Hyperpolarised 13C-MRI identifies the emergence of a glycolytic cell population within intermediate-risk human prostate cancer
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Authors
Sushentsev, Nikita
McLean, Mary A
Benjamin, Arnold JV
Brodie, Cara
Jones, Julia
Lamb, Benjamin W
Locke, Matthew J
Miller, Jodi L
Mills, Ian G
Priest, Andrew N
Robb, Fraser JL
Shah, Nimish
Schulte, Rolf S
Graves, Martin J
Journal Title
Nature Communications
ISSN
2041-1723
Publisher
Nature Research
Type
Article
This Version
VoR
Metadata
Show full item recordCitation
Sushentsev, N., McLean, M. A., Warren, A., Benjamin, A. J., Brodie, C., Frary, A., Gill, A., et al. Hyperpolarised 13C-MRI identifies the emergence of a glycolytic cell population within intermediate-risk human prostate cancer. Nature Communications https://doi.org/10.17863/CAM.78706
Abstract
Hyperpolarised magnetic resonance imaging (HP-13C-MRI) is an emerging clinical technique to detect [1-13C]lactate production in prostate cancer (PCa) following intravenous injection of hyperpolarised [1-13C]pyruvate. Here we differentiate clinically-significant PCa from indolent disease in a low/intermediate-risk population by correlating [1-13C]lactate labelling on MRI with the percentage of Gleason pattern 4 (%GP4) disease. Using immunohistochemistry and spatial transcriptomics, we show that HP-13C-MRI predominantly measures metabolism in the epithelial compartment of the tumour, rather than the stroma. MRI-derived tumour [1-13C]lactate labelling correlated with epithelial mRNA expression of the enzyme lactate dehydrogenase (LDHA and LDHB combined), and the ratio of lactate transporter expression between the epithelial and stromal compartments (epithelium-to-stroma MCT4). We observe similar changes in MCT4, LDHA, and LDHB between tumours with primary Gleason patterns 3 and 4 in an independent TCGA cohort. Therefore, HP-13C-MRI can metabolically phenotype clinically significant disease based on underlying metabolic differences in the epithelial and stromal tumour compartments.
Sponsorship
Prostate Cancer UK (PCUK; Grant PA14-012) and Cancer Research UK (CRUK; Grants C19212/A27150, C19212/A16628).
Identifiers
This record's DOI: https://doi.org/10.17863/CAM.78706
This record's URL: https://www.repository.cam.ac.uk/handle/1810/331260
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