2020
DOI: 10.1080/0284186x.2020.1742377
|View full text |Cite
|
Sign up to set email alerts
|

Molecularly matched therapy in the context of sensitivity, resistance, and safety; patient outcomes in end-stage cancer – the MetAction study

Abstract: Background: In precision cancer medicine, the challenge is to prioritize DNA driver events, account for resistance markers, and procure sufficient information for treatment that maintains patient safety. The MetAction project, exploring how tumor molecular vulnerabilities predict therapy response, first established the required workflow for DNA sequencing and data interpretation (2014)(2015). Here, we employed it to identify molecularly matched therapy and recorded outcome in end-stage cancer (2016)(2017)(2018… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
2
1
1

Citation Types

0
7
0
3

Year Published

2020
2020
2024
2024

Publication Types

Select...
7
1

Relationship

3
5

Authors

Journals

citations
Cited by 11 publications
(10 citation statements)
references
References 33 publications
0
7
0
3
Order By: Relevance
“…Less than 7% of cancer patients were estimated to benefit from genome-guided anti-cancer therapies in the US in 2018 [ 9 ]. Other studies using genomic profiling approaches with individualized matching of molecular variant and drug, report low inclusion rate and modest overall rate of clinical benefit [ 10 ], although much higher than the first generation precision medicine trials in oncology [ 11 13 ]. This is probably due to increasing knowledge about actionable genes and driver mutations in tumour development, resistance mechanisms, a more refined diagnostic work-up and availability of new targeted therapeutics [ 14 ].…”
Section: Introductionmentioning
confidence: 99%
“…Less than 7% of cancer patients were estimated to benefit from genome-guided anti-cancer therapies in the US in 2018 [ 9 ]. Other studies using genomic profiling approaches with individualized matching of molecular variant and drug, report low inclusion rate and modest overall rate of clinical benefit [ 10 ], although much higher than the first generation precision medicine trials in oncology [ 11 13 ]. This is probably due to increasing knowledge about actionable genes and driver mutations in tumour development, resistance mechanisms, a more refined diagnostic work-up and availability of new targeted therapeutics [ 14 ].…”
Section: Introductionmentioning
confidence: 99%
“…We assembled an international data set of 13 published 5,[12][13][14][15] (n = 6) and nonpublished (n = 7) cases of ALK fusionpositive GI cancer patients treated with ALKi. We collected information about social and demographic characteristics of patients, primary tumor site and histology, ALK fusion partner or site of breakpoint, microsatellite status, or other baseline next-generation sequencing (NGS)/mutational data.…”
Section: Patient Populationmentioning
confidence: 99%
“…Det viktigaste viste seg å vere kompetansebygging blant alle involverte fagpersonar. I neste del av studien, med inklusjon av 26 pasientar frå mars 2016 til mars 2017, fekk ti av dei behandling basert på NGS-data frå metastatisk svulstvev (3). Av desse oppnådde to tarmkreftpasientar partiell behandlingsrespons som varte 10-17 veker før ny sjukdomsprogresjon.…”
Section: Laerdom Frå Metaction-studienunclassified
“…Hos tre studiepasientar med gastrointestinal kreft identifiserte vi ALK-eller ROS1-fusjon som antatt drivarmutasjon, kor crizotinib gjev overtydande behandlingseffektar ved avansert ikkje-småcella lungekreft (5,18). Men MetAction-pasientane hadde ingen effekt av crizotinib, noko som er ein brest for konseptet om biologisk målretta medikament utanfor etablert indikasjon (3). Konklusjon I MetAction-studien tok vi omsyn til svulstmutasjonar som tilsa resistens så vel som respons på terapi.…”
Section: Laerdom Frå Metaction-studienunclassified
See 1 more Smart Citation