, M. Ledroit-Guillon, F. Lehmann, G. Leitner, R. Lelas, D. Lester, C. G. Liang, Z. Lichard, P. and Liebig, W. Lipniacka, A. Lokajicek, M. Louchard, L. and Loureiro, K. F. Lucotte, A. Luehring, F. Lund-Jensen, B. and Lundberg, B. Ma, H. Mackeprang, R. Maio, A. Maleev, V. P. Malek, F. Mandelli, L. Maneira, J. Mangin-Brinet, M. and Manousakis, A. Mapelli, L. Marques, C. Marti i Garcia, S. Martin, F. Mathes, M. Mazzanti, M. McFarlane, K. W. and McPherson, R. Mchedlidze, G. Mehlhase, S. Meirosu, C. and Meng, Z. Meroni, C. Mialkovski, V. Mikulec, B. and Milstead, D. Minashvili, I. Mindur, B. Mitsou, V. A. and Moed, S. Monnier, E. Moorhead, G. Morettini, P. Morozov, S. V. Mosidze, M. Mouraviev, S. V. Moyse, E. W. J. and Munar, A. Myagkov, A. Nadtochi, A. V. Nakamura, K. and Nechaeva, P. Negri, A. Nemecek, S. Nessi, M. Nesterov, S. Y. Newcomer, F. M. Nikitine, I. Nikolaev, K. and Nikolic-Audit, I. Ogren, H. Oh, S. H. Oleshko, S. B. and Olszowska, J. Onofre, A. Aranda, C. Padilla Paganis, S. and Pallin, D. Pantea, D. Paolone, V. Parodi, F. Parsons, J. and Parzhitskiy, S. Pasqualucci, E. Passmored, S. M. Pater, J. Patrichev, S. Peez, M. Reale, V. Perez Perini, L. and Peshekhonov, V. D. Petersen, J. Petersen, T. C. Petti, R. and Phillips, P. W. Pilcher, J. Pina, J. Pinto, B. and Podlyski, F. Poggioli, L. Poppleton, A. Poveda, J. and Pralavorio, P. Pribyl, L. Price, M. J. Prieur, D. and Puigdengoles, C. Puzo, P. Ragusa, F. Rajagopalan, S. and Reeves, K. Reisinger, I. Rembser, C. de Renstrom, P. A. Bruckman Reznicek, P. Ridel, M. Risso, P. Riu, I. and Robinson, D. Roda, C. Roe, S. Rohne, O. Romaniouk, A. and Rousseau, D. Rozanov, A. Ruiz, A. Rusakovich, N. and Rust, D. Ryabov, Y. F. Ryjov, V. Salto, O. Salvachua, B. and Salzburger, A. Sandaker, H. Rios, C. Santamarina Santi, L. Santoni, C. Saraiva, J. G. Sarri, F. Sauvage, G. and Says, L. P. Schaefer, M. Schegelsky, V. A. Schiavi, C. and Schieck, J. Schlager, G. Schlereth, J. Schmitt, C. and Schultes, J. Schwemling, P. Schwindling, J. Seixas, J. M. and Seliverstov, D. M. Serin, L. Sfyrla, A. Shalanda, N. and Shaw, C. Shin, T. Shmeleva, A. Silva, J. Simion, S. and Simonyan, M. Sloper, J. E. Smirnov, S. Yu. Smirnova, L. and Solans, C. Solodkov, A. Solovianov, O. Soloviev, I. and Sosnovtsev, V. V. Spano, F. Speckmayer, P. Stancu, S. and Stanek, R. Starchenko, E. Straessner, A. Suchkov, S. I. and Suk, M. Szczygiel, R. Tarrade, F. Tartarelli, F. Tas, P. and Tayalati, Y. Tegenfeldt, F. Teuscher, R. Thioye, M. and Tikhomirov, V. O. Timmermans, C. J. W. P. Tisserant, S. and Toczek, B. Tremblet, L. Troncon, C. Tsiareshka, P. and Tyndel, M. Unel, M. Karagoez Unal, G. Unel, G. Usai, G. and Van Berg, R. Valero, A. Valkar, S. Valls, J. A. and Vandelli, W. Vannucci, F. Vartapetian, A. Vassilakopoulos, V. I. Vasilyeva, L. Vazeille, F. Vernocchi, F. and Vetter-Cole, Y. Vichou, I. Vinogradov, V. Virzi, J. and Vivarelli, I. de Vivie, J. B. Volpi, M. Anh, T. Vu Wang, C. Warren, M. Weber, J. Weber, M. Weidberg, A. R. and Weingarten, J. Wells, P. S. Werner, P. Wheeler, S. and Wiessmann, M. Wilkens, H. Williams, H. H. Wingerter-Seez, I. and Yasu, Y. Zaitsev, A. Zenin, A. Zenis, T. Zenonos, Z. and Zhang, H. Zhelezkobk, A. Zhou, N.

Subjects
Physics::Instrumentation and Detectors, High Energy Physics::Experiment
Abstract

The reconstruction of photons in the ATLAS detector is studied with data taken during the 2004 Combined Test Beam, where a full slice of the ATLAS detector was exposed to beams of particles of known energy at the CERN SPS. The results presented show significant differences in the longitudinal development of the electromagnetic shower between converted and unconverted photons as well as in the total measured energy. The potential to use the reconstructed converted photons as a means to precisely map the material of the tracker in front of the electromagnetic calorimeter is also considered. All results obtained are compared with a detailed Monte-Carlo simulation of the test-beam setup which is based on the same simulation and reconstruction tools as those used for the ATLAS detector itself.

Published
2011

17. Detection of ALL-1/AF4 fusion transcript by reverse transcription- polymerase chain reaction for diagnosis and monitoring of acute leukemias with the t(4;11) translocation

Author

Vincenzo Rossi, R Battista, Corrado Caslini, Alessandro Rambaldi, F Mandelli, L Elia, Andrea Biondi, T Barbui, Giuseppe Basso, and Giuseppe Masera

Subjects
Genetics, Immunology, Chromosomal translocation, Cell Biology, Hematology, Biology, Biochemistry, Molecular biology, Reverse transcription polymerase chain reaction, Fusion gene, Exon, Chromosome 4, Fusion transcript, Primer (molecular biology), Gene
Abstract

The chromosomal breakpoints of t(4;11) translocation of acute lymphoblastic leukemia (ALL) have been recently identified at molecular level and shown to involve the AF4 (FEL) gene on chromosome 4 and the ALL-1 (MLL, Hrx) gene on chromosome 11. The ALL-1/AF4 fusion gene is transcribed into a chimeric mRNA. Using primer sets derived from ALL-1 and AF4 cDNAs by reverse transcription-polymerase chain reaction (RT- PCR), we were able to amplify the breakpoint sites of the fusion transcript of all 15 ALL cases with karyotypic or molecular evidence of the t(4;11). DNA fragments of different size were obtained as the consequence of different breakpoints on chromosome 11 and the presence of alternative splicing of ALL-1 exon 8. The feasibility of monitoring the residual cells carrying the t(4;11) in 2 ALL patients with different clinical outcome was evaluated. Overall, the presented results provide evidence that RT-PCR can be used as a rapid method for detecting this chromosomal abnormality and following the patient's response to therapy.

Published
1993

18. Combined performance studies for electrons at the 2004 ATLAS combined test-beam

Author

Abat, E. Abdallah, J.M. Addy, T.N. Adragna, P. Aharrouche, M. Ahmad, A. Akesson, T.P.A. Aleksa, M. Alexa, C. Anderson, K. Andreazza, A. Anghinolfi, F. Antonaki, A. Arabidze, G. Arik, E. Atkinson, T. Baines, J. Baker, O.K. Banfi, D. Baron, S. Barr, A.J. Beccherie, R. Beck, H.P. Belhorma, B. Bell, P.J. Benchekroun, D. Benjamin, D.P. Benslama, K. Kuutmann, E.B. Bernabeu, J. Bertelsen, H. Binet, S. Biscarat, C. Boldea, V. Bondarenko, V.G. Boonekamp, M. Bosman, M. Bourdarios, C. Broklova, Z. Chromek, D.B. Bychkov, V. Callahan, J. Calvet, D. Canneri, M. Garrido, M.C. Caprini, M. Sas, L.C. Carli, T. Carminati, L. Carvalho, J. Cascella, M. Castillo, M.V. Catinaccio, A. Cauz, D. Cavalli, D. Sforza, M.C. Cavasinni, V. Cetin, S.A. Chen, H. Cherkaoui, R. Chevalier, L. Chevallier, F. Chouridou, S. Ciobotaru, M. Citterio, M. Clark, A. Cleland, B. Cobal, M. Cogneras, E. Muino, P.C. Consonni, M. Constantinescu, S. Cornelissen, T. Correard, S. Radu, A.C. Costa, G. Costa, M.J. Costanzo, D. Cuneo, S. Cwetanski, P. Da Silva, D. Dam, M. Dameri, M. Danielsson, H.O. Dannheim, D. Darbo, G. Davidek, T. De, K. Defay, P.O. Dekhissi, B. Del Peso, J. Del Prete, T. Delmastro, M. Derue, F. Di Ciaccio, L. Di Girolamo, B. Dita, S. Dittus, F. Djama, F. Djobava, T. Dobos, D. Dobson, M. Dolgoshein, B.A. Dotti, A. Drake, G. Drasal, Z. Dressnandt, N. Driouchi, C. Drohan, J. Ebenstein, W.L. Eerola, P. Efthymiopoulos, I. Egorov, K. Eifert, T.F. Einsweiler, K. El Kacimi, M. Elsing, M. Emelyanov, D. Escobar, C. Etienvre, A.I. Fabich, A. Facius, K. Fakhr-Edine, A.I. Fanti, M. Farbin, A. Farthouat, P. Fassouliotis, D. Fayard, L. Febbraro, R. Fedin, O.L. Fenyuk, A. Fergusson, D. Ferrari, P. Ferrari, R. Ferreira, B.C. Ferrer, A. Ferrere, D. Filippini, G. Flick, T. Fournier, D. Francavilla, P. Francis, D. Froeschl, R. Froidevaux, D. Fullana, E. Gadomski, S. Gagliardi, G. Gagnon, P. Gallas, M. Gallop, B.J. Gameiro, S. Gan, K.K. Garcia, R. Garcia, C. Gavrilenko, I.L. Gemme, C. Gerlach, P. Ghodbane, N. Giakoumopoulou, V. Giangiobbe, V. Giokaris, N. Glonti, G. Goettfert, T. Golling, T. Gollub, N. Gomes, A. Gomez, M.D. Gonzalez-Sevilla, S. Goodrick, M.J. Gorfine, G. Gorini, B. Goujdami, D. Grahn, K-J. Grenier, P. Grigalashvili, N. Grishkevich, Y. Grosse-Knetter, J. Gruwe, M. Guicheney, C. Gupta, A. Haeberli, C. Haertel, R. Hajduk, Z. Hakobyan, H. Hance, M. Hansen, J.D. Hansen, P.H. Hara, K. Harvey Jr., A. Hawkings, R.J. Heinemann, F.E.W. Henriques Correia, A. Henss, T. Hervas, L. Higon, E. Hill, J.C. Hoffman, J. Hostachy, J.Y. Hruska, I. Hubaut, F. Huegging, F. Hulsbergen, W. Hurwitz, M. Iconomidou-Fayard, L. Jansen, E. Jen-La Plante, I. Johansson, P.D.C. Jon-And, K. Joos, M. Jorgensen, S. Joseph, J. Kaczmarska, A. Kado, M. Karyukhin, A. Kataoka, M. Kayumov, F. Kazarov, A. Keener, P.T. Kekelidze, G.D. Kerschen, N. Kersten, S. Khomich, A. Khoriauli, G. Khramov, E. Khristachev, A. Khubua, J. Kittelmann, T.H. Klingenberg, R. Klinkby, E.B. Kodys, P. Koffas, T. Kolos, S. Konovalov, S.P. Konstantinidis, N. Kopikov, S. Korolkov, I. Kostyukhin, V. Kovalenko, S. Kowalski, T.Z. Krüger, K. Kramarenko, V. Kudin, L.G. Kulchitsky, Y. Lacasta, C. Lafaye, R. Laforge, B. Lampl, W. Lanni, F. Laplace, S. Lari, T. Le Bihan, A.-C. Lechowski, M. Ledroit-Guillon, F. Lehmann, G. Leitner, R. Lelas, D. Lester, C.G. Liang, Z. Lichard, P. Liebig, W. Lipniacka, A. Lokajicek, M. Louchard, L. Lourerio, K.F. Lucotte, A. Luehring, F. Lund-Jensen, B. Lundberg, B. Ma, H. Mackeprang, R. Maio, A. Maleev, V.P. Malek, F. Mandelli, L. Maneira, J. Mangin-Brinet, M. Manousakis, A. Mapelli, L. Marques, C. Marti i Garcia, S. Martin, F. Mathes, M. Mazzanti, M. McFarlane, K.W. McPherson, R. Mchedlidze, G. Mehlhase, S. Meirosu, C. Merigo, Z. Meroni, C. Mialkovski, V. Mikulec, B. Milstead, D. Minashvili, I. Mindur, B. Mitsou, V.A. Moed, S. Monnier, E. Moorhead, G. Morettini, P. Morozov, S.V. Mosidze, M. Mouraviev, S.V. Moyse, E.W.J. Munar, A. Myagkov, A. Nadtochi, A.V. Nakamura, K. Nechaeva, P. Negri, A. Nemecek, S. Nessi, M. Nesterov, S.Y. Newcomer, F.M. Nikitine, I. Nikolaev, K. Nikolic-Audit, I. Ogren, H. Oh, S.H. Oleshko, S.B. Olszowska, J. Onofre, A. Aranda, C.P. Paganis, S. Pallin, D. Pantea, D. Paolone, V. Parodi, F. Parsons, J. Parzhitskiy, S. Pasqualucci, E. Passmored, S.M. Pater, J. Patrichev, S. Peez, M. Reale, V.P. Perini, L. Peshekhonov, V.D. Petersen, J. Petersen, T.C. Petti, R. Phillips, P.W. Pina, J. Pinto, B. Podlyski, F. Poggioli, L. Poppleton, A. Poveda, J. Pralavorio, P. Pribyl, L. Price, M.J. Prieur, D. Puigdengoles, C. Puzo, P. Røhne, O. Ragusa, F. Rajagopalan, S. Reeves, K. Reisinger, I. Rembser, C. De Renstrom, P.A.B. Reznicek, P. Ridel, M. Risso, P. Riu, I. Robinson, D. Roda, C. Roe, S. Rohne, O. Romaniouk, A. Rousseau, D. Rozanov, A. Ruiz, A. Rusakovich, N. Rust, D. Ryabov, Y.F. Ryjov, V. Salto, O. Salvachua, B. Salzburger, A. Sandaker, H. Rios, C.S. Santi, L. Santoni, C. Saraiva, J.G. Sarri, F. Sauvage, G. Says, L.P. Schaefer, M. Schegelsky, V.A. Schiavi, C. Schieck, J. Schlager, G. Schlereth, J. Schmitt, C. Schultes, J. Schwemling, P. Schwindling, J. Seixas, J.M. Seliverstov, D.M. Serin, L. Sfyrla, A. Shalanda, N. Shaw, C. Shin, T. Shmeleva, A. Silva, J. Simion, S. Simonyan, M. Sloper, J.E. Smirnov, S.Yu. Smirnova, L. Solans, C. Solodkov, A. Solovianov, O. Soloviev, I. Sosnovtsev, V.V. Spanò, F. Speckmayer, P. Stancu, S. Stanek, R. Starchenko, E. Straessner, A. Suchkov, S.I. Suk, M. Szczygiel, R. Tarrade, F. Tartarelli, F. Tas, P. Tayalati, Y. Tegenfeldt, F. Teuscher, R. Thioye, M. Tikhomirov, V.O. Timmermans, C.J.W.P. Tisserant, S. Toczek, B. Tremblet, L. Troncon, C. Tsiareshka, P. Tyndel, M. Unel, M.K. Unal, G. Unel, G. Usai, G. Van Berg, R. Valero, A. Valkar, S. Valls, J.A. Vandelli, W. Vannucci, F. Vartapetian, A. Vassilakopoulos, V.I. Vasilyeva, L. Vazeille, F. Vernocchi, F. Vetter-Cole, Y. Vichou, I. Vinogradov, V. Virzi, J. Vivarelli, I. De Vivie, J.B. Volpi, M. Vu Anh, T. Wang, C. Warren, M. Weber, J. Weber, M. Weidberg, A.R. Weingarten, J. Wells, P.S. Werner, P. Wheeler, S. Wiessmann, M. Wilkens, H. Williams, H.H. Wingerter-Seez, I. Yasu, Y. Zaitsev, A. Zenin, A. Zenis, T. Zenonos, Z. Zhang, H. Zhelezko, A. Zhou, N.

Subjects
Physics::Instrumentation and Detectors, High Energy Physics::Experiment, Nuclear Experiment
Abstract

In 2004 at the ATLAS (A Toroidal LHC ApparatuS) combined test beam, one slice of the ATLAS barrel detector (including an Inner Detector set-up and the Liquid Argon calorimeter) was exposed to particles from the H8 SPS beam line at CERN. It was the first occasion to test the combined electron performance of ATLAS. This paper presents results obtained for the momentum measurement p with the Inner Detector and for the performance of the electron measurement with the LAr calorimeter (energy E linearity and resolution) in the presence of a magnetic field in the Inner Detector for momenta ranging from 20 GeV/c to 100 GeV/c. Furthermore the particle identification capabilities of the Transition Radiation Tracker, Bremsstrahlungs-recovery algorithms relying on the LAr calorimeter and results obtained for the E/p ratio and a way how to extract scale parameters will be discussed. © 2010 IOP Publishing Ltd and SISSA.

Published
2010

19. Epidemiology of acute promyelocytic leukemia in Italy

Author

G. Avvisati, A. Mele, M.A. Stazi, M.L. Vegna, P. Pasquini, F. Mandelli, B. Rotoli, G. De Rosa, G. Papa, A. Venditti, P. Citarrella, M. Tambone Reyes, E. Ascari, R. Invernizzi, A. Cajozzo, M. Musso, A. Alberti, A. Peta, P. Rossi Ferrini, F. Leoni, F. Caronia, S. Mirto, F. Nobile, P. Iacopino, L. Resegotti, B. Allione, S. Monfardini, V. Zagonel, V. Liso, G. Specchia, S. Tura, G. Visani, G. Broccia, W. Deplano, F. Ricciuti, M. Pizzuti, M. Longinotti, S. Bonfigli, A. De Laurenzi, L. Pacilli, L. Deriu, A. Chierichini, B. Bizzi, G. Leone, R. De Biasi, E. Miraglia, L. Bruzzese, and A. Abbadessa

Subjects
Acute promyelocytic leukemia, medicine.medical_specialty, Pediatrics, Hematology, Epidemiologic study, business.industry, Incidence (epidemiology), Age at diagnosis, medicine.disease, Leukemia, Oncology, immune system diseases, hemic and lymphatic diseases, Internal medicine, Epidemiology, medicine, business, neoplasms, Median survival
Abstract

Summary This retrospective epidemiologic study on 256 cases of Acute Promyelocitic Leukemia (APL) observed in 20 Italian hematology centers between 1980 and 1988 demonstrated that APL is different from the other acute non-lymphocytic leukemias (ANLL). The male/female ratio was 0.9; median age at diagnosis was 40 years (with 80% of patients between 15 and 54 years of age). The minimal annual incidence of APL in Italy per 1,000,000 inhabitants was estimated to be 0.6; an increased incidence was observed in spring and in autumn. The overall median survival duration of APL patients was 12.6 months. From an epidemiological point of view APL is a distinctive subtype of ANLL.

Published
1991

20. Blastoschizomyces capitatus: An Emerging Cause of Invasive Fungal Disease in Leukemia Patients

Author

P. Martino, M. Venditti, A. Micozzi, G. Morace, L. Polonelli, M. P. Mantovani, M. C. Petti, V. L. Burgio, C. Santini, P. Serra, and F. Mandelli

Subjects
Adult, Male, Microbiology (medical), medicine.medical_specialty, Antifungal Agents, Adolescent, Opportunistic Infections, Kidney, Gastroenterology, Flucytosine, Amphotericin B, Internal medicine, Trichosporon, medicine, Humans, Child, Lung, Mycosis, Aged, Retrospective Studies, Hepatitis, Acute leukemia, Leukemia, Hematology, biology, business.industry, Middle Aged, medicine.disease, biology.organism_classification, Infectious Diseases, Liver, Mycoses, Immunology, Female, Mitosporic Fungi, business, Spleen, medicine.drug
Abstract

Blastoschizomyces capitatus (formerly named Trichosporon capitatum or Geotrichum capitatum) is a rare cause of invasive fungal disease in immunocompromised hosts. We retrospectively studied epidemiologic, clinical, pathologic, and microbiologic features of this infection during a 68-month period at the Division of Hematology of the University La Sapienza in Rome. Twenty patients with evidence of B. capitatus were identified: 12 were infected, four were possibly infected, and four had evidence of B. capitatus colonization but were not infected by this fungus. Pulmonary infiltrates were seen in seven infected patients; four of these patients eventually developed mycetomalike cavitations. Eight infected patients presented clinical and radiologic features of focal hepatitis compatible with hepatosplenic candidiasis. Of the 12 infected patients, two did not receive any antifungal treatment and died, five did not show any response to systemic antifungal therapy, and five received prolonged amphotericin B plus 5-fluorocytosine therapy. Of the last group, three patients achieved stable remission of their acute leukemia and were cured, and two improved but had an apparent relapse of B. capitatus infection after their acute leukemia recurred.

Published
1990

21. Study of copper(II) association with dissolved organic matter in surface waters of three Mexican coastal lagoons

Author

R. Scott. Altmann, A. M. K. Hansen, James O. Leckie, and Enrique F. Mandelli

Subjects
Chemistry, Environmental chemistry, Dissolved organic carbon, Environmental Chemistry, Mineralogy, chemistry.chemical_element, General Chemistry, Copper
Abstract

Evaluation par titrage potentiometrique de la fixation du cuivre par la matiere organique dissoute dans les eaux de surface de 3 lagons de la zone mexicaine. Mesure de l'activite des ions cupriques au moyen d'une electrode selective. Calcul des constantes de liaison des complexes du cuivre avec des coordinats organiques en utilisant un modele mathematique

Published
1990

22. Autologous versus allogeneic stem cell transplantation in acute myeloid leukemia

Author

R, Willemze, S, Suciu, F, Mandelli, T, de Witte, and S, Amador

Subjects
Adult, Leukemia, Myeloid, Antineoplastic Combined Chemotherapy Protocols, Remission Induction, Humans, Transplantation, Homologous, Middle Aged, Transplantation, Autologous, Stem Cell Transplantation
Abstract

Using the data of the patients in complete remission (CR) up to the age of 45 years included in the EORTC-LG/GIMEMA AML-10 trial we investigated the value of the strategy to perform either an autologous (auto-SCT) or an allogeneic (allo-SCT) stem cell transplantation on an intention to treat basis. Between 1993 and 1999, out of 1198 pts, 822 achieved CR. 734 pts, constituting the study group, received an intensieve consolidation course: 293 had a sibling donor and 441 had not. Allo-SCT and auto-SCT was performed in 68.9% and 55.8%, respectively. Cytogenetics was successfully performed in 446 pts. Risk groups were: good (t(8;21), inv(16)), intermediate (NN or -Y only), bad/very bad (all others). Median follow-up was 4 years. The 4-year disease-free survival (DFS) rate of patients with a donor vs of those without a donor was 52.2% vs 42.2%, p = 0.044; the relapse incidence was 30.4% vs 52.5%, death in first complete remission was 17.4% vs 5.3%, and the survival rate was 58.3% vs 50.8% (p = 0.18). The DFS rates in pts with and without a sibling donor were similar in pts with good or intermediate risk cytogenetics, but 43.4% and 18.4%, respectively, in pts with bad or very bad risk cytogenetics. In younger patients (15-35 yrs), the difference was more pronounced. The strategy to perform an allo-SCT in patients where a family donor was available led to better overall results than to perform an auto-SCT, especially for younger patients or those with bad or very bad risk cytogenetics.

Published
2004

24. Low Roughness Values of RBCs Membrane in Cells with Cytoskeleton Alterations

Author

G. Boumis, F. Mandelli, G. Amiconi, S. Fenu, A. Congiu-Castellano, F. Mancini, M. Girasole, and Antonio Cricenti

Subjects
Membrane, Atomic force microscopy, Chemistry, Spherocyte, Sample preparation, Surface finish, Cytoskeleton, Staining, Fixation (histology), Cell biology
Abstract

In order to quantitatively investigate their ultramorphological characteristics, normally‐ and abnormally‐shaped human erythrocytes have been imaged by atomic force microscopy. Various fixation and staining methods have been examined for sample preparation. Roughness of the external membrane appeared to be independent of the overall cell shape (discocyte or spherocyte) and sample preparation; very stable in time up to one year and, most important, coupled with the meshwork of the membrane skeleton.

Published
2003

25. A phase II study of alpha-interferon and oral arabinosyl cytosine (YNK01) in chronic myeloid leukemia

Author

E. Zuffa, A. M. Carella, G. L. Gaidano, L. Luciano, C. Bergonzi, Domenico Russo, A. De Vivo, E. Volpe, Enrico Pogliani, S. Bassi, S. Rupoli, V. Liso, R Fanin, Giorgina Specchia, E. Gallo, M. Candela, E Trabacchi, B. Rotoli, E. M. Schiavone, E. Montefusco, T. Chisesi, F. Ciccone, M. A. Pistone, Nicoletta Testoni, Mario Tiribelli, Giovanni Rosti, A. Ambrosetti, Francesca Bonifazi, P. Mazza, Giovanni Martinelli, G. Fioritoni, S. Pardini, F. Lauria, A. Polacco, R. Battista, M. Michieli, S. Sica, F. Grignani, R. Di Lorenzo, F. Iuliano, A. Gabbas, Michele Baccarani, A. Peta, F. Mandelli, F. Palmieri, M. Bertini, Mario Boccadoro, Monica Bocchia, F. Frigeri, A. Blasio, P. Leoni, D. Noli, G. Leone, Giovanni Pizzolo, D. Ferrero, C. Miccolis, L. Garetto, M. Cervellera, C. A. Bodenizza, and A. M. Liberati

Subjects
Male, Cancer Research, medicine.medical_treatment, Administration, Oral, Phases of clinical research, Gastroenterology, cytogenetic response, Antineoplastic Combined Chemotherapy Protocols, Prodrugs, Chronic, CML, alpha IFN, YNK01, Starasid, Leukemia, Hematology, Remission Induction, Cytarabine, Myeloid leukemia, Middle Aged, Recombinant Proteins, Treatment Outcome, Oncology, Administration, Female, Complete Hematologic Response, Cytogenetic response, αIFN, Adult, Aged, Humans, Interferon-alpha, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Patient Compliance, Anesthesiology and Pain Medicine, medicine.drug, Oral, medicine.medical_specialty, medicine.drug_class, Alpha interferon, Interferon alpha-2, Antimetabolite, Internal medicine, medicine, Chemotherapy, business.industry, Immunology, BCR-ABL Positive, business, Myelogenous
Abstract

YNK01 (Starasid) is a prodrug that is adsorbed in the gut and is transformed in the liver in arabinosyl cytosine (AC). Low-dose AC (LDAC) is useful for the treatment of Philadelphia positive (Ph+) chronic myeloid leukemia (CML), especially in combination with alpha-interferon (alphaIFN). The use of YNK01 can avoid the daily s.c. injection of conventional AC. To assess the safety and the efficacy of alphaIFN and YNK01, we enrolled 86 consecutive previously untreated chronic phase Ph+ CML patients in a phase II study of alphaIFN (Intron-A) 5 MIU/m(2) daily and YNK01 600 mg daily 14 days a month. The 6-month complete hematologic response and the 12-month major cytogenetic response rates were 78 and 28%, respectively. In a prior study of alphaIFN and conventional LDAC, they were 62 and 22%, respectively. However, the compliance to the treatment was poor, with 25% of cases discontinuing the treatment within the first year. This was not because of the severity of the side effects but because of the frequency, duration and repetition of the side effects, for an overall frequency of 13.17 adverse events, mostly grade 1 and 2, per patient per year. Therefore, the study of this effective combination is being pursued, testing lower doses of alphaIFN and YNK01.

Published
2003

26. Melphalan treatment in patients with myelofibrosis with myeloid metaplasia

Author

M C, Petti, R, Latagliata, T, Spadea, A, Spadea, E, Montefusco, M A, Aloe Spiriti, G, Avvisati, M, Breccia, E, Pescarmona, and F, Mandelli

Subjects
Adult, Aged, 80 and over, Male, Anemia, Middle Aged, Prognosis, Survival Rate, Leukocyte Count, Treatment Outcome, Primary Myelofibrosis, Humans, Female, Antineoplastic Agents, Alkylating, Melphalan, Aged, Follow-Up Studies
Abstract

Between January 1985 and December 1992, 104 consecutive patients with symptomatic myelofibrosis with myeloid metaplasia (MMM) [splenic enlargement5 cm and/or transfusional requirement or Hb10 g/dl and/or white blood cell (WBC) count20 x 10(9)/l and/or platelets1.0 x 10(9)/l] received low-dose Melphalan (2.5 mg/3 times/week) to evaluate the efficacy and toxicity of this approach. Among 99 evaluable patients, 66 (66.7%) achieved a response after a median time of 6.7 months: 26 (26.3%) had a normalization of all clinical and haematological parameters (complete response, CR) and 40 (40.4%) showed an improvement50% (partial response, PR). Thirty-three patients (33.3%) were resistant. Reversible haematological toxicity was the most common complication. Median durations of CR and PR were 28.4 and 26 months respectively: median survival of CR + PR patients was 71.2 months (95%CI: 33.8-108.7) versus 36.5 months (95%CI: 24.5-48.5) for the non-responders (log-rank test, P =0.002). In the multivariate analysis, the following variables were significantly associated with a shorter survival: anaemia [hazard risk (HR) = 2.7], WBC count20 x 10(9)/l (HR = 2.4) and not achieving any type of response, either partial or complete (HR = 3.9). In conclusion, Melphalan could be a promising first-line option for MMM patients with clinical or haematological symptoms requiring treatment.

Published
2002

29. Use of erithropoietin in hematologic oncology

Author

F, Mandelli, M A, Aloe Spiriti, and R, Latagliata

Subjects
Humans, Erythropoietin, Hematologic Diseases
Abstract

Erythropoietin (EPO) is a glycoprotein synthesized by the kidney, which has a stimulating effect on bone marrow erythroid precursors. It has been identified many years ago, but its clinical use has been developed only since 1985 with the introduction of recombinant molecle (rHuEPO). In the past decade, rHuEPO has been employed in neoplastic as well as in chronic inflammatory diseases associated with anemia, that recognizes a multifactorial pathogenesis: defective endogenous EPO production, impaired erythroid proliferation due to excessive release of inflammatory cytokines, intrinsic abnormalities of erythroid precursors, reticulo-endothelial blockage with reduced erythroid uptake of iron. Anemia of neoplastic diseases, moreover, may be induced or worsened by marrow toxicity of chemotherapy. The efficacy of rHuEPO in these conditions is still unclear.

Published
2001

30. Ten-year follow-up of a single center prospective trial of unmanipulated peripheral blood stem cell autograft and interferon-alpha in early phase chronic myeloid leukemia

Author

G, Meloni, S, Capria, M, Vignetti, G, Alimena, P, de Fabritiis, E, Montefusco, and F, Mandelli

Subjects
Adult, Male, Time Factors, autologous stem cell transplantation, Hematopoietic Stem Cell Transplantation, Interferon-alpha, Antineoplastic Agents, Middle Aged, Combined Modality Therapy, Transplantation, Autologous, Cohort Studies, Survival Rate, chronic myelogenous leukemia, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Humans, Female, Prospective Studies, long-term survival, high-dose chemotherapy, interpheron-α, Follow-Up Studies
Abstract

The potential role of autologous stem cell transplantation (ASCT) as an alternative therapeutic strategy in chronic myelogenous leukemia (CML) has been widely explored in pilot studies, but the clinical results in terms of survival have so far been evaluated only retrospectively and in heterogeneous groups of patients. The goal of our prospective study was to evaluate the feasibility and long-term efficacy of unmanipulated ASCT followed by low-dose interferon-alpha in a homogeneous group of patients affected by CML in a very early phase of disease.Twenty-six unselected consecutive patients with CML in chronic phase underwent stem cell collection at diagnosis, then received cytoreductive treatment with hydroxyurea and, subsequently, a busulphan-melphalan myeloablative regimen followed by unmanipulated stem cell graft within one year of diagnosis. Interferon was given a median of 6.5 months after transplant at escalating doses, starting from 0.5 x 10(6) IU 3 times/week, on the basis of the clinical and hematologic tolerance.Median chronic phase duration from diagnosis is 9 years. The ten-year projected probability of overall survival from diagnosis is 55% with a median follow-up of surviving patients of 9.5 years (8-10.5); median survival has not been reached after ten years.Our experience suggests that high-dose therapy followed by unmanipulated peripheral blood stem cell transplantation and low-dose interferon-alpha is a feasible approach, which results in long-term survival in newly diagnosed CML patients. These data need to be confirmed in controlled trials comparing ASCT with other therapeutic approaches, such as the use of interferon-alpha alone or in combination with other agents.

Published
2001

31. Feasibility of peripheral blood stem cell rescue as intensification in elderly patients with acute myelocytic leukaemia: a pilot study from the Gimema Group. Gruppo Italiano Malattie Ematologiche Maligne Dell'Adulto

Author

M, Montillo, A, Tedeschi, L, Pagano, A, Venditti, F, Ferrara, P, Fabris, B, Martino, M, Musso, G, De Rosa, G, Specchia, M, Monaco, G, Sparaventi, A, Spadea, A, Palmas, W, Deplano, A, Manna, L, Melillo, E, Miraglia, S, Mirto, and F, Mandelli

Subjects
Aged, 80 and over, Male, Remission Induction, Hematopoietic Stem Cell Transplantation, Pilot Projects, Middle Aged, Transplantation, Autologous, Leukemia, Myeloid, Acute Disease, Granulocyte Colony-Stimulating Factor, Feasibility Studies, Humans, Female, Aged
Abstract

Elderly patients with untreated acute myeloid leukaemia (AML, n = 47) tested the feasibility of out-patient consolidation therapy and post-consolidation treatment (for patients aged71 years) with autologous peripheral blood stem cell transplantation (APBSCT). Overall, 13 patients out of 24 (51%) who achieved complete remission (CR) were eligible for further treatment after consolidation. Five patients were primed with granulocyte colony stimulating factor (G-CSF); a suitable number of CD34+ cells were harvested in three patients and were actually autotransplanted. The toxicity of APBSCT was negligible. Psychosocial problems impaired treatment of some patients on an out-patient basis. Resistant disease, toxicity and logistic problems reduced the number of patients to whom this procedure could actually be applied.

Published
2000

32. [The role of biotherapy in multiple myeloma]

Author

M T, Petrucci, A, Tafuri, and F, Mandelli

Subjects
Biological Factors, Interleukin-6, Granulocyte Colony-Stimulating Factor, Antibodies, Monoclonal, Granulocyte-Macrophage Colony-Stimulating Factor, Humans, Interleukin-2, Interferons, Multiple Myeloma, Erythropoietin, Antibodies, Anti-Idiotypic
Abstract

Despite considerable progress in recent years in the understanding of the biology of multiple myeloma (MM), this disease remains incurable, although many new therapeutic approaches are under evaluation. The rapid development of recombinant technologies has permitted the production of large amounts of cytokines and growth factors, favoring the use of biotherapies also in this disease. Among these products, the interferons have been the most extensively used in clinical trials, giving the most promising results especially in the setting of minimal residual disease, as maintenance therapy after response to conventional therapies, or to high dose chemotherapies followed by bone marrow (BM) or peripheral blood stem cell (PBSC) transplantation. However, more recently, a large number of cytokines and growth factors have been introduced in the clinical practice. Data of the use of erythropoietin have consistently demonstrated the role of this growth factor in ameliorating the grade of anemia as well as the quality of life of those MM patients whose disease is complicated by the presence of a severe or moderate anemia. Using hematopoietic growth factor in the mobilization of PBSC, the quantity of progenitor cells in the peripheral blood increased and the hematological toxicity of chemotherapy could be reduced. Despite the large amount of experimental data indicating a role for interleukins, as IL-2 and IL-6, in controlling tumor growth, there are only few clinical studies dealing with their use in MM. Results show that they arrest tumor progression rather than aid tumor regression, for this reason it appears that IL-2 and anti IL-6 antibodies should be investigated as maintenance therapy, in MM patients responding to chemotherapy. In the future it will be necessary to clarify for MM patients the role of other cytokines such as IL-1 beta and TNF alpha. A possible strategy to improve the clinical outcome of MM patients is to prevent the regrowth of residual tumor cells by establishing adoptive immunity at the stages of minimal residual disease previous obtained using chemotherapy. To this end a possible strategy is to induce an immune response against residual tumor cells by passive (using monoclonal antibodies) or active (using the idiotype expressed by malignant cells) immunotherapy.

Published
2000

33. Centre effect on treatment outcome for patients with untreated acute myelogenous leukaemia? An analysis of the AML 8A Study of the Leukemia Cooperative Group of the EORTC and GIMEMA. European Organization for Research and Treatment of Cancer (EORTC) Leukemia Cooperative Group and the Gruppo Italiano Malattie Ematologiche Maligne dell'Adulto (GIMEMA)

Author

S, Keating, T, de Witte, S, Suciu, F, Mandelli, E, Damasio, R, Willemze, E, Morra, S, Amadori, M, Dardenne, M L, Vegna, and R A, Zittoun

Subjects
Adult, Male, Adolescent, Histocompatibility Testing, Cancer Care Facilities, Middle Aged, Survival Analysis, Transplantation, Autologous, Tissue Donors, Clinical Protocols, Leukemia, Myeloid, Acute Disease, Antineoplastic Combined Chemotherapy Protocols, Humans, Female, Prospective Studies, Child, Bone Marrow Transplantation
Abstract

In the AML 8A study patients were treated with remission-induction therapy followed by one consolidation course. Patients in complete remission (CR) were randomised between autologous bone marrow transplantation (ABMT) and a second intensive consolidation course, except for those with a histocompatible sibling donor, who received allogeneic bone marrow transplantation (alloBMT). This analysis was performed to determine whether centres which only performed induction and consolidation therapy, achieved similar results as centres who also performed transplantation. 542/676 (80%) from transplantation centres and 150/194 (77%) from referring centres achieved CR, with an early death rate of 5% and 11%, respectively (P = 0.01). 66% of patients with a donor from transplantation centres received alloBMT in first CR compared with 57% from referring centres (P = 0.2). Transplantation centres randomised 64% of patients without a donor, referring centres 47% (P = 0.04). The full protocol treatment was completed by 275/542 (51%) and 61/150 (41%) patients, respectively (P = 0.04). The overall survival rate at 6 years from diagnosis was 34% and 36%, respectively (P = 0.9). In conclusion, the type of centre did not appear to have an influence on overall survival. The feasibility of the study was acceptable for both types of centres. The referring centres applied more selection for transplantation. Despite a more intensive second-line treatment at transplantation centres, the overall outcome remained similar to that of referring centres.

Published
2000

34. [Treatment of acute and chronic leukemias]

Author

F, Mandelli and E, Montefusco

Subjects
Chromosome Aberrations, Leukemia, Hairy Cell, Antibiotics, Antineoplastic, Leukemia, Daunorubicin, Antineoplastic Agents, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Combined Modality Therapy, Leukemia, Lymphocytic, Chronic, B-Cell, Transplantation, Autologous, Leukemia, Myeloid, Karyotyping, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Acute Disease, Antineoplastic Combined Chemotherapy Protocols, Humans, Transplantation, Homologous, Idarubicin, Aged, Bone Marrow Transplantation, Randomized Controlled Trials as Topic
Abstract

In the last decade the use of new drugs (retinoic acid, interferons, purine nucleoside analogs etc.) had only minimal impact in the evolution of leukemia management. In most cases, therapeutic options have progressed because of advances in supportive therapies and optimization of old chemotherapeutic strategies. Several experiences with autologous bone marrow transplantation (BMT) have proved that in acute leukemias and in selected patients with chronic leukemias is a valid alternative to allogeneic BMT. The availability of hematopoietic stem cells from unrelated donors and from cord blood, has overcome difficulties related to the absence of a suitable HLA identical sibling donor. Modern therapeutic approaches point to tailor treatment intensity according to risk categories, defined by clinical and biological parameters at diagnosis. In this context, the prognostic role of karyotypic lesions is under investigation.

Published
1999

35. A prospective study of residual-disease monitoring of the ALL1/AF4 transcript in patients with t(4;11) acute lymphoblastic leukemia

Author

G, Cimino, L, Elia, M C, Rapanotti, T, Sprovieri, M, Mancini, A, Cuneo, C, Mecucci, G, Fioritoni, M, Carotenuto, E, Morra, V, Liso, L, Annino, G, Saglio, G, De Rossi, R, Foà, and F, Mandelli

Subjects
Adult, Male, Neoplasm, Residual, Time Factors, Oncogene Proteins, Fusion, Reverse Transcriptase Polymerase Chain Reaction, Chromosomes, Human, Pair 11, Remission Induction, Infant, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Disease-Free Survival, Translocation, Genetic, Recurrence, Karyotyping, Humans, Female, Prospective Studies, Chromosomes, Human, Pair 4, Follow-Up Studies, Monitoring, Physiologic
Abstract

Twenty-five patients (22 adults and 3 infants) with ALL1/AF4-positive acute lymphoblastic leukemia (ALL) were prospectively monitored by reverse transcriptase-polymerase chain reaction (RT-PCR) between January 1992 and July 1999. After high-dose induction and consolidation chemotherapy without bone marrow transplantation, all patients had a complete hematologic remission. Using nested RT-PCR (sensitivity 10(-4)), we observed conversion to PCR negativity in 11 (44%) of the patients. Thirteen of the 14 patients who did not have a molecular remission had a relapse at a median time of 4 months (range, 1 - 20 months). Of the 11 patients who had a conversion to PCR negativity, 5 reconverted to PCR positivity within 1 to 14 months. These 5 patients all progressed to hematologic relapse after 2, 3, 4, 4, and 7 months, respectively. Of the remaining 6 patients, 4 are in persistent hematologic and molecular remission at 12, 14, 88, and 96 months, whereas 2 are early in their follow-up. Actuarial probabilities of relapse and overall survival were 100% and 0% at 14 and 24 months and 67% and 43% at 96 and 100 months, respectively, in patients who had persistent RT-PCR positivity and in those who had a molecular remission. For both relapse and survival, the differences observed between the two groups were significant (P =.003 and P.005, respectively). This study, which represents the first prospective analysis of residual-disease monitoring carried out in a substantial series of patients with t(4;11)-positive ALL, emphasizes the clinical relevance of RT-PCR-based methods to monitor minimal residual disease in this leukemia subset. (Blood. 2000;95:96-101)

Published
1999

36. VH gene usage by family members affected with chronic lymphocytic leukaemia

Author

O, Pritsch, X, Troussard, C, Magnac, F R, Mauro, F, Davi, B, Payelle-Brogard, G, Dumas, M, Pulik, F, Clerget, F, Mandelli, N, Chiorazzi, H W, Schroeder, M, Leporrier, and G, Dighiero

Subjects
Adult, Aged, 80 and over, Male, Genes, Immunoglobulin, Molecular Sequence Data, Mutation, Humans, Female, familial chronic lymphocytic leukaemia, V-H genes, Amino Acid Sequence, Middle Aged, Leukemia, Lymphocytic, Chronic, B-Cell, Aged
Abstract

The excess risk of chronic lymphocytic leukaemia (CLL) in the first-degree relatives of affected patients suggests that familial CLL might constitute a useful model to study the pathogenesis of this disease, as has been demonstrated in numerous other neoplastic disorders. Previous studies have shown non-random utilization of immunoglobulin genes in CLL, some germline in sequence and others containing numerous somatic mutations. To investigate whether familial cases of CLL exhibit similarities in the composition of the B-cell receptor repertoire to the pattern expressed by CLL patients as a whole, we have studied 25 CLL patients belonging to 12 different families (four French and eight Italian), each of which contained at least two affected members. Among familial cases, VH gene segment utilization proved non-random and diverged from the frequencies previously reported among unrelated patients with CLL. Specifically, although the 4-34 and 5-51 gene segments were found repeatedly, the 1-69 and 4-39 gene segments were used sparingly and the 3-23 gene segment presented with increased frequency. Following the pattern detected in studies of unrelated patients, the single 1-69 expressing CLL contained an unmutated H chain sequence and included a long HCDR3 interval. In contrast, 3-23 containing H chains all used JH4, retained at most 93% homology with germline sequence, and included only short HCDR3 intervals. The vast majority of the CLL variable domains contained a high degree of somatic mutation and exhibited an excess of replacement mutations in the CDR intervals. These findings suggest that familial CLL cases may preferentially derive from B-cell progenitors that have responded to antigen.

Published
1999

37. Characterization of 12p molecular events outside ETV6 in complex karyotypes of acute myeloid malignancies

Author

R, La Starza, M, Stella, N, Testoni, E, Di Bona, S, Ciolli, P, Marynen, M F, Martelli, F, Mandelli, and C, Mecucci

Subjects
Adult, Gene Rearrangement, Male, Chromosomes, Human, Pair 12, Leukemia, Myeloid, Karyotyping, Humans, Chromosome Breakage, Female, Middle Aged, In Situ Hybridization, Fluorescence, Translocation, Genetic, Aged
Abstract

Acute myeloid disorders with rearrangements of 12p outside the ETV6 gene were characterized by fluorescence in situ hybridization (FISH) with a panel of DNA probes. Seven patients with de novo acute myeloid leukaemia (AML), one with secondary acute myeloid leukaemia (sAML), and one in the blast phase of chronic myeloid leukaemia (CML-BP) were enrolled in the study. All AML cases showed multiple karyotypic changes. Chromosome 5 and/or 7 deletions were the most frequent accompanying changes. FISH revealed amplification, cryptic translocation, and fragmentation of chromosome 12, not discernible at karyotypic level. Different karyotypic rearrangements of 12p showed a common molecular event. Among the seven cases in which breakpoints could be determined, six were telomeric and one centromeric to ETV6. In three AML cases a new recurrent breakpoint in the telomeric region was identified distally to locus D12S158 and to pac 922B22 which is the most telomeric probe available for 12p. Accompanying cryptic deletions were also detected in five patients and the commonly deleted region, of around 700 kb, included the ETV6 gene and the D12S391 locus.

Published
1999

38. Analysis of the B-cell receptor B29 (CD79b) gene in familial chronic lymphocytic leukemia

Author

B, Payelle-Brogard, C, Magnac, F R, Mauro, F, Mandelli, and G, Dighiero

Subjects
Adult, Aged, 80 and over, Male, Sequence Homology, Amino Acid, DNA Mutational Analysis, Molecular Sequence Data, DNA, Neoplasm, Middle Aged, Leukemia, Lymphocytic, Chronic, B-Cell, Antigens, CD, Humans, Female, Amino Acid Sequence, Immunoglobulin Heavy Chains, CD79 Antigens, Aged
Abstract

The B-cell antigen receptor (BCR) comprises membrane Igs (mIgs) and a heterodimer of Igalpha (CD79a) and Igbeta (CD79b) transmembrane proteins, encoded by the mb-1 and B29 genes, respectively. These accessory proteins are required for surface expression of mIg and BCR signaling. B cells from chronic lymphocytic leukemia (B-CLL) frequently express low to undetectable surface Ig, as well as CD79b protein. Recent work described genetic aberrations affecting B29 expression and/or function in B-CLL. Because the prevalence of CLL is increased among first degree relatives, we analyzed the B29 gene in 10 families including 2 affected members each. A few silent or replacement mutations were observed at the genomic level, which never lead to truncated CD79b protein. Both members of the same family did not harbor the same mutations. However, a single silent base change in the B29 extracellular domain, corresponding to a polymorphism, was detected on 1 allele of most patients. These results indicate that the few mutations observed in the B29 gene in these patients do not induce structural abnormalities of the CD79b protein and thus do not account for its low surface expression in B-CLL. Furthermore, genetic factors were not implicated, because identical mutations were not observed among 2 members of the same family.

Published
1999

39. A prospective study of alpha-interferon and autologous bone marrow transplantation in chronic myeloid leukemia. The Italian Co-operative Study Group on Chronic Myeloid Leukemia

Author

G, Meloni, D, Russo, M, Baccarani, N, Testoni, G, Martinelli, R, Fanin, E, Zuffa, G, Rosti, G, Alimena, G, Saglio, F, Mandelli, and S, Tura

Subjects
Adult, Treatment Outcome, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Interferon Type I, Humans, Prospective Studies, Middle Aged, Combined Modality Therapy, Transplantation, Autologous, Recombinant Proteins, Bone Marrow Transplantation
Abstract

Alpha-interferon (alphaIFN) can induce cytogenetic remissions in chronic myeloid leukemia (CML). Hemopoietic progenitors can be collected from the marrow in remission and utilized for autologous repopulation after high dose chemotherapy. This study was designed with the purpose of evaluating the feasibility of a combined treatment policy of alphaIFN followed by autologous bone marrow transplantation (autoBMT).A prospective study of alphaIFN and autoBMT was begun in 1989. Two hundred and seventy-two consecutive previously untreated non-blastic Ph positive chronic myeloid leukemia (CML) patients, who were less than 56 years old, were enrolled over a 3-year period (1989-1991) and were assigned to receive human recombinant alphaIFN 2a (Roferon-A) at a dose of 9 MIU daily for at least one year. If they achieved a cytogenetic response consisting in a percentage of Ph neg metaphases of more than 25%, they were eligible for marrow harvesting and subsequent autografting after high dose busulfan (16 mg/kg) and melphalan (60 mg/m(2)).Seventy-six patients (28%) were eligible for a marrow harvest but the marrow was harvested in only 37 cases (14%), and only twenty-three patients (8%) were actually autografted. One patient died of infection nine days after autoBMT. The other patients recovered and did not suffer any late adverse events. Five patients progressed to blastic phase, six are alive in complete hematologic remission and eleven are alive in complete hematologic and cytogenetic remission. AlphaIFN treatment was reinstituted after autoBMT in 18 of 22 cases, but four patients who are in continuous complete cytogenetic remission were not given alphaIFN anymore. The progression-free survival of the autografted patients is 65% 8 years after registration.This study shows that bone marrow hemopoietic progenitors (Ph neg and Ph pos) can be collected from patients who respond to alphaIFN and can be used to rescue hemopoietic activity after high dose chemotherapy. Though some complete and durable cytogenetic remissions were obtained, the treatment could be applied only to a small group of good risk patients, highlighting that selection is very important and results cannot be extrapolated to the average patient.

Published
1999

40. Acute lymphoblastic leukaemia occurring as second malignancy: report of the GIMEMA archive of adult acute leukaemia. Gruppo Italiano Malattie Ematologiche Maligne dell'Adulto

Author

L, Pagano, A, Pulsoni, M E, Tosti, L, Annino, A, Mele, A, Camera, B, Martino, C, Guglielmi, R, Cerri, E, Di Bona, R, Invernizzi, C, Castagnola, R, Bassan, L, Mele, G, Todeschini, G, Leone, and F, Mandelli

Subjects
Adult, Aged, 80 and over, Male, Adolescent, Italy, Humans, Female, Neoplasms, Second Primary, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Aged
Abstract

Between July 1992 and June 1996, 901 new cases of adult acute lymphoblastic leukaemia were recorded in the GIMEMA Archive of Adult Acute Leukaemia; 21 of them (2.3%) had a previous primary malignancy (PM). We found that secondary acute lymphoblastic leukaemia cases (sALL) presented with older age, a high incidence of pre-pre-B immunophenotype and a significantly higher prevalence of cancer among relatives compared to de novo ALL. The leukaemogenic activity of the cytotoxic drugs employed for the treatment of PM may have played a potential role in only a proportion of patients, opening the possibility that some sALL patients may have developed two or more malignancies due to individual predisposing factors.

Published
1999

41. Disappearance of PML/RAR alpha acute promyelocytic leukemia-associated transcript during consolidation chemotherapy

Author

G, Martinelli, E, Ottaviani, N, Testoni, G, Visani, D, Diverio, G, D'Elia, F, Mandelli, and S, Tura

Subjects
Adult, Male, Neoplasm, Residual, Adolescent, Remission Induction, Tretinoin, Middle Aged, Combined Modality Therapy, Leukemia, Promyelocytic, Acute, Bone Marrow, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Neoplastic Stem Cells, Humans, Immunologic Factors, Female, RNA, Messenger, RNA, Neoplasm, Idarubicin
Abstract

Acute promyelocytic leukemia (APL) (M3 according to FAB classification) is a subtype of acute myelogenous leukemia characterized by a specific t(15;17) (q22;q12) chromosomal translocation. The majority of APL patients achieve morphologic remission after induction chemotherapy. They can be followed from this point by cytogenetic and molecular analysis of the persistence of the PML/RAR alpha transcript. In order to determine the influence of successive courses of consolidation chemotherapy on clinical and molecular outcome, APL patients treated with all-trans retinoic acid (ATRA) and chemotherapy (AIDA-GIMEMA-LAP0493 protocol) were investigated.Twenty-four APL patients (pts) (15 males; 9 females) were studied by RT-PCR and cytogenetic analysis at diagnosis, after induction chemotherapy, at each point after any of three consolidation courses, and every 3 months during the first years of maintenance therapy. The median follow-up was 24 months (mths) (range 7-40 mths).All pts achieved hematologic remission after induction chemotherapy. Our results demonstrate that the majority (87%) of APL patients were still molecularly positive for the APL associated transcript after induction chemotherapy, while the majority (80%) of APL patients became PCR-after the second consolidation chemotherapy.The role of the third consolidation chemotherapy course in converting patients with persistent molecular evidence of disease from PCR+ to PCR- was minimal. We confirm the validity of molecular follow-up after single courses of chemotherapy in monitoring the role of molecular remission.

Published
1998

42. Management of advanced acute lymphoblastic leukemia in children and adults: results of the ALL R-87 protocol. AIEOP and GIMEMA Cooperative Groups

Author

F, Giona, L, Annino, A M, Testi, R, Rondelli, W, Arcese, G, Meloni, M L, Moleti, and F, Mandelli

Subjects
Adult, Male, Adolescent, bmt, Disease-Free Survival, Prednisone, Age Factors, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Humans, Child, Recurrence, Child, Preschool, Infant, Idarubicin, Survival Rate, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols, Middle Aged, Bone Marrow Transplantation, Cytarabine, Female, Remission Induction, advanced all, Preschool, idarubicin, intermediate dose ara-c, Settore MED/15 - Malattie del Sangue
Abstract

Fifty-seven patients aged55 years with acute lymphoblastic leukemia (ALL) in second or third bone marrow (BM) relapse or refractory to first-line therapy were enrolled in an Italian cooperative study. The ALL R-87 protocol included idarubicin (IDA) plus intermediate dose cytarabine (IDARA-C) and Prednisone (PDN) as induction, followed by a consolidation phase and BMT. Complete remission (CR) was achieved in 41/57 patients (72%). The CR rate was significantly higher in patients aged15 years at diagnosis and at time of treatment compared to those agedor = 15 (84% vs 50%, p=0.01 and 85% vs 54%, p = 0.02, respectively). Nineteen of 41 responders (46.3%) underwent bone marrow transplant (BMT) (10 autologous and 9 allogeneic). The estimated probabilities of event free survival (EFS +/- SE) and survival +/- SE at 6 years were 0.13 +/- 0.05 and 0.20 +/- 0.06, respectively, for all enrolled patients. Univariate analysis showed that children had a better EFS rate compared to adults (0.16 +/- 0.07 vs 0.08 +/- 0.07, p = 0.014). The estimated probability of disease free survival (DFS +/- SE) at 6 years was 0.18 +/- 0.07 for all responders. No differences in DFS were observed between patients submitted to allogeneic or autologous BMT (0.33 +/- 0.16 vs 0.25 +/- 0.15). Among patients treated in second or third relapse, a first CR lengthor = 48 months favorably influenced both DFS (p = 0.014) and EFS (p = 0.018). Our results show the efficacy of the intermediate dose ARA-C plus IDA schedule for high risk adult and childhood ALL patients. No differences in disease outcome were observed between allogeneic and autologous BMT.

Published
1998

43. The risk of acute leukemia in patients treated for Hodgkin's disease is significantly higher aft [see bined modality programs than after chemotherapy alone and is correlated with the extent of radiotherapy and type and duration of chemotherapy: a case-control study

Author

E, Brusamolino, A P, Anselmo, C, Klersy, M, Santoro, E, Orlandi, G, Pagnucco, F, Lunghi, R, Maurizi-Enrici, C D, Baroni, M, Lazzarino, F, Mandelli, and C, Bernasconi

Subjects
Adult, Male, Risk, Adolescent, Pelvis, Actuarial Analysis, Lomustine, Cause of Death, Abdomen, Antineoplastic Combined Chemotherapy Protocols, Odds Ratio, Humans, Mechlorethamine, Child, Antineoplastic Agents, Alkylating, Aged, Aged, 80 and over, Leukemia, Radiation-Induced, Leukemia, Dose-Response Relationship, Drug, Radiotherapy, Age Factors, Neoplasms, Second Primary, Middle Aged, Combined Modality Therapy, Hodgkin Disease, Italy, Vincristine, Case-Control Studies, Myelodysplastic Syndromes, Procarbazine, Acute Disease, Splenectomy, Prednisone, Female, Follow-Up Studies
Abstract

Patients treated for Hodgkin's disease have an increased risk of developing subsequent acute leukemia. This co-operative study was conducted to assess the relative risk associated with several candidate factors including age, splenectomy, combined modality therapy and cumulative drug dose including alkylating agents and nitrosurea derivatives.This study evaluated the risk of acute leukemia according to pretreatment variables and therapy modalities among 1659 patients treated for Hodgkin's disease and followed for a median time of 10 years. Both case-control and actuarial risk studies were performed. Median age was 34 years (range: 12-83); 53% of patients were splenectomized. As to the overall therapy, 348 patients (21%) were given radiotherapy (RT) alone, 375 (23%) chemotherapy (CT) alone (including MOPP, MOPP + ABVD or MOPP + ABVD + lomustine); 936 (56%) received both CT and RT, either as primary or salvage treatment.The overall 15-year actuarial risk of leukemia was 4.2%; the hazard function curve showed two peaks of risk at the 3th and the 8th year from the initiation of therapy and no leukemia beyond the 12th year of follow-up. Risk of leukemia was 0.3% after RT alone, 2.8% after CT alone (2.2% after MOPP; 4.4% after MOPP + ABVD + lomustine), and 5.4% in patients given combined modality therapy (10.2% for RT + MOPP; 15.6% for RT + MOPP + lomustine). No leukemia occurred after ABVD alone and the risk was low (0.6%) when neither mechlorethamine nor lomustine were utilized. Patients who had received extended radiotherapy including abdomen and pelvis in addition to MOPP showed a significantly higher risk of leukemia compared to those given limited RT + MOPP (P = 0.01). Case-control analysis indicated advanced stage, type and duration (8 months) of CT and extension of RT as significant risk factors for leukemia. Compared to RT alone, the odds ratio was 5.9 after MOPP + extended RT, and 8 when a lomustine-containing regimen was used, as well. Neither age nor splenectomy were independent risk factors for leukemia; splenectomy was influential only when patients had been given MOPP chemotherapy, as well.Both case-control and actuarial analyses indicated that: a) combined modality therapy with MOPP and extensive RT (including abdomen and pelvis), and the use of lomustine added to the leukemogenic risk of MOPP alone; b) programs without mechlorethamine, procarbazine and lomustine were almost devoid of leukemogenic risk.

Published
1998

44. Therapy of acute myeloid leukemia: towards a patient-oriented, risk-adapted approach

Author

F, Mandelli, M C, Petti, and F, Lo Coco

Subjects
Chromosome Aberrations, Myeloid, Risk, Salvage Therapy, Tumor, Leukemia, Palliative Care, Remission Induction, Prognosis, Neoplasm Proteins, Acute Disease, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Bone Marrow Transplantation, DNA-Binding Proteins, Feasibility Studies, Humans, Karyotyping, Leukemia, Myeloid, Transcription Factors, Treatment Outcome, Case Management, Settore MED/15 - Malattie del Sangue, Biomarkers
Abstract

The successful use of differentiating treatment for patients with acute promyelocytic leukemia (APL) suggests that other acute myeloid leukemias (AML) may benefit from tailored and subtype-specific therapy. Despite the fact that new drugs specifically targeting AML genetic lesions have not yet been developed, distinct karyotypic categories have been identified which may deserve differentiated treatment. In addition, molecular assays to assess response to therapy more sensitively are now available for several AML subsets. In this review, we discuss the role of genetic characterization in the therapy of AML, and the investigative efforts which we believe are still needed for the design of tailored treatment for each and every patient with this disease.The authors have been working in this field for many years and have contributed original papers, the data of which are incorporated in this article. In addition, the material analyzed in this overview includes articles and reviews covered by the Science Citation Index and Medline as well as some more recent unpublished personal observations.Modern therapeutic approaches to AML tend to differentiate post-induction treatment intensity according to cytogenetically defined risk categories. Such prognostic categorization is largely unsatisfactory. In fact, following the advent of newly developed molecular assays (e.g. RT-PCR and FISH), specific and prognostically relevant lesions are frequently found in patients with an apparently normal karyotype, and these patients are, therefore, re-assigned to more appropriate prognostic categories. In addition, recent studies suggest that some patients may benefit from an increase in induction intensity; rapid genetic characterization will be needed for future differentiation of initial therapy. However, preliminary investigation of AML by integrated karyotypic/molecular analyses show that no specific abnormalities are detectable in at least half of the cases. Therefore, use of genetic criteria for prognostic stratification is currently feasible in only a proportion of patients.The prognostic role of genetic lesions, currently identified by karyotypic studies, needs to be validated in large series of AML patients prospectively characterized by advanced molecular/cytogenetic analyses and treated uniformly. In addition, searches for new clinically relevant genetic abnormalities, and diagnostic tools for their rapid identification are urgently needed to identify prognostic categories better. Elucidation of AML gene alterations should foster basic investigation aimed at developing new drugs targeted to the specific lesion in the individual patient. Before these more specific therapeutic agents are developed, diagnostic genetic characterization should add to other well-established prognostic factors to optimize the use of the presently available therapies.

Published
1998

45. The influence of HLA-matched sibling donor availability on treatment outcome for patients with AML: an analysis of the AML 8A study of the EORTC Leukaemia Cooperative Group and GIMEMA. European Organization for Research and Treatment of Cancer. Gruppo Italiano Malattie Ematologiche Maligne dell'Adulto

Author

S, Keating, T, de Witte, S, Suciu, R, Willemze, M, Hayat, B, Labar, L, Resegotti, P R, Ferrini, F, Caronia, M, Dardenne, G, Solbu, M C, Petti, M L, Vegna, F, Mandelli, and R A, Zittoun

Subjects
Adult, Male, Transplantation Conditioning, Adolescent, Histocompatibility Testing, Middle Aged, Risk Assessment, Transplantation, Autologous, Disease-Free Survival, Tissue Donors, Leukemia, Myeloid, Acute, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols, Humans, Female, Prospective Studies, Child, Bone Marrow Transplantation
Abstract

To determine whether patients with a HLA-identical sibling donor have a better outcome than patients without a donor, an analysis on the basis of intention-to-treat principles was performed within the framework of the EORTC-GIMEMA randomized phase III AML 8A trial. Patients in complete remission (CR) received one intensive consolidation course. Patients with a histocompatible sibling donor were then allocated allogeneic bone marrow transplantation (alloBMT), the patients without a donor were randomized between autologous BMT (ABMT) and a second intensive consolidation (IC2). 831 patients46 years old and alive8 weeks from diagnosis were included. HLA typing was performed in 672 patients. AlloBMT was performed during CR1 in 180 (61%) out of 295 patients with a donor. Another 38 patients were allografted: five in resistant disease, 14 during relapse and 19 in CR2. ABMT was performed in 130 (34%) out of 377 patients without a donor in CR1, in six (2%) patients during relapse and in 38 (10%) patients during CR2. The disease-free survival (DFS) from CR for patients with a donor was significantly longer than for patients without a donor (46% v 33% at 6 years; P=0.01, RR 0.78, 95% confidence interval 0.63-0.96). The overall survival from diagnosis for patients with a donor was longer, but not statistically significant, than for patients without a donor (48% v 40% at 6 years; logrank P=0.24). When patients were stratified according to prognostic risk groups, the same trend in favour of patients with a donor was seen for survival duration and the DFS remained significantly longer for this group of patients.

Published
1998

46. The risk of non-Hodgkin's lymphoma after Hodgkin's disease, with special reference to splenic treatment

Author

R M, Enrici, A P, Anselmo, V, Iacari, M F, Osti, M, Santoro, V, Tombolini, F, Mandelli, and C, Biagini

Subjects
Adult, Male, Neoplasms, Radiation-Induced, Risk Factors, Lymphoma, Non-Hodgkin, Humans, Female, Hodgkin Disease, Spleen, Follow-Up Studies
Abstract

One of the consequences of the enormous improvement in survival rates of patients treated for Hodgkin's disease (HD) is the emergence in the long term of treatment-related complications, particularly secondary cancers. This study was undertaken to observe the occurrence of non-Hodgkin's lymphoma (NHL) in patients treated for HD and to identify the etiological role of various risk factors, especially spleen irradiation, in the pathogenesis of this illness.From 1972 to 1996, the Department of Radiation Oncology and the Hematology Section of "La Sapienza" University of Rome observed and analyzed the occurrence of NHL in 1,391 patients treated for HD. The average follow-up period was 84 months. For a more accurate calculation of the risk of the occurrence of NHL, the patients were first divided into 3 groups according to their initial treatment and also according to the total treatment they had received. Then, in order to establish the possible connection between NHL and splenic treatment the patients were also divided into 3 subgroups according to whether they had undergone splenectomy, splenic irradiation or neither of these. Two different methods of statistical analysis were used: (a) the cumulative risk (confidence interval) was evaluated in relation to treatment (initial and at the time of salvage) and (b) the Cox model was applied to identify the variables which play a role in the appearance of NHL. The cumulative risk of developing NHL was assessed using the Kaplan and Meier method. A multivariate analysis was performed using the Cox Proportional Hazard Model.A total of 20 cases of NHL were observed, appearing between 17 and 206 months after initial treatment. The cumulative risk was 0.8%, 1.8%, 2.6% and 3.5% at 5, 10, 15 and 20 years respectively. According to the multivariate analysis, significant risk factors were splenic irradiation and age (40 years). Splenic irradiation (vs no splenectomy/no splenic irradiation) showed a relative risk of 5.69, p = 0.0280, while age over 40 showed a relative risk of 3.05, p = 0.0152.From the results of this study, if appears that there is a possibility that splenic irradiation and age over 40 increase the risk of NHL in HD patients. Further studies are needed to investigate in greater depth the role of spleen irradiation in the occurrence of this illness.

Published
1998

47. Umbilical cord blood transplant from HLA-mismatched unrelated donor in high-risk leukemia

Author

W, Arcese, A P, Iori, M, Screnci, C, Guglielmi, A, Mengarelli, D, Carmini, A M, Testi, M L, Moleti, G, Cimino, P, Perrone, L, Laurenti, L, Elia, F, Boecklin, A, Romano, L, De Felice, and F, Mandelli

Subjects
Male, Leukemia, Adolescent, Histocompatibility Testing, Hematopoietic Stem Cell Transplantation, Fetal Blood, Disease-Free Survival, Treatment Outcome, Fetal Tissue Transplantation, Child, Preschool, Humans, Transplantation, Homologous, Female, Child
Abstract

Twelve consecutive children with high-risk leukemia have been submitted to UCB transplant from unrelated 1 or 2 loci HLA-mismatched donor. All patients received an identical regimen for conditioning and GVHD prophylaxis. The median dose of viable nucleated cells infused was 2.8 x 10(7)/kg bw (range 1.4-7.9). Of 11 patients evaluable for engraftment, the hematopoiesis was of full donor origin in seven patients and autologous in four. The probability of disease-free survival at 1 and 2 years from UCB transplant is 60 and 42%, respectively.

Published
1998

48. The threshold for prophylactic platelet transfusions in adults with acute myeloid leukemia. Gruppo Italiano Malattie Ematologiche Maligne dell'Adulto

Author

P, Rebulla, G, Finazzi, F, Marangoni, G, Avvisati, L, Gugliotta, G, Tognoni, T, Barbui, F, Mandelli, and G, Sirchia

Subjects
Adult, Male, Treatment Outcome, Adolescent, Leukemia, Myeloid, Humans, Female, Hemorrhage, Platelet Transfusion, Middle Aged, Thrombocytopenia, Aged
Abstract

Prophylactic platelet transfusions are usually administered to patients receiving myelotoxic chemotherapy when their platelet count falls below 20,000 per cubic millimeter. Some observations suggest that lower platelet counts can be appropriate in patients in stable condition, but the safety of lower thresholds is uncertain.We evaluated 255 adolescents and adults (age, 16 to 70 years) with newly diagnosed acute myeloid leukemia (but not acute promyelocytic leukemia), who were treated in 21 centers. One hundred thirty-five patients were randomly assigned to receive a transfusion when their platelet count fell below 10,000 per cubic millimeter (or 10,000 to 20,000 per cubic millimeter in those with a temperature above 38 degrees C, with active bleeding, or a need for invasive procedures), and 120 patients were assigned to receive a transfusion when their platelet count was less than 20,000 per cubic millimeter.Patients in the group with a threshold of 10,000 platelets per cubic millimeter received 21.5 percent fewer platelet transfusions than the patients in the group with a threshold of 20,000 platelets per cubic millimeter (P=0.001). The numbers of red-cell units transfused were not significantly different between groups. Major bleeding (defined as any bleeding more than petechiae or mucosal or retinal bleeding) occurred in 21.5 and 20 percent of patients, respectively (P=0.41), and on 3.1 and 2.0 percent of the days of hospitalization. One episode of fatal cerebral hemorrhage occurred in the group with a threshold of 10,000 platelets per cubic millimeter; none occurred in the other group (P= 0.95). Actuarial estimates of survival during induction chemotherapy, actuarial estimates of the absence of major bleeding, and the length of hospital stay were not significantly different in the two groups.The risk of major bleeding during induction chemotherapy in adolescents and adults with acute myeloid leukemia (except acute promyelocytic leukemia, which we did not study) was similar with platelet-transfusion thresholds of 20,000 per cubic millimeter and 10,000 per cubic millimeter (or 10,000 to 20,000 per cubic millimeter when body temperature exceeded 38 degrees C, there was active bleeding, or invasive procedures were needed). Use of the lower threshold reduced platelet use by 21.5 percent.

Published
1997

49. Molecular remission in PML/RAR alpha-positive acute promyelocytic leukemia by combined all-trans retinoic acid and idarubicin (AIDA) therapy. Gruppo Italiano-Malattie Ematologiche Maligne dell'Adulto and Associazione Italiana di Ematologia ed Oncologia Pediatrica Cooperative Groups

Author

F, Mandelli, D, Diverio, G, Avvisati, A, Luciano, T, Barbui, C, Bernasconi, G, Broccia, R, Cerri, M, Falda, G, Fioritoni, F, Leoni, V, Liso, M C, Petti, F, Rodeghiero, G, Saglio, M L, Vegna, G, Visani, U, Jehn, R, Willemze, P, Muus, P G, Pelicci, A, Biondi, and F, Lo Coco

Subjects
Adult, Male, Neoplasm, Residual, Adolescent, Oncogene Proteins, Fusion, Leukocytosis, Tretinoin, Polymerase Chain Reaction, Disease-Free Survival, Translocation, Genetic, Leukemia, Promyelocytic, Acute, Bone Marrow, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Humans, Prospective Studies, Child, Aged, Chromosomes, Human, Pair 15, Antibiotics, Antineoplastic, Remission Induction, Syndrome, Middle Aged, Neoplasm Proteins, Treatment Outcome, Child, Preschool, Female, Idarubicin, Chromosomes, Human, Pair 17
Abstract

Two hundred fifty-three patients with newly diagnosed acute promyelocytic leukemia (APL) were eligible to enter the multicentric GIMEMA-AIEOP "AIDA" trial during the period July 1993 to February 1996. As a mandatory prerequisite for eligibility, all patients had genetic evidence of the specific t(15;17) lesion in their leukemic cells confirmed by karyotyping or by reverse transcription-polymerase chain reaction (RT-PCR) of the PML/RAR alpha fusion gene (the latter available in 247 cases). Median age was 37.8 years (range, 2.2 to 73.9). Induction treatment consisted of oral all-trans retinoic acid (ATRA), 45 mg/m2/d until complete remission (CR), given with intravenous Idarubicin, 12 mg/m2/d on days 2, 4, 6, and 8. Three polychemotherapy cycles were given as consolidation. Hematologic and molecular response by RT-PCR was assessed after induction and after consolidation. At the time of analysis, 240 of the 253 eligible patients were evaluable for induction. Of these, 11 (5%) died of early complications and 229 (95%) achieved hematologic remission. No cases of resistant leukemia were observed. Of 139 cases studied by RT-PCR after induction, 84 (60.5%) were PCR-negative and 55 (39.5%) PCR-positive. One hundred sixty-two patients were evaluable by RT-PCR at the end of consolidation. Of these, 159 (98%) tested PCR-negative and 3 (2%), PCR-positive. After a median follow up of 12 months (range, 0 to 33), the estimated actuarial event-free survival for the whole series of 253 eligible patients was 83% +/- 2.6% and 79% +/- 3.2% at 1 and 2 years, respectively. This study indicates that the AIDA protocol is a well-tolerated regimen that induces molecular remission in almost all patients with PML/RAR alpha-positive APL. Preliminary survival data suggest that a remarkable cure rate can be obtained with this treatment.

Published
1997

50. Transcription of latent and replicative Epstein-Barr-virus genes in bone-marrow and peripheral-blood mononuclear cells of healthy donors

Author

R, Gonnella, A, Angeloni, A, Calogero, A, Farina, R, Santarelli, G, Gentile, W, Arcese, P, Martino, F, Mandelli, L, Frati, A, Faggioni, and G, Ragona

Subjects
Viral Matrix Proteins, Herpesvirus 4, Human, Viral Proteins, Genes, Viral, Bone Marrow, Animals, Humans, Polymerase Chain Reaction, Cell Line
Abstract

Reverse-transcriptase polymerase chain reaction has been used to analyze the expression of 2 latent genes (EBNA-1 and LMP-1) and one replicative gene (BZLF-1) of Epstein-Barr virus in mononuclear cells from bone marrow and peripheral blood of healthy donors. EBV-gene transcription was detected in 8 out of 15 bone-marrow samples. Among these, 5 allowed the detection of latency-associated transcripts in the absence of BZLF-1 expression. Only one sample showed positivity for expression of both latent and lytic genes. In 2 cases, BZLF-1 was the only transcript detected. In peripheral blood, 4 out of 7 samples showed evidence of EBNA-1 transcription; LMP-1 was expressed in 5 samples, and in 2 cases concomitant expression of EBNA-1 and BZLF-1 was detected. These results provide a direct demonstration by RT-PCR of EBV-gene transcription in bone-marrow-resident viral infected cells and suggest, in contrast to previous studies on peripheral blood, that LMP-1 and BZLF-1 are frequently transcribed also in absence of EBV-related disease. The heterogeneous viral gene expression found makes it difficult to define a pattern of viral latency in vivo which coincides with that described for lymphoblastoid or Burkitt's-lymphoma cell lines at different stages of differentiation.

Published
1997

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