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Please use this identifier to cite or link to this item: https://ahro.austin.org.au/austinjspui/handle/1/11992
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dc.contributor.authorJonker, D Jen
dc.contributor.authorKarapetis, C Sen
dc.contributor.authorHarbison, Cen
dc.contributor.authorO'Callaghan, Christopher Jen
dc.contributor.authorTu, Den
dc.contributor.authorSimes, R Jen
dc.contributor.authorMalone, D Pen
dc.contributor.authorLanger, Cen
dc.contributor.authorTebbutt, Niall Cen
dc.contributor.authorPrice, Timothy Jen
dc.contributor.authorShapiro, Jen
dc.contributor.authorSiu, L Len
dc.contributor.authorWong, R P Wen
dc.contributor.authorBjarnason, Gen
dc.contributor.authorMoore, M Jen
dc.contributor.authorZalcberg, John Ren
dc.contributor.authorKhambata-Ford, Sen
dc.date.accessioned2015-05-16T01:37:39Z
dc.date.available2015-05-16T01:37:39Z
dc.date.issued2013-12-12en
dc.identifier.citationBritish Journal of Cancer 2013; 110(3): 648-55en
dc.identifier.govdoc24335920en
dc.identifier.otherPUBMEDen
dc.identifier.urihttps://ahro.austin.org.au/austinjspui/handle/1/11992en
dc.description.abstractAnti-EGFR antibody, cetuximab, improves overall survival (OS) in K-ras wild-type chemotherapy-refractory colorectal cancer. Epidermal growth factor receptor ligand epiregulin (EREG) gene expression may further predict cetuximab benefit.Tumour samples from a phase III clinical trial of cetuximab plus best supportive care (BSC) vs BSC alone (CO.17) were analysed for EREG mRNA gene expression. Predictive effects of high vs low EREG on OS and progression-free survival (PFS) were examined for treatment-biomarker interaction.Both EREG and K-ras status were ascertained in 385 (193 cetuximab, 192 BSC) tumour samples. Within the high EREG and K-ras wild-type status ('co-biomarker')-positive group (n=139, 36%), median PFS was 5.4 vs 1.9 months (hazard ratio (HR) 0.31; P<0.0001), and median OS was 9.8 vs 5.1 months (HR 0.43; P<0.001) for cetuximab vs BSC, respectively. In the rest (n=246, 64%), PFS (HR 0.82; P=0.12) and OS (HR 0.90; P=0.45) were not significantly different. Test for treatment interaction showed a larger cetuximab effect on OS (HR 0.52; P=0.007) and PFS (HR 0.49; P=0.001) in the co-biomarker-positive group.In pre-treated K-ras wild-type status colorectal cancer, patients with high EREG gene expression appear to benefit more from cetuximab therapy compared with low expression. Epiregulin as a selective biomarker requires further evaluation.en
dc.language.isoenen
dc.subject.otherAdulten
dc.subject.otherAgeden
dc.subject.otherAged, 80 and overen
dc.subject.otherAntibodies, Monoclonal, Humanized.administration & dosageen
dc.subject.otherClinical Trials, Phase III as Topicen
dc.subject.otherColorectal Neoplasms.drug therapy.genetics.pathologyen
dc.subject.otherDisease-Free Survivalen
dc.subject.otherEpidermal Growth Factor.biosynthesis.geneticsen
dc.subject.otherEpiregulinen
dc.subject.otherFemaleen
dc.subject.otherGene Expression Regulation, Neoplasticen
dc.subject.otherHumansen
dc.subject.otherMaleen
dc.subject.otherMiddle Ageden
dc.subject.otherMutationen
dc.subject.otherNeoplasm Stagingen
dc.subject.otherTumor Markers, Biological.geneticsen
dc.subject.otherras Proteins.geneticsen
dc.titleEpiregulin gene expression as a biomarker of benefit from cetuximab in the treatment of advanced colorectal cancer.en
dc.typeJournal Articleen
dc.identifier.journaltitleBritish Journal of Canceren
dc.identifier.affiliationNCIC - Clinical Trials Group, Queens University, Cancer Research Institute, 10 Stuart Street, Kingston, ON K7P 3E3, Canadaen
dc.identifier.affiliationNational Health and Medical Research Council Clinical Trials Centre, University of Sydney, ABN 15 211 513 464, Camperdown, NSW 1450, Australiaen
dc.identifier.affiliationFlinders Medical Centre and Flinders University, Flinders Drive, Bedford Park, Adelaide, SA 5042, Australiaen
dc.identifier.affiliationPeter MacCallum Cancer Centre, Australasian Gastrointestinal Trials Group, University of Melbourne, 1 Street Andrews Place, East Melbourne, VIC 3002, Australiaen
dc.identifier.affiliationCabrini Hospital and Monash University, Isabella Street, Malvern, VIC 3144, Australiaen
dc.identifier.affiliationThe Queen Elizabeth Hospital and University of Adelaide, 28 Woodville Road, Woodville South SA 5011, Australiaen
dc.identifier.affiliationAustin Health and University of Melbourne, 145 Studley Road, Heidelberg, VIC 3084, Australiaen
dc.identifier.affiliationThe Ottawa Hospital Research Institute, University of Ottawa, 501 Smyth Road, Ottawa, ON K1H 8L6, Canadaen
dc.identifier.affiliationResearch and Development, Bristol-Myers Squibb, 100 Nassau Park Boulevard, Princeton, NJ 08540, USAen
dc.identifier.affiliationGenetech Inc., 1 Dna Way, South San Francisco, CA 94080, USAen
dc.identifier.affiliationPrincess Margaret Hospital and University of Toronto, 610 University Avenue, Suite 5-718, Toronto, ON M5G 2M9, Canadaen
dc.identifier.affiliationSunnybrook Health Sciences Centre, University of Toronto, 2075 Bayview Avenue, Toronto, ON M4N 3M5, Canadaen
dc.identifier.affiliationCancercare Manitoba, St Boniface General Hospital, 409 Tache Avenue, Rm L1-102, Winnipeg, MB R2H 2A6, Canadaen
dc.identifier.doi10.1038/bjc.2013.753en
dc.description.pages648-55en
dc.relation.urlhttps://pubmed.ncbi.nlm.nih.gov/24335920en
dc.type.austinJournal Articleen
local.name.researcherO'Callaghan, Christopher J
item.openairetypeJournal Article-
item.cerifentitytypePublications-
item.grantfulltextnone-
item.fulltextNo Fulltext-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.languageiso639-1en-
crisitem.author.deptClinical Pharmacology and Therapeutics-
crisitem.author.deptMedical Oncology-
crisitem.author.deptOlivia Newton-John Cancer Wellness and Research Centre-
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