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Series GSE269968 Query DataSets for GSE269968
Status Public on Jun 21, 2024
Title Cancer-associated fibroblasts (CAFs) gene signatures predict outcomes in breast and prostate tumor patients
Organism Homo sapiens
Experiment type Expression profiling by high throughput sequencing
Summary Over the last two decades, tumor-derived RNA expression signatures have been developed for the two most commonly diagnosed tumors worldwide, namely prostate and breast tumors, in order to improve both outcome prediction and treatment decision-making. In this context, molecular signatures gained by main components of the tumor microenvironment, such as cancer-associated fibroblasts (CAFs), have been explored as prognostic and therapeutic tools. Nevertheless, a deeper understanding of the significance of CAFs-related gene signatures in breast and prostate cancers still remains to be disclosed. RNA sequencing technology (RNA-seq) was employed to profile and compare the transcriptome of CAFs isolated from patients affected by breast and prostate tumors. The differentially expressed genes (DEGs) characterizing breast and prostate CAFs were intersected with data from public datasets derived from bulk RNA-seq profiles of breast and prostate tumor patients. Pathway enrichment analyses allowed us to appreciate the biological significance of the DEGs. K-means clustering was applied to construct CAFs-related gene signatures specific for breast and prostate cancer and to stratify independent cohorts of patients into high and low gene expression clusters. Kaplan-Meier survival curves and log-rank tests were employed to predict differences in the outcome parameters of the clusters of patients. Decision-tree analysis was used to validate the clustering results and boosting calculations were then employed to improve the results obtained by the decision-tree algorithm. Data obtained in breast CAFs allowed us to assess a signature that includes 8 genes (ITGA11, THBS1, FN1, EMP1, ITGA2, FYN, SPP1, and EMP2) belonging to pro-metastatic signaling routes, such as the focal adhesion pathway. Survival analyses indicated that the cluster of breast cancer patients showing a high expression of the aforementioned genes displays worse clinical outcomes. Next, we identified a prostate CAFs-related signature that includes 11 genes (IL13RA2, GDF7, IL33, CXCL1, TNFRSF19, CXCL6, LIFR, CXCL5, IL7, TSLP, and TNFSF15) associated with immune responses. A low expression of these genes was predictive of poor survival rates in prostate cancer patients. The results obtained were significantly validated through a two-step approach, based on unsupervised (clustering) and supervised (classification) learning techniques, showing a high prediction accuracy (≥ 90%) in independent RNA-seq cohorts. We identified a huge heterogeneity in the transcriptional profile of CAFs derived from breast and prostate tumors. Of note, the two novel CAFs-related gene signatures might be considered as reliable prognostic indicators and valuable biomarkers for a better management of breast and prostate cancer patients.
 
Overall design Identification of CAFs-related gene signatures for breast and prostate cancer patients by integrating RNA-seq data from both primary CAFs and cancer patients datasets.
 
Citation(s) 38937754
Submission date Jun 16, 2024
Last update date Jul 31, 2024
Contact name Rosamaria Lappano
E-mail(s) rosamaria.lappano@unical.it
Organization name University of Calabria
Street address via P. Bucci
City Rende
State/province Cs
ZIP/Postal code 87036
Country Italy
 
Platforms (1)
GPL34284 Illumina NovaSeq X Plus (Homo sapiens)
Samples (6)
GSM8331616 1370819
GSM8331617 1370820
GSM8331618 1370821
Relations
BioProject PRJNA1124516

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE269968_raw_gene_counts.tsv.gz 483.9 Kb (ftp)(http) TSV
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Raw data are available in SRA

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