Coordinating single‐cell and bulk RNA‐seq in deciphering the intratumoral immune landscape and prognostic stratification of prostate cancer patients

Author:

Sun Zhou1,Wang Jie12,Zhang Qiang2,Meng Xiangdi1,Ma Zhaosen1,Niu Jiqiang1,Guo Rui1,Tran Lisa Jia3,Zhang Jing4,Liu Yunfei3,Ye Fangdie5ORCID,Ma Baoluo16

Affiliation:

1. Department of Urology China‐Japan Union Hospital of Jilin University Jilin China

2. Department of Urology The Second People's Hospital of Meishan City Meishan Sichuan China

3. Department of General, Visceral, and Transplant Surgery Ludwig‐Maximilians‐University Munich Munich Germany

4. Division of Basic Biomedical Sciences The University of South Dakota Sanford School of Medicine Vermillion South Dakota USA

5. Fudan Institute of Urology, Huashan Hospital Fudan University Shanghai China

6. Department of Urology, Xiangyang Central Hospital Affiliated Hospital of Hubei University of Arts and Science Xiangyang Hubei China

Abstract

AbstractIntroductionProstate cancer is a common cancer among male population. The aberrant expression of histone modifiers has been identified as a potential driving force in numerous cancer types. However, the mechanism of histone modifiers in the development of prostate cancer remains unknown.MethodsExpression profiles and clinical data were obtained from GSE70769, GSE46602, and GSE67980. Seruat R package was utilized to calculate the gene set enrichment of the histone modification pathway and obtain the Histone score. Least absolute shrinkage and selection operator (LASSO) and Cox regression analyses were employed to identify marker genes with prognostic value. Kaplan–Meier survival analysis was conducted to assess the efficacy of the prognostic model. In addition, microenvironment cell populations counter (MCPcounter), single‐sample gene set enrichment analysis (ssGSEA), and xCell algorithms were employed for immune infiltration analysis. Drug sensitivity prediction was performed using oncoPredict R package.ResultsWe screened differentially expressed genes (DEGs) between Histone‐high score (Histone‐H) and Histone‐low score (Histone‐L) groups, which were enriched in RNA splicing and DNA‐binding transcription factor binding pathways. We retained four prognostic marker genes, including TACC3, YWHAH, TAF1C and TTLL5. The risk model showed significant efficacy in stratification of the prognosis of prostate cancer patients in both internal and external cohorts (p < .0001 and p = .032, respectively). In addition, prognostic gene YWHAH was infiltrated in abundance of fibroblasts and highly correlated with Entinostat_1593 drug sensitivity score and the value of risk score.ConclusionWe innovatively developed a histone modification‐related prognostic model with high prognostic potency and identified YWHAH as possible diagnostic and therapeutic biomarkers for prostate cancer. It provides novel insights to address prostate cancer and enhance clinical outcomes, thereby opening up a new avenue for customized treatment alternatives.

Publisher

Wiley

Subject

Health, Toxicology and Mutagenesis,Management, Monitoring, Policy and Law,Toxicology,General Medicine

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