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Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/19234
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dc.contributor.authorBrandes, Alba A-
dc.contributor.authorCarpentier, Antoine F-
dc.contributor.authorKesari, Santosh-
dc.contributor.authorSepulveda-Sanchez, Juan M-
dc.contributor.authorWheeler, Helen R-
dc.contributor.authorChinot, Olivier-
dc.contributor.authorCher, Lawrence M-
dc.contributor.authorSteinbach, Joachim P-
dc.contributor.authorCapper, David-
dc.contributor.authorSpecenier, Pol-
dc.contributor.authorRodon, Jordi-
dc.contributor.authorCleverly, Ann-
dc.contributor.authorSmith, Claire-
dc.contributor.authorGueorguieva, Ivelina-
dc.contributor.authorMiles, Colin-
dc.contributor.authorGuba, Susan C-
dc.contributor.authorDesaiah, Durisala-
dc.contributor.authorLahn, Michael M-
dc.contributor.authorWick, Wolfgang-
dc.date2016-02-21-
dc.date.accessioned2018-09-13T00:21:14Z-
dc.date.available2018-09-13T00:21:14Z-
dc.date.issued2016-08-
dc.identifier.citationNeuro-oncology 2016; 18(8): 1146-1456-
dc.identifier.urihttps://ahro.austin.org.au/austinjspui/handle/1/19234-
dc.description.abstractThe combination of galunisertib, a transforming growth factor (TGF)-β receptor (R)1 kinase inhibitor, and lomustine was found to have antitumor activity in murine models of glioblastoma. Galunisertib (300 mg/day) was given orally 14 days on/14 days off (intermittent dosing). Lomustine was given as approved. Patients were randomized in a 2:1:1 ratio to galunisertib + lomustine, galunisertib monotherapy, or placebo + lomustine. The primary objective was overall survival (OS); secondary objectives were safety, pharmacokinetics (PKs), and antitumor activity. One hundred fifty-eight patients were randomized: galunisertib + lomustine (N = 79), galunisertib (N = 39), and placebo + lomustine (N = 40). Baseline characteristics were: male (64.6%), white (75.3%), median age 58 years, ECOG performance status (PS) 1 (63.3%), and primary glioblastoma (93.7%). The PKs of galunisertib were not altered with lomustine, and galunisertib had a median half-life of ∼8 hours. Median OS in months (95% credible interval [CrI]) for galunisertib + lomustine was 6.7 (range: 5.3-8.5), 8.0 (range: 5.7-11.7) for galunisertib alone, and 7.5 (range: 5.6-10.3) for placebo + lomustine. There was no difference in OS for patients treated with galunisertib + lomustine compared with placebo + lomustine [P (HR < 1) = 26%]. Median progression-free survival of ∼2 months was observed in all 3 arms. Among 8 patients with IDH1 mutation, 7 patients were treated with galunisertib (monotherapy or with lomustine); OS ranged from 4 to 17 months. Patients treated with galunisertib alone had fewer drug-related grade 3/4 adverse events (n = 34) compared with lomustine-treated patients (10% vs 26%). Baseline PS, post-discontinuation of bevacizumab, tumor size, and baseline levels of MDC/CCL22 were correlated with OS. Galunisertib + lomustine failed to demonstrate improved OS relative to placebo + lomustine. Efficacy outcomes were similar in all 3 arms. NCT01582269, ClinicalTrials.gov.-
dc.language.isoeng-
dc.subjectBayesian design-
dc.subjectPhase II randomized study-
dc.subjectantitumor activity-
dc.subjectgalunisertib monohydrate (LY2157299)-
dc.subjectpharmacokinetics-
dc.subjectsafety-
dc.titleA Phase II randomized study of galunisertib monotherapy or galunisertib plus lomustine compared with lomustine monotherapy in patients with recurrent glioblastoma.-
dc.typeJournal Article-
dc.identifier.journaltitleNeuro-oncology-
dc.identifier.affiliationDepartment of Oncology, Royal North Shore Hospital, St Leonards, Australiaen
dc.identifier.affiliationHospital Universitario 12 de Octubre, Madrid, Spainen
dc.identifier.affiliationUniversity of California San Diego Health System, La Jolla, California, USAen
dc.identifier.affiliationHôpital Avicenne, Paris 13 University, Bobigny, Franceen
dc.identifier.affiliationMedical Oncology Department, Bellaria-Maggiore Hospitals, Azienda USL - IRCCS Institute of Neurological Sciences, Bologna, Italyen
dc.identifier.affiliationAustin Health, Heidelberg, Victoria, Australiaen
dc.identifier.affiliationDepartment of Neuropathology, University Hospital Heidelberg, Heidelberg, Germanyen
dc.identifier.affiliationAntwerp University Hospital, Edegem, Belgiumen
dc.identifier.affiliationMedical Oncology, Vall d'Hebron University Hospital and Universitat Autònoma de Barcelona, Barcelona, Spainen
dc.identifier.affiliationDr. Senckenberg Institute of Neurooncology, University Hospital Frankfurt, Frankfurt, Germanyen
dc.identifier.affiliationEli Lilly and Company, Indianapolis, Indianaen
dc.identifier.affiliationEli Lilly and Company, Erl Wood, Englanden
dc.identifier.affiliationCHU Hôspital De La Timone, Rue Saint Pierre, Franceen
dc.identifier.affiliationNeurology Clinic, University of Heidelberg, Heidelberg, Germanyen
dc.identifier.doi10.1093/neuonc/now009-
dc.identifier.pubmedid26902851-
dc.type.austinClinical Trial, Phase II-
dc.type.austinJournal Article-
dc.type.austinRandomized Controlled Trial-
dc.type.austinResearch Support, Non-U.S. Gov't-
local.name.researcherCher, Lawrence M
item.languageiso639-1en-
item.cerifentitytypePublications-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.grantfulltextnone-
item.openairetypeJournal Article-
item.fulltextNo Fulltext-
crisitem.author.deptMedical Oncology-
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