Network-guided identification of cancer-selective combinatorial therapies in ovarian cancer

Liye He; Daria Bulanova; Jaana Oikkonen; Antti Häkkinen; Kaiyang Zhang; Shuyu Zheng; Wenyu Wang; Erdogan Pekcan Erkan; Olli Carpén; Titta Joutsiniemi; Sakari Hietanen; Johanna Hynninen; Kaisa Huhtinen; Sampsa Hautaniemi; Anna Vähärautio; Jing Tang; Krister Wennerberg; Tero Aittokallio

doi:10.1093/bib/bbab272

Network-guided identification of cancer-selective combinatorial therapies in ovarian cancer

Brief Bioinform. 2021 Nov 5;22(6):bbab272. doi: 10.1093/bib/bbab272.

Authors

Liye He¹, Daria Bulanova², Jaana Oikkonen³, Antti Häkkinen⁴, Kaiyang Zhang³, Shuyu Zheng³, Wenyu Wang³, Erdogan Pekcan Erkan³, Olli Carpén³, Titta Joutsiniemi⁵, Sakari Hietanen⁶, Johanna Hynninen⁷, Kaisa Huhtinen⁷, Sampsa Hautaniemi⁷, Anna Vähärautio⁷, Jing Tang⁷, Krister Wennerberg⁸, Tero Aittokallio⁹

Affiliations

¹ Institute for Molecular Medicine Finland (FIMM), Helsinki, Finland.
² Biotech Research & Innovation Centre (BRIC) at the University of Copenhagen (UC), Helsinki, Finland.
³ ONCOSYS Research Program in UH, Helsinki, Finland.
⁴ University of Helsinki (UH), Helsinki, Finland.
⁵ Gynecologic oncology in Turku University Hospital, Helsinki, Finland.
⁶ ONCOSYS Research Program in UH and in University of Turku (UTU), Helsinki, Finland.
⁷ ONCOSYS Research Programme in UH, Helsinki, Finland.
⁸ Biotech Research & Innovation Centre (BRIC), Helsinki, Finland.
⁹ FIMM and OCBE/OUH, Helsinki, Finland.

Abstract

Each patient's cancer consists of multiple cell subpopulations that are inherently heterogeneous and may develop differing phenotypes such as drug sensitivity or resistance. A personalized treatment regimen should therefore target multiple oncoproteins in the cancer cell populations that are driving the treatment resistance or disease progression in a given patient to provide maximal therapeutic effect, while avoiding severe co-inhibition of non-malignant cells that would lead to toxic side effects. To address the intra- and inter-tumoral heterogeneity when designing combinatorial treatment regimens for cancer patients, we have implemented a machine learning-based platform to guide identification of safe and effective combinatorial treatments that selectively inhibit cancer-related dysfunctions or resistance mechanisms in individual patients. In this case study, we show how the platform enables prediction of cancer-selective drug combinations for patients with high-grade serous ovarian cancer using single-cell imaging cytometry drug response assay, combined with genome-wide transcriptomic and genetic profiles. The platform makes use of drug-target interaction networks to prioritize those combinations that warrant further preclinical testing in scarce patient-derived primary cells. During the case study in ovarian cancer patients, we investigated (i) the relative performance of various ensemble learning algorithms for drug response prediction, (ii) the use of matched single-cell RNA-sequencing data to deconvolute cell population-specific transcriptome profiles from bulk RNA-seq data, (iii) and whether multi-patient or patient-specific predictive models lead to better predictive accuracy. The general platform and the comparison results are expected to become useful for future studies that use similar predictive approaches also in other cancer types.

Keywords: combination synergy; drug combinations; machine learning; network visualization; ovarian cancer; precision oncology; toxic effects.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Algorithms
Combined Modality Therapy
Female
Humans
Ovarian Neoplasms / therapy*
Tumor Cells, Cultured