Analysis of the prognostic, diagnostic and immunological role of HSP90α in malignant tumors

Yuan, Zhimin; Wang, Longhao; Chen, Cheng

doi:10.3389/fonc.2022.963719

Cited by 8 publications

(7 citation statements)

References 63 publications

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“…Our approach provided a significant number of genes related to T cell function in the tumor microenvironment, including HSP90AA1, ETS1, CXCR4, RGS1, and FYN, all detected at the gene level. HSP90AA1, for instance, encodes a heat shock protein, whose overexpression correlates with tumor progression and a poor prognosis in NSCLC [53, 54], and has been shown to correlate with an exhausted phenotype of CD8 T cells in tumors [55]. CXCR4 encodes a chemokine receptor whose expression is associated with the formation of lymphoid follicles that we detected outside of the tumor [56].…”

Section: Resultsmentioning

confidence: 99%

Calibrated Identification of Feature Dependencies in Single-cell Multiomics

Boyeau,

Bates,

Ergen

et al. 2023

Preprint

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Data-driven identification of functional relationships between cellular properties is an exciting promise of single-cell genomics, especially given the increasing prevalence of assays for multiomic and spatial transcriptomic analysis. Major challenges include dealing with technical factors that might introduce or obscure dependencies between measurements, handling complex generative processes that require nonlinear modeling, and correctly assessing the statistical significance of discoveries.VI-VS(Variational Inference for Variable Selection) is a comprehensive framework designed to strike a balance between robustness and interpretability.VI-VSemploys nonlinear generative models to identify conditionally dependent features, all while maintaining control over false discovery rates. These conditional dependencies are more stringent and more likely to represent genuine causal relationships.VI-VSis openly available athttps://github.com/YosefLab/VIVS, offering a no-compromise solution for identifying relevant feature relationships in multiomic data, advancing our understanding of molecular biology.

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Section: Resultsmentioning

confidence: 99%

Calibrated Identification of Feature Dependencies in Single-cell Multiomics

Boyeau,

Bates,

Ergen

et al. 2023

Preprint

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“…Overexpression of HSP90 is strongly associated with various cancers; for example, in breast cancer, the expression level of HSP90 is closely related to the survival of patients, and the abnormally high expression level of HSP90 reflects the poor treatment effect [16][17][18]. HSP90 is a promising marker for the diagnosis and prognosis of malignant tumors [14,19]. In glioblastoma, the expression of HSP90α was abnormally high [20,21].…”

Section: Discussionmentioning

confidence: 99%

Network Pharmacology and Bioinformatics Analysis to Identify the Molecular Targets and its Biological Mechanisms of Sciadopitysin against Glioblastoma

Lian,

Xiong,

Zhao

et al. 2024

J. Cancer

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Glioblastoma multiform (GBM) is categorized as the most malignant subtype of gliomas, which comprise nearly 75% of malignant brain tumors in adults. Increasing evidence suggests that network pharmacology will be a novel method for identifying the systemic mechanism of therapeutic compounds in diseases like cancer. The present study aimed to use a network pharmacology approach to establish the predictive targets of sciadopitysin against GBM and elucidate its biological mechanisms. Firstly, targets of sciadopitysin were obtained from the SwissTargetPrediction database, and genes associated with the pathogenesis of GBM were identified from the DiGeNET database. Sixty-four correlative hits were identified as anti-glioblastoma targets of sciadopitysin. Functional enrichment and pathway analysis revealed significant biological mechanisms of the targets. Interaction of protein network and cluster analysis using STRING resulted in two crucial interacting hub genes, namely, HSP90 and AKT1. Additionally, the in vitro cytotoxic potential of sciadopitysin was assessed on GBM U87 cells. The findings indicate that the pharmacological action of sciadopitysin against GBM might be associated with the regulation of two core targets: HSP90 and AKT1. Thus, the network pharmacology undertaken in the current study established the core active targets of sciadopitysin, which may be extensively applied with further validations for treatment in GBM.

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“…Among the 6 signature genes, CRLF2 as part of an immune score-related risk signature, performed well in the prognostic stratification of OSCC patients and could effectively distinguish their survival status [ 44 ]. HSP90AA1 was highly expressed in various tumors and significantly correlated with poor prognosis [ 45 ]. HSP90AA1/IL-17 signaling pathway was associated with cisplatin resistance in head and neck squamous carcinoma [ 46 ].…”

Section: Discussionmentioning

confidence: 99%

A comprehensive prognostic score for head and neck squamous cancer driver genes and phenotype traits

Zeng,

Xie,

Pan

et al. 2023

Discov Onc

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Background Head and neck squamous cancer (HNSCC) presents variable phenotype and progression features. Clinically applicable, high-accuracy multifactorial prognostic models for HNSCC survival outcomes are warranted and an active area of research. This study aimed to construct a comprehensive prognostic tool for HNSCC overall survival by integrating cancer driver genes with tumor clinical and phenotype information. Methods Key overall survival-related cancer driver genes were screened from among main effector and reciprocal gene pairs using TCGA data using univariate Cox proportional hazard regression analysis. Independent validation was performed using the GSE41613 dataset. The main effector genes among these were selected using LASSO regression and transcriptome score modeling was performed using multivariate Cox regression followed by validation analysis of the prognostic score. Next, multivariate Cox regression analysis was performed using the transcriptome score combined with age, grade, gender, and stage. An ‘Accurate Prediction Model of HNSCC Overall Survival Score’ (APMHO) was computed and validated. Enriched functional pathways, gene mutational landscape, immune cell infiltration, and immunotherapy sensitivity markers associated with high and low APMHO scores were analyzed. Results Screening 107 overall survival-related cancer genes and 402 interacting gene pairs, 6 genes: CRLF2, HSP90AA1, MAP2K1, PAFAH1B2, MYCL and SET genes, were identified and a transcriptional score was obtained. Age, stage and transcriptional score were found to be significant predictors in Cox regression analysis and used to construct a final APMHO model showing an AUC > 0.65 and validated. Transcriptional score, age, pathologic_N, pathologic_T, stage, and TCGA_subtype were significantly different in distribution between high and low APMHO groups. High APMHO samples showed significantly higher mutation rate, enriched tumor-related pathways including Hypoxia, unfold_protein_response, Glycolysis, and mTORC1 signaling, along with differences in immune cell infiltration and immune checkpoint, interferon-γ pathway and m6A regulator expression patterns. Conclusion The APMHO score combining transcriptional and clinical variables showed good prognostic ability for HNSCC overall survival outcomes and was associated with different patterns of phenotypical features, immune and mutational landscape, and immunotherapy sensitivity marker expression. Future studies should validate this score in independent clinical cohorts.

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Analysis of the prognostic, diagnostic and immunological role of HSP90α in malignant tumors

Cited by 8 publications

References 63 publications

Calibrated Identification of Feature Dependencies in Single-cell Multiomics

Calibrated Identification of Feature Dependencies in Single-cell Multiomics

Network Pharmacology and Bioinformatics Analysis to Identify the Molecular Targets and its Biological Mechanisms of Sciadopitysin against Glioblastoma

A comprehensive prognostic score for head and neck squamous cancer driver genes and phenotype traits

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