Literature DB >> 21796439

A single-arm pilot phase II study of gefitinib and irinotecan in children with newly diagnosed high-risk neuroblastoma.

Wayne L Furman1, Lisa M McGregor, M Beth McCarville, Mihaela Onciu, Andrew M Davidoff, Sandy Kovach, Dana Hawkins, Valerie McPherson, Peter J Houghton, Catherine A Billups, Jianrong Wu, Clinton F Stewart, Victor M Santana.   

Abstract

BACKGROUND: Gefitinib potently inhibits neuroblastoma proliferation in vitro, and the gefitinib/irinotecan combination shows greater than additive activity against neuroblastoma xenografts. This Phase II pilot study estimated the rate of response to two courses of intravenous irinotecan plus oral gefitinib in children with untreated high-risk neuroblastoma.
METHODS: Two courses of irinotecan [15 mg/m(2)/day (daily ×5)×2] were combined with 12 daily doses of gefitinib (112.5 mg/m(2)/day). Response was assessed after 6 weeks. A response rate >55% was sought.
RESULTS: Of the 23 children enrolled, 19 were evaluable for response. Median age at diagnosis was 3.1 years (range, 18 days-12.7 years). Most patients were older than 24 months (n = 20; 87%), male (n = 18; 78%), white (n = 16; 70%), had INSS 4 disease (n = 19; 83%), and had adrenal primary tumors (n = 18; 78%); nine patients (39%) had amplified tumor MYCN. The toxicity of gefitinib/irinotecan was mild and reversible (nausea, 5/20; diarrhea, 8/20; vomiting, 7/20). Five patients had partial responses; 9 others had a 23%-60% decrease in primary tumor volume and/or improved MIBG scans or decreased bone or bone marrow tumor burden. Median (range) systemic irinotecan exposure (AUC) was 283 ng/ml*hr (range, 163-890 ng/ml*hr) and 28 ng/ml*hr (3.6-297 ng/ml*hr) for the active metabolite, SN-38. No relation was observed between response and tumor expression of EGFR, MRP2-4, ABCG2, and Pgp.
CONCLUSIONS: Although the gefitinib/irinotecan combination was very tolerable and induced responses, it was not sufficiently active to warrant further investigation. Initial investigational studies of this type can preclude the necessity for larger, longer, and costlier trials.

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Year:  2011        PMID: 21796439      PMCID: PMC3232294          DOI: 10.1007/s10637-011-9724-3

Source DB:  PubMed          Journal:  Invest New Drugs        ISSN: 0167-6997            Impact factor:   3.850


  58 in total

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4.  Expression of multidrug transporter MRP4/ABCC4 is a marker of poor prognosis in neuroblastoma and confers resistance to irinotecan in vitro.

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Review 5.  The role of the multidrug resistance-associated protein 1 gene in neuroblastoma biology and clinical outcome.

Authors:  Marina Pajic; Murray D Norris; S L Cohn; Michelle Haber
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6.  Phase I trial of oral irinotecan and temozolomide for children with relapsed high-risk neuroblastoma: a new approach to neuroblastoma therapy consortium study.

Authors:  Lars M Wagner; Judith G Villablanca; Clinton F Stewart; Kristine R Crews; Susan Groshen; C Patrick Reynolds; Julie R Park; John M Maris; Randall A Hawkins; Heike E Daldrup-Link; Hollie A Jackson; Katherine K Matthay
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8.  Gefitinib in combination with oral topotecan and cyclophosphamide in relapsed neuroblastoma: pharmacological rationale and clinical response.

Authors:  Alberto Donfrancesco; Maria Antonietta De Ioris; Heather Prudence McDowell; Maria Debora De Pasquale; Ilaria Ilari; Alessandro Jenkner; Aurora Castellano; Samantha Cialfi; Clementina De Laurentis; Carlo Dominici
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10.  Tyrosine kinase inhibitor enhances the bioavailability of oral irinotecan in pediatric patients with refractory solid tumors.

Authors:  Wayne L Furman; Fariba Navid; Najat C Daw; M Beth McCarville; Lisa M McGregor; Sheri L Spunt; Carlos Rodriguez-Galindo; John C Panetta; Kristine R Crews; Jianrong Wu; Amar J Gajjar; Peter J Houghton; Victor M Santana; Clinton F Stewart
Journal:  J Clin Oncol       Date:  2009-08-17       Impact factor: 44.544

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2.  Validation of a prognostic multi-gene signature in high-risk neuroblastoma using the high throughput digital NanoString nCounter™ system.

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4.  The role of inherited TPMT and COMT genetic variation in cisplatin-induced ototoxicity in children with cancer.

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Journal:  Clin Pharmacol Ther       Date:  2013-06-11       Impact factor: 6.875

5.  Combination of bevacizumab, irinotecan, and temozolomide for refractory or relapsed neuroblastoma: Results of a phase II study.

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6.  Novel phage display-derived neuroblastoma-targeting peptides potentiate the effect of drug nanocarriers in preclinical settings.

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7.  Epigallocatechin-3-gallate and 6-OH-11-O-Hydroxyphenanthrene Limit BE(2)-C Neuroblastoma Cell Growth and Neurosphere Formation In Vitro.

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8.  Impact of Neoadjuvant Chemotherapy on Image-Defined Risk Factors in High-Risk Neuroblastoma.

Authors:  Sara A Mansfield; M Beth McCarville; John T Lucas; Matthew J Krasin; Sara M Federico; Victor M Santana; Wayne L Furman; Andrew M Davidoff
Journal:  Ann Surg Oncol       Date:  2021-07-02       Impact factor: 5.344

9.  Combination therapy with gefitinib and doxorubicin inhibits tumor growth in transgenic mice with adrenal neuroblastoma.

Authors:  Kumi Kawano; Yoshiyuki Hattori; Hiroshi Iwakura; Takashi Akamizu; Yoshie Maitani
Journal:  Cancer Med       Date:  2013-04-02       Impact factor: 4.452

Review 10.  Molecular profiling of childhood cancer: Biomarkers and novel therapies.

Authors:  Federica Saletta; Carol Wadham; David S Ziegler; Glenn M Marshall; Michelle Haber; Geoffrey McCowage; Murray D Norris; Jennifer A Byrne
Journal:  BBA Clin       Date:  2014-06-28
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