New insights into markers for distinguishing neuroendocrine prostate cancer: evidence from single-cell analysis
Hailang Luo, Boyang Li, Meng Zhang, Hongqun Wang, Zongyao Hao, Qintao Ge, Chaozhao Liang

TL;DR
This study uses single-cell analysis to identify new biomarkers for neuroendocrine prostate cancer, which could help in early detection and treatment.
Contribution
The study identifies ASCL1 and WDFY4 as novel potential markers for distinguishing neuroendocrine prostate cancer.
Findings
Five distinct expression programs were identified in prostate cancer cells, with Module 3 showing NEPC patterns.
High Module 3 proportion correlates with poor clinical outcomes and advanced cancer stages.
ASCL1 and WDFY4 expression increases during progression to NEPC and is validated by immunohistochemistry.
Abstract
Neuroendocrine prostate cancer (NEPC) is a highly aggressive malignancy with few effective treatment options. The identification of reliable biomarkers for NEPC is essential for early detection and intervention. We combined single-cell and bulk transcriptome analysis to identify novel markers of NEPC. InferCNV to assess copy number variations and leveraging consensus non-negative matrix factorization (cNMF) to characterize transcriptional programs. Pseudotime analysis was used to decipher prostate cancer (PCa) progression differentiation trajectory. BayesPrism integrates single-cell results and TCGA-PRAD sequencing information to further study prognostic features. Immunohistochemistry (IHC) was performed to validate the elevated expression of ASCL1 and WDFY4 in NEPC. We identified five distinct expression programs of PCa malignant epithelial cells, where Module 3 presented NEPC…
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Taxonomy
TopicsProstate Cancer Treatment and Research · Cancer Immunotherapy and Biomarkers · Receptor Mechanisms and Signaling
