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Implementing precision cancer medicine in the public health services of Norway: the diagnostic infrastructure and a cost estimate

dc.date.accessioned2018-02-07T14:13:57Z
dc.date.available2018-02-07T14:13:57Z
dc.date.created2017-05-18T13:18:41Z
dc.date.issued2017
dc.identifier.citationRee, Anne Hansen Russnes, Hege Elisabeth Giercksky Heinrich, Daniel Dueland, Svein Pedersen, Kjetil Boye Nygaard, Vigdis Silwal-Pandit, Laxmi Østrup, Olga Hovig, Eivind Nygaard, Vegard Rødland, Einar Andreas Nakken, Sigve Øien, Janne T Johansen, Christin Bergheim, Inger Skarpeteig, Veronica Sathermugathevan, Menaka Sauer, Torill Lund-Iversen, Marius Beiske, Klaus Nasser, Salah Julsrud, Lars Reisse, Claudius Ruud, Espen Asak Flørenes, Vivi Ann Hagene, Kirsten T Aas, Eline Lurås, Hilde Soriano, Siv Johnsen Geitvik, Gry Aarum Lingjærde, Ole Christian Børresen-Dale, Anne-Lise Mælandsmo, Gunhild Flatmark, Kjersti . Implementing precision cancer medicine in the public health services of Norway: the diagnostic infrastructure and a cost estimate. ESMO Open Cancer Horizons. 2017, 2(2)
dc.identifier.urihttp://hdl.handle.net/10852/59924
dc.description.abstractObjective Through the conduct of an individual-based intervention study, the main purpose of this project was to build and evaluate the required infrastructure that may enable routine practice of precision cancer medicine in the public health services of Norway, including modelling of costs. Methods An eligible patient had end-stage metastatic disease from a solid tumour. Metastatic tissue was analysed by DNA sequencing, using a 50-gene panel and a study-generated pipeline for analysis of sequence data, supplemented with fluorescence in situ hybridisation to cover relevant biomarkers. Cost estimations compared best supportive care, biomarker-agnostic treatment with a molecularly targeted agent and biomarker-based treatment with such a drug. These included costs for medication, outpatient clinic visits, admission from adverse events and the biomarker-based procedures. Results The diagnostic procedures, which comprised sampling of metastatic tissue, mutation analysis and data interpretation at the Molecular Tumor Board before integration with clinical data at the Clinical Tumor Board, were completed in median 18 (8-39) days for the 22 study patients. The 23 invasive procedures (12 from liver, 6 from lung, 5 from other sites) caused a single adverse event (pneumothorax). Per patient, 0–5 mutations were detected in metastatic tumours; however, no actionable target case was identified for the current single-agent therapy approach. Based on the cost modelling, the biomarker-based approach was 2.5-fold more costly than best supportive care and 2.5-fold less costly than the biomarker-agnostic option. Conclusions The first project phase established a comprehensive diagnostic infrastructure for precision cancer medicine, which enabled expedite and safe mutation profiling of metastatic tumours and data interpretation at multidisciplinary tumour boards for patients with end-stage cancer. Furthermore, it prepared for protocol amendments, recently approved by the designated authorities for the second study phase, allowing more comprehensive mutation analysis and opportunities to define therapy targets.en_US
dc.languageEN
dc.language.isoenen_US
dc.publisherBMJ on behalf of the European Society of Medical Oncology (ESMO)
dc.rightsAttribution-NonCommercial 4.0 International
dc.rights.urihttps://creativecommons.org/licenses/by-nc/4.0/
dc.titleImplementing precision cancer medicine in the public health services of Norway: the diagnostic infrastructure and a cost estimateen_US
dc.typeJournal articleen_US
dc.creator.authorRee, Anne Hansen
dc.creator.authorRussnes, Hege Elisabeth Giercksky
dc.creator.authorHeinrich, Daniel
dc.creator.authorDueland, Svein
dc.creator.authorPedersen, Kjetil Boye
dc.creator.authorNygaard, Vigdis
dc.creator.authorSilwal-Pandit, Laxmi
dc.creator.authorØstrup, Olga
dc.creator.authorHovig, Eivind
dc.creator.authorNygaard, Vegard
dc.creator.authorRødland, Einar Andreas
dc.creator.authorNakken, Sigve
dc.creator.authorØien, Janne T
dc.creator.authorJohansen, Christin
dc.creator.authorBergheim, Inger
dc.creator.authorSkarpeteig, Veronica
dc.creator.authorSathermugathevan, Menaka
dc.creator.authorSauer, Torill
dc.creator.authorLund-Iversen, Marius
dc.creator.authorBeiske, Klaus
dc.creator.authorNasser, Salah
dc.creator.authorJulsrud, Lars
dc.creator.authorReisse, Claudius
dc.creator.authorRuud, Espen Asak
dc.creator.authorFlørenes, Vivi Ann
dc.creator.authorHagene, Kirsten T
dc.creator.authorAas, Eline
dc.creator.authorLurås, Hilde
dc.creator.authorSoriano, Siv Johnsen
dc.creator.authorGeitvik, Gry Aarum
dc.creator.authorLingjærde, Ole Christian
dc.creator.authorBørresen-Dale, Anne-Lise
dc.creator.authorMælandsmo, Gunhild
dc.creator.authorFlatmark, Kjersti
cristin.unitcode185,53,82,0
cristin.unitnameKlinikk for indremedisin og laboratoriefag
cristin.ispublishedtrue
cristin.fulltextoriginal
cristin.qualitycode1
dc.identifier.cristin1470800
dc.identifier.bibliographiccitationinfo:ofi/fmt:kev:mtx:ctx&ctx_ver=Z39.88-2004&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.jtitle=ESMO Open Cancer Horizons&rft.volume=2&rft.spage=&rft.date=2017
dc.identifier.jtitleESMO Open Cancer Horizons
dc.identifier.volume2
dc.identifier.issue2
dc.identifier.doihttp://dx.doi.org/10.1136/esmoopen-2017-000158
dc.identifier.urnURN:NBN:no-62600
dc.type.documentTidsskriftartikkelen_US
dc.type.peerreviewedPeer reviewed
dc.source.issn2059-7029
dc.identifier.fulltextFulltext https://www.duo.uio.no/bitstream/handle/10852/59924/2/Ree%2BESMOOpen2017.pdf
dc.type.versionPublishedVersion
cristin.articleide000158


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