Simona Sammassimo
European Institute of Oncology
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Featured researches published by Simona Sammassimo.
Leukemia & Lymphoma | 2010
Paola Bertazzoni; Cristina Rabascio; Federica Gigli; Liliana Calabrese; Davide Radice; Angelica Calleri; Giuliana Gregato; Mara Negri; Sarah Liptrott; Simona Bassi; Luca Nassi; Simona Sammassimo; Daniele Laszlo; Lorenzo Preda; Giancarlo Pruneri; Laura Orlando; Giovanni Martinelli
The aim of this study was to investigate the efficacy of combined treatment with rituximab and subcutaneous cladribine in patients with newly diagnosed and relapsed chronic lymphocytic leukemia (CLL). Forty-three patients with active CLL or small lymphocytic lymphoma received rituximab 375 mg/m2 on day 1 and cladribine 0.1 mg/kg subcutaneously on days 2–6. The treatment was repeated every 4 weeks for a total of four cycles. Sixteen patients were pretreated. The overall response rate was 88% (50% complete remission and 38% partial remission). The median time to treatment failure was 37.9 months. Grade 4 neutropenia developed in 5% of patients. The data indicate that combination therapy with rituximab and cladribine is a valuable and safe treatment for patients with CLL.
Ecancermedicalscience | 2013
Angelo Gardellini; Federica Gigli; Aleksandra Babic; Giovanna Andreola; Davide Radice; Simona Sammassimo; Giovanni Martinelli; Daniele Laszlo
Purpose Granulocyte colony-stimulating factors (G-CSFs), filgrastim and lenograstim, are recognised to be useful in accelerating engraftment after autologous stem cell transplantation. Several forms of biosimilar non-glycosylated G-CSF have been approved by the European Medicines Agency, with limited published data supporting the clinical equivalence in peripheral blood stem cell mobilisation and recovery after autologous stem cell transplantation. Method With the aim of comparing cost-effective strategies in the use of G-CSF after autologous stem cell transplantation, we retrospectively evaluated 32 patients consecutively treated with biosimilar filgrastim XM02 (Tevagrastim) and 26 with lenograstim. All patients received G-CSF (biosimilar or lenograstim) at a dosage of 5 mcg/kg/day subcutaneously from day 5 to absolute neutrophil count of 1500/mmc for three days. Results The median time to absolute neutrophil count engraftment was 11 days for the filgrastim XM02 group and 12 days for the lenograstim group. As for platelets recovery, the median time was 12 days in both groups. The median number of G-CSF vials used for patients was 9.5 for Tevagrastim and 10.5 for lenograstim, reflecting a mean estimated cost of about 556.1 euros for Tevagrastim versus 932.2 euros for lenograstim (p< 0.001). The median days of febrile neutropenia were 1.5 and 1 for filgrastim XM02 and lenograstim, respectively. No adverse event related to the use of XM02 filgrastim was recorded. Conclusion In our experience, filgrastim XM02 and lenograstim showed comparable efficacy in shortening the period of neutropenia after cytoreduction and autologous stem cell transplantation, with a favourable cost effect for filgrastim XM02.
Hematological Oncology | 2016
Simona Sammassimo; Giancarlo Pruneri; Giovanna Andreola; Juan Montoro; Sara Steffanoni; Grzegorz S. Nowakowski; Sara Gandini; Mara Negri; Thomas M. Habermann; Markus Raderer; Zhi Ming Li; Pier Luigi Zinzani; Patrick Adam; Emanuele Zucca; Giovanni Martinelli
Primary lymphoma of the lung is a rare entity. Clinical features, optimal treatment, role of surgery and outcomes are not well defined, and the follow‐up is variable in published data. Clinical data of 205 patients who were confirmed to have bronchus mucosa‐associated lymphoid tissue lymphoma from December 1986 to December 2011 in 17 different centres worldwide were evaluated. Fifty‐five per cent of the patients were female. The median age at diagnosis was 62 (range 28–88) years. Only 9% had a history of exposure to toxic substances, while about 45% of the patients had a history of smoking. Ten per cent of the patients had autoimmune disease at presentation, and 19% patients had a reported preexisting lung disease. Treatment modalities included surgery alone in 63 patients (30%), radiotherapy in 3 (2%), antibiotics in 1 (1%) and systemic treatment in 128 (62%). Patients receiving a local approach, mainly surgical resection, experienced significantly improved progression‐free survival (p = 0.003) versus those receiving a systemic treatment. There were no other significant differences among treatment modalities. The survival data confirm the indolent nature of the disease. Local therapy (surgery or radiotherapy) results in long‐term disease‐free survival for patients with localized disease. Systemic treatment, including alkylating‐containing regimens, can be reserved to patients in relapse after incomplete surgical excision or for patients with advanced disease. Copyright
Archive | 2016
Corrado Tarella; Safaa Ramadan; Angela Gueli; Simona Sammassimo; Stefano Pileri
Sjogren syndrome is the second most prevalent autoimmune disease after rheumatoid arthritis. It is a slowly progressing systemic autoimmune disease characterized by lymphocytic infiltrates of the exocrine organs. The clinical spectrum and disease complications are broad, and approximately half of the patients develop systemic disorders during their disease course. Lymphoproliferative complications range from benign to malignant lymphoproliferation. Sjogren syndrome is associated with a higher risk of developing non-Hodgkin lymphoma compared to other autoimmune diseases. Non-Hodgkin lymphoma is thought to have a detrimental effect on the survival of Sjogren syndrome patients. For these reasons, we will review the risk of non-Hodgkin lymphoma in Sjogren syndrome patients. The prognosis and outcome of non-Hodgkin lymphoma following Sjogren syndrome will be summarized. Possible predictors and mechanisms of non-Hodgkin lymphoma development will be reviewed as well.
Blood | 2011
Simona Sammassimo; Giancarlo Pruneri; Patrick Adam; Stefano Pileri; Paola Rafaniello; Sara Steffanoni; Sara Gandini; Mara Negri; Thomas M. Habermann; Zhi Ming Li; Pier Luigi Zinzani; Markus Raderer; James O. Armitage; Dennis D. Weisenburger; Osnat Bairey; María Elena Cabrera; Emanuele Zucca; Benedetta Puccini; Gonzalo Gutiérrez-García; Ewa Kalinka-Warzocha; Andrea Carpaneto; Caroline Besson; Elena Porro; Franco Cavalli; Grzegorz S. Nowakowski; Giovanni Martinelli
Hematological Oncology | 2018
Nicola Stefano Fracchiolla; Silvia Artuso; Agostino Cortelezzi; Anna Maria Pelizzari; Paola Tozzi; Maurizio Bonfichi; Federica Bocchio; Livio Gargantini; Elisa De Rosa; Giuseppe Vighi; Lucia Prestini; Simona Sammassimo; Niccolò Frungillo; Maria Cristina Pasquini; Alessandra Ragazzi; Daniele Boghi; Alessia Pastore; Eraldo Lanzi; Giuseppe Gritti; Giulia Quaresmini; Simone Voltolini; Roberta Gaiardoni; Consuelo Corti; Maria C. Vilardo; Maria L. La Targia; Giacomo Berini; Massimo Magagnoli; Claudia Bacci; Dario Consonni; Alma Lisa Rivolta
Blood | 2016
Enrico Derenzini; Angela Gueli; Safaa Ramadan; Anna Vanazzi; Simona Sammassimo; Federica Gigli; Niccolò Frungillo; Riccardo Bruna; Alberto Agazzi; Alberto De Crescenzo; Rocco Pastano; Laura Lavinia Travaini; Chiara Grana; Laszlo Daniele; William Arcese; Corrado Tarella
Blood | 2015
Rocco Pastano; Giovanna Andreola; Federica Gigli; Simona Sammassimo; Mara Negri; Liptrott Jayne Sarah; Corrado Tarella
Blood | 2010
Simona Bassi; Simona Sammassimo; Federica Gigli; Giancarlo Pruneri; Paola Bertazzoni; Jessica Quarna; Emilia Cocorocchio; Daniele Laszlo; Mara Negri; Maria Teresa Lionetti; Anna Vanazzi; Alessandra Alietti; Alberto Agazzi; Angelo Gardellini; Giovanna Andreola; Lorenzo Preda; Rocco Pastano; Giovanni Martinelli
Blood | 2010
Simona Sammassimo; Giancarlo Pruneri; Stefano Pileri; Paola Rafaniello; Sara Steffanoni; Sara Gandini; Mara Negri; Pier Luigi Zinzani; Markus Raderer; Patrick Adam; James O. Armitage; Dennis D. Weisenburger; Osnat Bairey; María Elena Cabrera; Emanuele Zucca; Luigi Rigacci; Gonzalo Gutiérrez-García; Andrea Carpaneto; Caroline Besson; Ewa Kalinka Warzocha; Franco Cavalli; Giovanni Martinelli