Clinical use of RNA sequencing and oncobox analytics to predict personalized targeted therapeutic efficacy.

6533b832fe1ef96bd129aca5

RESEARCH PRODUCT

Clinical use of RNA sequencing and oncobox analytics to predict personalized targeted therapeutic efficacy.

Marina Sekacheva Alex Glusker Viktoria Barbara Maxim Sorokin Anton Buzdin Alexey Moisseev Ella L. Kim Maria Suntsova Elena Poddubskaya Andrew Garazha Victor Tkachev Nurshat Gaifullin Nikolay M. Borisov Alf Giese

subject

Cancer Research Oncology business.industry Analytics Gene expression Mutation (genetic algorithm)medicine Cancer RNA Computational biology medicine.disease business

description

e13676 Background: Analysis of mutation profiles in cancer patients does not provide clinical benefits in 80-90% of cases in the US (Marquart et al., 2018). Gene expression analysis potentially complements standard detection of clinically relevant mutations. Methods: 239 adult late-stage cancer patients. RNA gene expression sequencing completed on solid tumor samples using FFPE blocks. Patient mRNA profiles were analyzed using Oncobox bioinformatics, prioritizing target drugs according to their personalized predicted efficacy. Summary reports were provided to oncologists and resulting treatment selection and outcomes were assessed. Results: As of February 2020, feedback was received from participating doctors for 224 patients; 34 patients died before therapy prescription, 52 patients received treatment other than targeted therapy (chemo, surgery, radiation, or palliative care), 75 patients received at least one targeted therapy (single or combination therapy) predicted to be effective based on Oncobox analysis (“RNAseq cohort”). 63 patients received chemo or other drug therapy predicted to be potentially ineffective from Oncobox analysis (“other cohort”). Therapeutic response was obtained on 46 patients with biopsies collected no longer than 6 months prior to analysis who had no further surgery (30 in the RNAseq cohort and 16 in the other cohort). 63% of the RNAseq cohort obtained either partial response or stable disease using Oncobox guided therapies, compared to 44% of the other cohort (19% increase of disease control). The RNAseq cohort had higher mean prior therapies (1.3) compared to the other cohort (0.8) indicating more advanced disease. The similarly designed WINTHER trial reported ~8% increase of disease control using gene expression-guided vs mutation-guided therapeutics in a cohort of advanced cancer patients averaging three prior therapies (Rodon et al., 2019). Conclusions: Collectively these data suggest that gene expression profiling provides a more clinically relevant therapeutic match, and better response rates, than mutation guided therapeutic treatments. This potentially results in improved clinical outcomes for cancer patients. Clinical trial information: NCT03724097.

year	journal	country	edition	language
2020-05-20	Journal of Clinical Oncology

https://doi.org/10.1200/jco.2020.38.15_suppl.e13676