Construction of a prognostic signature for serous ovarian cancer based on lactate metabolism-related genes

Xiang, Jianbin; Su, Rongjia; Wu, Sufang; Zhou, Lina

doi:10.3389/fonc.2022.967342

Cited by 6 publications

(8 citation statements)

References 46 publications

(50 reference statements)

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“…For example, a study reporting extraction of metabolism‐related genes from TCGA database identified a prognostic signature comprised of PTGIS, AOC3 and IDO1 28 . Meng et al 29 . screened TCGA and GTEx databases for differentially expressed genes in high‐grade serous ovarian cancer and demonstrated that these genes are involved in multiple metabolic pathways.…”

Section: Discussionmentioning

confidence: 99%

Comprehensive profiling of endocrine metabolism identifies a novel signature with robust predictive value in ovarian cancer

Yu,

Luo,

Guo

et al. 2024

The Journal of Gene Medicine

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BackgroundThe cell endocrine pathway is a critical physiological process composed of the endoplasmic reticulum, Golgi apparatus and associated vesicles. Loss of enzymes or proteins can cause dysfunction of endoplasmic reticulum and Golgi apparatus and affect secretion pathways leading to a variety of human diseases, including cancer.MethodsThe single‐cell RNA sequencing and single nucleotide variant principal component analysis data of ovarian cancer were retrieved from The Cancer Genome Atlas and Gene Expression Omnibus (GEO) datasets. Eighty‐four genes from SECRETORY_PATHWAYs were obtained from the gene set enrichment analysis (GSEA) website. Univariate cox regression analyses and ConsensusClusterPlus were used to identify prognostic genes and molecular subtypes, which were validated using the tumor immune dysfunction and exclusion (i.e. TIDE) analysis and gene mutation analysis. A prognosis model was established by randomForestSRC. Abundant infiltrated immune cells and pathway enrichment analyses were carried out, respectively, through ssGSEA, ESTIMATE, MCP‐counter and GSEA. The drug sensitive analysis was performed using pRRophetic package. Immunotherapy datasets and pan‐carcinoma analysis were used to examine the performance of prognostic model.ResultsEighteen prognostic genes from SECRETORY_PATHWAYs were found in both TCGA and GEO datasets. Next, two clusters (C1 and C2) were determined, for which C1 with a poor prognosis had higher immune infiltration. Tumor‐related pathways, such as PATHWAYS_IN_CANCER and B_CELL_RECEPTOR_SIGNALING_PATHWAY, were enriched in C1. Moreover, C2 was suitable for immunotherapy. A four‐gene (DNAJA1, NDRG3, LUZP1 and ZCCHC24) signature was developed and successfully validated. RiskScore of higher levels were significantly associated with worse prognoses. An enhanced immune infiltration, increased pathways score and inappropriate immunotherapy were observed in the high RiskScore group. The high‐ and low‐RiskScore groups had different drug sensitivities. Immunotherapy datasets and pan‐carcinoma analysis indicated that the low RiskScore group may benefit from immunotherapy.ConclusionsBased on the perspective of the secretory signaling pathway, a robust prognostic signature with great performances was determined, which may provide clues for clinical precision treatment of ovarian cancer.

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Section: Discussionmentioning

confidence: 99%

Comprehensive profiling of endocrine metabolism identifies a novel signature with robust predictive value in ovarian cancer

Yu,

Luo,

Guo

et al. 2024

The Journal of Gene Medicine

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“…Several systematic strati cation strategies have been developed to investigate OV metabolic heterogeneity [17,51,15,52,53,14]; however, they rarely consider MIPros. In this study, we not only rede ned and validated the OV subtypes based on the MPIscore in the TCGA-OV and GEO validation sets but also characterized the subtype-speci c clinical features, metabolism, genomic mutations, immune in ltration and regulations between the MPIscore groups, providing a comprehensive understanding of OV metabolism and guidelines for the precision diagnosis and treatment of OV.…”

Section: Discussionmentioning

confidence: 99%

Landscape of Metabolite-Protein Interaction Networks Reveals Prognostic Subtypes of Ovarian Cancer

Chen

Zhu

et al. 2023

Preprint

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Background Metabolic reprogramming, a hallmark of cancer, can promote tumorigenesis and tumour progression through metabolite-protein interactions (MPIs). However, MPI functions and related genes in ovarian cancer (OV) development and treatment remain largely unknown. Methods A TCGA-based metabolic heterogeneity analysis of pancancer was used to identify OV-specific metabolic altered genes (MIPros) and classify OV by MPIScore. MPIscores were based on hub genes intersecting the WGCNA module genes and DEGs of the PCA subtype and LASSO Cox regression analysis. A correlation analysis of the MPIscore, clinical features, functional and genomic characteristics, and the immune landscape was performed. The Gene Expression Omnibus (GEO) database was used for validation. Result In total, 323 OV-specific MIPros were identified by pancancer analysis and used for PCA. Two subtypes with different survival times, ages, and HRD scores were recognized. Five hub prognosis-related genes were included in the MPIscore, an independent prognostic factor (HR = 4.029, P = 0.0118) of patient survival, and possessed distinct metabolism-related pathways and clinical features. Genomic mutations were distributed diversely among MPIscore subgroups; comutations among frequently mutated were detected. Tumour microenvironment analyses correlated a high MPIscore with greater immune infiltration and TIDE scores, leading to poor responses to immunotherapy. Subtyping was consistent across multiple OV cohorts. Conclusion A new OV typing method was developed using specific MIPros, showing differences in metabolism, mutation, immune landscape, and drug response, improving understanding and clinical applications of OV metabolism heterogeneity.

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“…(“Chen signature”), a prognostic model for platinum‐treated OC reported by Sabatier et al 25 . (“Sabatier signature”), a lactate metabolism‐related signature reported by Xiang et al 26 . (“Xiang signature”), a hematogenous and lymphatic metastasis signature reported by Yue et al 27 .…”

Section: Methodsmentioning

confidence: 99%

“…The proportional hazards (PH) assumption was verified with the Schoenfeld test. Additionally, the 3-and 5-year ROC values of the GMPI were compared with those of other published gene signatures for OC, including a prognosisrelated genes signature reported by Chen et al 24 ("Chen signature"), a prognostic model for platinum-treated OC reported by Sabatier et al 25 ("Sabatier signature"), a lactate metabolism-related signature reported by Xiang et al 26 ("Xiang signature"), a hematogenous and lymphatic metastasis signature reported by Yue et al 27 ("Yue signature"), and an omentum metastasis-related prognostic signature reported by Zhang et al 28 ("Zhang signature"). Finally, the precision and accuracy of nomogram was evaluated with ROC curves, the Concordance index (C index) and restricted mean survival (RMS) time curves.…”

Section: Construction and Validation Of A Predictive Nomogrammentioning

confidence: 99%

Glutamine metabolism prognostic index predicts tumour microenvironment characteristics and therapeutic efficacy in ovarian cancer

Gao,

Wei,

Ying

et al. 2024

J Cellular Molecular Medi

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Mounting evidence has highlighted the multifunctional characteristics of glutamine metabolism (GM) in cancer initiation, progression and therapeutic regimens. However, the overall role of GM in the tumour microenvironment (TME), clinical stratification and therapeutic efficacy in patients with ovarian cancer (OC) has not been fully elucidated. Here, three distinct GM clusters were identified and exhibited different prognostic values, biological functions and immune infiltration in TME. Subsequently, glutamine metabolism prognostic index (GMPI) was constructed as a new scoring model to quantify the GM subtypes and was verified as an independent predictor of OC. Patients with low‐GMPI exhibited favourable survival outcomes, lower enrichment of several oncogenic pathways, less immunosuppressive cell infiltration and better immunotherapy responses. Single‐cell sequencing analysis revealed a unique evolutionary trajectory of OC cells from high‐GMPI to low‐GMPI, and OC cells with different GMPI might communicate with distinct cell populations through ligand‐receptor interactions. Critically, the therapeutic efficacy of several drug candidates was validated based on patient‐derived organoids (PDOs). The proposed GMPI could serve as a reliable signature for predicting patient prognosis and contribute to optimising therapeutic strategies for OC.

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Construction of a prognostic signature for serous ovarian cancer based on lactate metabolism-related genes

Cited by 6 publications

References 46 publications

Comprehensive profiling of endocrine metabolism identifies a novel signature with robust predictive value in ovarian cancer

Comprehensive profiling of endocrine metabolism identifies a novel signature with robust predictive value in ovarian cancer

Landscape of Metabolite-Protein Interaction Networks Reveals Prognostic Subtypes of Ovarian Cancer

Glutamine metabolism prognostic index predicts tumour microenvironment characteristics and therapeutic efficacy in ovarian cancer

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