Cristina Noberasco

Publications (44) View all

• Article: Phase I/II study of the tumour-targeting human monoclonal antibody-cytokine fusion protein L19-TNF in patients with advanced solid tumours.

  G Spitaleri, R Berardi, C Pierantoni, T De Pas, C Noberasco, C Libbra, R González-Iglesias, L Giovannoni, A Tasciotti, D Neri, H D Menssen, F de Braud
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  ABSTRACT: PURPOSE: L19-TNF is an armed antibody that selectively targets human TNF to extra domain B-fibronectin on tumour blood vessels. We performed a phase I/II first-in-man trial with L19-TNF monotherapy in metastatic solid cancer patients to study safety and signs of clinical activity. METHODS: Six cohorts of patients were treated with increasing (1.3-13 μg/kg) doses of intravenous L19-TNF on day 1, 3, and 5 of repeated 3-weekly cycles, and 12 colorectal cancer patients were treated at 13 μg/kg. PK, antibody formation, changes in lymphocyte subsets, 5-HIAA plasma levels as well as safety and clinical activity were analysed. RESULTS: Thirty-four patients received at least one L19-TNF dose. The serum half-life of L19-TNF at 13 μg/kg was 33.6 min, and maximum peak serum concentration was 73.14 μg/L. Mild chills, nausea and vomiting but no haemato- or unexpected toxicity were observed. Grade 3 lumbar pain in bone metastasis was the only dose-limiting toxicity found in one patient. Objective tumour responses were not detected. Transient stable disease occurred in 19 of 31 evaluable patients. CONCLUSIONS: Intravenous L19-TNF on day 1, 3, and 5 of a 3-weekly schedule was safe up to 13 μg/kg, but did not result in objective tumour responses. The maximally tolerated dose (MTD) was not reached, allowing for further dose escalation of L19-TNF possibly in combination with chemotherapy.
  Journal of Cancer Research and Clinical Oncology 11/2012; · 2.56 Impact Factor
• Source

  Available from: Gerardo Rosati

  Article: Optimizing clinical care in patients with advanced soft tissue sarcoma: a phase II study of a new schedule of high-dose continuous infusion ifosfamide and doxorubicin combination.

  T De Pas, G Rosati, G Spitaleri, C Boni, A Tucci, S Frustaci, R Scalamogna, D Radice, S Boselli, F Toffalorio, C Catania, C Noberasco, A Delmonte, F Vecchio, F de Braud
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  ABSTRACT: Ifosfamide and doxorubicin combination is an active regimen for patients with advanced soft tissue sarcomas (STS) but is burdened by high toxicity. A phase II trial was designed to assess the activity of continuous infusion ifosfamide and doxorubicin combination. Thirty-four chemotherapy-naive patients with advanced STS were treated with ifosfamide (13 g/m(2)/12 days as continuous infusion) and doxorubicin (75 mg/m(2) on day 8) every 28 days with granulocyte colony-stimulating factor. The major toxicity was hematological: grade 3/4 neutropenia, anemia and thrombocytopenia occurred in 63, 30 and 12% of patients, respectively. The disease control rate was 68% and the median time to progression was 7.1 months. Among leiomyosarcomas, 2 partial responses and 4 stable diseases were observed. Our study confirms that the ifosfamide and doxorubicin combination has a very low non-hematological toxicity profile. This regimen attained a high disease control rate with moderate activity. Further investigation into leiomyosarcoma is warranted.
  Chemotherapy 01/2011; 57(3):217-24. · 1.82 Impact Factor
• Article: A FOLFIRI-induced complete tumor response in a patient with FOLFOX-refractory metastatic duodenal adenocarcinoma.

  Chiara Catania, G Pelosi, N Fazio, R Biffi, G Spitaleri, C Noberasco, M G Zampino, A Maggioni, G Trifirò, F Toffalorio, P Della Vigna, F De Braud, T De Pas
  Acta oncologica (Stockholm, Sweden) 01/2010; 49(1):120-1. · 2.27 Impact Factor
• Article: Expression of gemcitabine- and cisplatin-related genes in non-small-cell lung cancer.

  F Toffalorio, E Giovannetti, T De Pas, D Radice, G Pelosi, M Manzotti, D Minocci, L Spaggiari, G Spitaleri, C Noberasco, C Catania, S Boselli, R Danesi, F de Braud
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  ABSTRACT: The aim of this study was to investigate the influence of histology and site of analysis (primary tumor versus lymph node) on the expression of genes involved in gemcitabine and cisplatin activity in non-small-cell lung cancer (NSCLC). Excision repair cross-complementing-1 (ERCC1), human equilibrative nucleoside transporter-1 (hENT1), deoxycytidine kinase (dCK), 5'-nucleotidase (5'-NT), cytidine deaminase (CDA) and ribonucleotide-reductase regulatory subunits (RRM1 and RRM2) were analyzed by quantitative-reverse transcription-PCR in 88 microdissected samples from 69 chemonaive patients. The results showed different patterns of expression for all studied genes, suggesting a possible stratification of the patients. No difference was observed between primary tumor and lymph node metastasis, as well as in adenocarcinoma and squamous-cell carcinoma specimens, while we found a correlation between the CDA-A79C polymorphism and gene expression levels. These data suggest a similar genetic susceptibility to gemcitabine-cisplatin regimens for squamous cell and adenocarcinoma and support the use of both lymph node and primary tumor for the expression profiling of NSCLC.
  The Pharmacogenomics Journal 11/2009; 10(3):180-90. · 4.54 Impact Factor
• Source

  Available from: oxfordjournals.org

  Article: Gemcitabine and pemetrexed combination: the key role of the sequence of drugs administration.

  T M De Pas, F Toffalorio, C Catania, C Noberasco, G Spitaleri, L Spaggiari, F De Braud
  Annals of Oncology 09/2009; 20(10):1747-8. · 6.43 Impact Factor