Computational repurposing of oncology drugs through off-target drug binding interactions from pharmacological databases

Imogen R Walpole; Farzana Y Zaman; Peinan Zhao; Vikki M Marshall; Frank P Lin; David M Thomas; Mark Shackleton; Albert A Antolin; Malaka Ameratunga

doi:10.1002/ctm2.1657

Computational repurposing of oncology drugs through off-target drug binding interactions from pharmacological databases

Clin Transl Med. 2024 Apr;14(4):e1657. doi: 10.1002/ctm2.1657.

Authors

Imogen R Walpole¹, Farzana Y Zaman¹, Peinan Zhao², Vikki M Marshall², Frank P Lin^{3

4}, David M Thomas⁴, Mark Shackleton^{1

2}, Albert A Antolin^{5

6}, Malaka Ameratunga^{1

2}

Affiliations

¹ Department of Medical Oncology, The Alfred Hospital, Melbourne, Australia.
² School of Translational Medicine, Monash University, Melbourne, Australia.
³ NHMRC Clinical Trials Centre, University of Sydney, Sydney, Australia.
⁴ Garvan Institute of Medical Research, St Vincent's Clinical School, Faculty of Medicine, UNSW, Darlinghurst, Australia.
⁵ ProCURE, Catalan Institute of Oncology (ICO), Oncobell, Bellvitge Institute for Biomedical Research (IDIBELL), Barcelona, Spain.
⁶ The Division of Cancer Therapeutics, Center for Cancer Drug Discovery, The Institute of Cancer Research, London, UK.

Abstract

Purpose: Systematic repurposing of approved medicines for another indication may accelerate drug development in oncology. We present a strategy combining biomarker testing with drug repurposing to identify new treatments for patients with advanced cancer.

Methods: Tumours were sequenced with the Illumina TruSight Oncology 500 (TSO-500) platform or the FoundationOne CDx panel. Mutations were screened by two medical oncologists and pathogenic mutations were categorised referencing literature. Variants of unknown significance were classified as potentially pathogenic using plausible mechanisms and computational prediction of pathogenicity. Gain of function (GOF) mutations were evaluated through repurposing databases Probe Miner (PM), Broad Institute Drug Repurposing Hub (Broad Institute DRH) and TOPOGRAPH. GOF mutations were repurposing events if identified in PM, not indexed in TOPOGRAPH and excluding mutations with a known Food and Drug Administration (FDA)-approved biomarker. The computational repurposing approach was validated by evaluating its ability to identify FDA-approved biomarkers. The total repurposable genome was identified by evaluating all possible gene-FDA drug-approved combinations in the PM dataset.

Results: The computational repurposing approach was accurate at identifying FDA therapies with known biomarkers (94%). Using next-generation sequencing molecular reports (n = 94), a meaningful percentage of patients (14%) could have an off-label therapeutic identified. The frequency of theoretical drug repurposing events in The Cancer Genome Atlas pan-cancer dataset was 73% of the samples in the cohort.

Conclusion: A computational drug repurposing approach may assist in identifying novel repurposing events in cancer patients with no access to standard therapies. Further validation is needed to confirm a precision oncology approach using drug repurposing.

Keywords: drug repurposing; precision oncology; sequencing.

MeSH terms

Biomarkers
Drug Repositioning
Humans
Neoplasms* / drug therapy
Neoplasms* / genetics
Pharmaceutical Preparations
Precision Medicine

Substances

Pharmaceutical Preparations
Biomarkers