Prostate cancer is a disease which poses an interesting clinical question: Should it be treated? Only a small subset of prostate cancers are aggressive and require removal and treatment to prevent metastatic spread. However, conventional diagnostics remain challenged to risk-stratify such patients; hence, new methods of approach to biomolecularly sub-classify the disease are needed. Here we use an unsupervised self-organising map approach to analyse live-cell Raman spectroscopy data obtained from prostate cell-lines; our aim is to exemplify this method to sub-stratify, at the single-cell-level, the cancer disease state using high-dimensional datasets with minimal preprocessing. The results demonstrate a new sub-clustering of the prostate cancer cell-line into two groups-protein-rich and lipid-rich sub-cellular components-which we believe to be mechanistically linked. This finding shows the potential for unsupervised machine learning to discover distinct disease-state features for more accurate characterisation of highly heterogeneous prostate cancer. Applications may lead to more targeted diagnoses, prognoses and clinical treatment decisions via molecularly-informed stratification that would benefit patients. A method that could discover distinct disease-state features that are mechanistically linked could also assist in the development of more effective broad-spectrum treatments that simultaneously target linked disease-state processes.
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| http://dx.doi.org/10.1038/s41598-024-83708-6 | DOI Listing |
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11700215 | PMC |
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