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@ARTICLE{Wang:274213,
author = {Z. Wang and T. Wang and G. Wu and L. Zhu$^*$ and J. Zhang},
title = {{C}linical {S}ignificance and {T}umor {M}icroenvironment
{C}haracterization of a {N}ovel {I}mmune-{R}elated {G}ene
{S}ignature in {B}ladder {C}ancer.},
journal = {Journal of Clinical Medicine},
volume = {12},
number = {5},
issn = {2077-0383},
address = {Basel},
publisher = {MDPI},
reportid = {DKFZ-2023-00499},
pages = {1892},
year = {2023},
abstract = {Cancer immunotherapy plays a crucial role in bladder cancer
(BC) progression. Increasing evidence has elucidated the
clinicopathologic significance of the tumor microenvironment
(TME) in predicting outcomes and therapeutic efficacy. This
study sought to establish a comprehensive analysis of the
immune-gene signature combined with TME to assist in BC
prognosis. We selected sixteen immune-related genes (IRGs)
after a weighted gene co-expression network and survival
analysis. Enrichment analysis revealed that these IRGs were
actively involved in Mitophagy and Renin secretion pathways.
After multivariable COX analysis, the IRGPI comprising
NCAM1, CNTN1, PTGIS, ADRB3, and ANLN was established to
predict the overall survival of BC, which was validated in
both TCGA and GSE13507 cohorts. In addition, a TME gene
signature was developed for molecular and prognosis
subtyping with unsupervised clustering, followed by a
panoramic landscape characterization of BC. In summary, the
IRGPI model developed in our study provided a valuable tool
with an improved prognosis for BC.},
keywords = {biomarker (Other) / bladder cancer (Other) / immune-related
genes (Other) / prognosis (Other) / tumor microenvironment
(Other)},
cin = {A430},
ddc = {610},
cid = {I:(DE-He78)A430-20160331},
pnm = {311 - Zellbiologie und Tumorbiologie (POF4-311)},
pid = {G:(DE-HGF)POF4-311},
typ = {PUB:(DE-HGF)16},
pubmed = {pmid:36902678},
doi = {10.3390/jcm12051892},
url = {https://inrepo02.dkfz.de/record/274213},
}