The survival outcome of patients with metastatic colorectal cancer based on the site of metastases and the impact of molecular markers and site of primary cancer on metastatic pattern

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dc.contributor.authorPrasanna, Thiru
dc.contributor.authorKarapetis, C.S.
dc.contributor.authorRoder, David
dc.contributor.authorTie, Jeanne
dc.contributor.authorPadbury, Rob
dc.contributor.authorPrice, Timothy
dc.contributor.authorWong, Rachel
dc.contributor.authorShapiro, Jeremy
dc.contributor.authorNott, Louise M
dc.contributor.authorLee, Margaret
dc.contributor.authorChua, Yu Jo
dc.contributor.authorCraft, Paul
dc.contributor.authorPiantadosi, Cynthia
dc.contributor.authorSorich, Michael
dc.contributor.authorGibbs, Peter
dc.contributor.authorYip, Desmond
dc.date.accessioned2020-01-02T03:37:22Z
dc.date.issued2018
dc.date.updated2019-08-04T08:21:34Z
dc.description.abstractBackground: Pattern of spread in patients with metastatic colorectal cancer (mCRC) is variable and may reflect different biology in subsets of patients. This is a retrospective study to explore the outcome of patients with mCRC based on their site of metastasis at diagnosis and to explore the association between tumor characteristics [KRAS/RAS, BRAF, mismatch repair (MMR) status, site of primary] and the site of metastasis. Methods: Patients from two Australian databases were divided into six groups based on site of metastasis at time of diagnosis of metastatic disease; lung-only, liver-only, lymph node-only or any patients with brain, bone or peritoneal metastases. Primary endpoint was overall survival (OS) of each cohort compared with the rest of the population. A Mantel–Haenszel chi-squared test used to explore the association between site of metastasis and selected tumor characteristics. Results: Five thousand nine hundred and sixty-seven patients were included. In a univariate analysis, median OS was significantly higher when metastases were limited to lung or liver and shorter for those with brain, bone or peritoneal metastases (p < .001) in both datasets. BRAF mutation was strongly associated with peritoneal metastases (relative risk = 1.8, p < .001) with lower incidence of lung (RR = 0.3, p = .004) and liver (RR = 0.7, p = .005) limited metastases. Lung-only metastases were more frequent with KRAS/RAS mutation (RR = 1.4, p = .007). Left colon tumors were associated with bone (RR = 1.6, p < .001) and lung-only metastases (RR = 2.3, p = .001) while peritoneal spread was less frequent compared with right colon tumors (RR = 0.6, p < .001). Rectal cancer was associated with brain, bone and lung metastases (RR = 1.7; p = .002, 1.7; p < .001, 2.0; p < .001). Liver-only metastases were less frequent in deficient MMR tumors (RR = 0.7, p = .01). Conclusion: Survival duration with mCRC is related to the site of metastases with lung limited disease showing a more favorable survival outcome compared to other single metastatic site disease. The BRAF mutation and primary rectal cancer were associated with poor prognostic metastatic sites
dc.format.mimetypeapplication/pdfen_AU
dc.identifier.issn0284-186Xen_AU
dc.identifier.urihttp://hdl.handle.net/1885/196460
dc.language.isoen_AUen_AU
dc.publisherTaylor & Francisen_AU
dc.rights© 2018 Acta Oncologica Foundationen_AU
dc.sourceActa Oncologicaen_AU
dc.titleThe survival outcome of patients with metastatic colorectal cancer based on the site of metastases and the impact of molecular markers and site of primary cancer on metastatic patternen_AU
dc.typeJournal articleen_AU
local.bibliographicCitation.issue11en_AU
local.bibliographicCitation.startpage1438–1444en_AU
local.contributor.affiliationPrasanna, Thiru , Canberra Hospitalen_AU
local.contributor.affiliationKarapetis, C.S., Flinders Universityen_AU
local.contributor.affiliationRoder, David, University of South Australiaen_AU
local.contributor.affiliationTie, Jeanne, Walter and Eliza Hall Institute of Medical Researchen_AU
local.contributor.affiliationPadbury, Rob, Flinders Universityen_AU
local.contributor.affiliationPrice, Timothy, Queen Elizabeth Hospitalen_AU
local.contributor.affiliationWong, Rachel, The Walter and Eliza Hall Institute of Medical Researchen_AU
local.contributor.affiliationShapiro, Jeremy, Cabrini Hospital Malvernen_AU
local.contributor.affiliationNott, Louise M, Royal Hobart Hospital Department of Medical Oncology Hobarten_AU
local.contributor.affiliationLee, Margaret, Walter and Eliza Hall Institute of Medical Researchen_AU
local.contributor.affiliationChua, Yu Jo, College of Health and Medicine, ANUen_AU
local.contributor.affiliationCraft, Paul, College of Health and Medicine, ANUen_AU
local.contributor.affiliationPiantadosi, Cynthia, Flinders Medical Centreen_AU
local.contributor.affiliationSorich, Michael, Flinders Universityen_AU
local.contributor.affiliationGibbs, Peter, Walter and Eliza Hall Institute of Medical Researchen_AU
local.contributor.affiliationYip, Desmond, College of Health and Medicine, ANUen_AU
local.contributor.authoremailu3757667@anu.edu.auen_AU
local.contributor.authoruidChua, Yu Jo, u5101833en_AU
local.contributor.authoruidCraft, Paul, u3757667en_AU
local.contributor.authoruidYip, Desmond, u5086006en_AU
local.description.embargo2037-12-31
local.description.notesImported from ARIES
local.identifier.absfor111201 - Cancer Cell Biologyen_AU
local.identifier.absseo920102 - Cancer and Related Disordersen_AU
local.identifier.ariespublicationu5234101xPUB261en_AU
local.identifier.citationvolume57en_AU
local.identifier.doi10.1080/0284186X.2018.1487581en_AU
local.identifier.scopusID2-s2.0-85050571162
local.identifier.uidSubmittedByu5234101en_AU
local.publisher.urlhttps://www.routledge.com/en_AU
local.type.statusPublished Versionen_AU

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