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Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/30038
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dc.contributor.authorvan Dijk, Erik-
dc.contributor.authorvan Werkhoven, Erik-
dc.contributor.authorAsher, Rebecca-
dc.contributor.authorMooi, Jennifer K-
dc.contributor.authorEspinoza, David-
dc.contributor.authorvan Essen, Hendrik F-
dc.contributor.authorvan Tinteren, Harm-
dc.contributor.authorvan Grieken, Nicole C T-
dc.contributor.authorPunt, Cornelis J A-
dc.contributor.authorTebbutt, Niall C-
dc.contributor.authorYlstra, Bauke-
dc.date2022-05-23-
dc.date.accessioned2022-06-22T06:51:07Z-
dc.date.available2022-06-22T06:51:07Z-
dc.date.issued2022-10-01-
dc.identifier.citationInternational Journal of Cancer 2022; 151(7): 1166-1174en
dc.identifier.urihttps://ahro.austin.org.au/austinjspui/handle/1/30038-
dc.description.abstractThe VEGF-A monoclonal antibody bevacizumab is currently recommended for first-line treatment of all metastatic colorectal cancer (mCRC) patients. Cost-benefit ratio and side-effects however necessitate patient selection. A large retrospective yet nonrandomized study showed that patients with loss of chromosome 18q11.2-q12.1 in the tumor and treated with bevacizumab have 3 months improved median progression-free (PFS) and overall survival (OS) benefit compared to patients without this loss and/or treatment modality. Implementation for loss of chromosome 18q11.2-q12.1 as a marker in clinical practice mandates evidence in a randomized controlled trial for bevacizumab. Of the trials with randomization of chemotherapy vs chemotherapy with bevacizumab, the AGITG-MAX trial was the only one with tumor materials available. Chromosome 18q11.2-q12.1 copy number status was measured for 256 AGITG-MAX trial patients and correlated with PFS according to a predefined analysis plan with marker-treatment interaction as the primary end-point. Chromosome 18q11.2-q12.1 losses were detected in 71% of patients (181/256) characteristic for mCRC. Consistent with the nonrandomized study, significant PFS benefit of bevacizumab was observed in patients with chromosome 18q11.2-q12.1 loss (P = .009), and not in patients without 18q loss (P = .67). Although significance for marker-treatment interaction was not reached (Pinteraction  = .28), hazard ratio and 95% confidence interval of this randomized cohort (HRinteraction  = 0.72; 95% CI = 0.39-1.32) shows striking overlap with the nonrandomized study cohorts (HRinteraction  = 0.41; 95% CI = 0.32-0.8) supported by a nonsignificant Cochrane χ2 test (P = .11) for heterogeneity. We conclude that post hoc analysis of the AGITG-MAX RCT provides supportive evidence for chromosome 18q11.2-q12.1 as a predictive marker for bevacizumab in mCRC patients.en
dc.language.isoeng-
dc.subjectanti-VEGF monoclonal antibodyen
dc.subjectbevacizumaben
dc.subjectchromosome 18qen
dc.subjectmetastatic colorectal canceren
dc.subjectpredictive biomarkeren
dc.subjectrandomized controlled trialen
dc.titlePredictive value of chromosome 18q11.2-q12.1 loss for benefit from bevacizumab in metastatic colorectal cancer: A post hoc analysis of the randomized phase III-trial AGITG-MAX.en
dc.typeJournal Articleen
dc.identifier.journaltitleInternational Journal of Canceren
dc.identifier.affiliationOlivia Newton-John Cancer Research Instituteen
dc.identifier.affiliationMedical Oncologyen
dc.identifier.affiliationDepartment of Medicine, University of Melbourne, Melbourne, Australiaen
dc.identifier.affiliationPeter MacCallum Cancer Institute, Melbourne, Australiaen
dc.identifier.affiliationDepartment of Surgery, University of Melbourne, Melbourne, Australiaen
dc.identifier.affiliationDepartment of Biostatistics, NHMRC Clinical Trials Centre, University of Sydney, Camperdown, Australiaen
dc.identifier.affiliationBiometrics Department, Erasmus Medical Center, Rotterdam, The Netherlandsen
dc.identifier.affiliationDepartment of Pathology, Cancer Center Amsterdam, Amsterdam UMC, VU University Medical Center, Amsterdam, The Netherlandsen
dc.identifier.affiliationTrial and Datacenter, Princess Máxima Center for Pediatric Oncology, Utrecht, The Netherlandsen
dc.identifier.affiliationJulius Centre for Health Sciences and Primary Care, University Medical Centre Utrecht, Utrecht University, Utrecht, The Netherlandsen
dc.identifier.affiliationDepartment of Epidemiology, University Medical Centre Utrecht, Utrecht University, Utrecht, The Netherlandsen
dc.identifier.pubmedurihttps://pubmed.ncbi.nlm.nih.gov/35489024/en
dc.identifier.doi10.1002/ijc.34061en
dc.type.contentTexten
dc.identifier.orcid0000-0001-9479-3010en
dc.identifier.orcid0000-0002-4188-6149en
dc.identifier.orcid0000-0003-2613-5168en
dc.identifier.pubmedid35489024-
local.name.researcherMooi, Jennifer K
item.openairetypeJournal Article-
item.cerifentitytypePublications-
item.grantfulltextnone-
item.fulltextNo Fulltext-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.languageiso639-1en-
crisitem.author.deptOlivia Newton-John Cancer Research Institute-
crisitem.author.deptMedical Oncology-
crisitem.author.deptOlivia Newton-John Cancer Wellness and Research Centre-
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