An Endothelial Gene Signature Score Predicts Poor Outcome in Patients with Endocrine-Treated, Low Genomic Grade Breast Tumors

Tobin, Nicholas P.; Wennmalm, Kristian; Lindström, Linda S.; Foukakis, Theodoros; He, Liqun; Genové, Guillem; Östman, Arne; Landberg, Göran; Betsholtz, Christer; Bergh, Jonas

doi:10.1158/1078-0432.ccr-15-1691

Cited by 8 publications

(11 citation statements)

References 45 publications

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“…We generated an MV score by summarizing the standardized mRNA expression levels for the vascular enriched genes as described. 24 By dichotomizing patients into 2 groups of equal size according to their MV scores, we found that a high MV score was significantly associated with shorter survival ( P = 0.0265, log-rank test) ( Fig. 2A , Supplementary Tables S7 and S8 ).…”

Section: Resultsmentioning

confidence: 90%

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IDH mutation status is associated with distinct vascular gene expression signatures in lower-grade gliomas

Zhang

Lugano

et al. 2018

Neuro-Oncology

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BackgroundVascular gene expression patterns in lower-grade gliomas (LGGs; diffuse World Health Organization [WHO] grades II–III gliomas) have not been thoroughly investigated. The aim of this study was to molecularly characterize LGG vessels and determine if tumor isocitrate dehydrogenase (IDH) mutation status affects vascular phenotype.MethodsGene expression was analyzed using an in-house dataset derived from microdissected vessels and total tumor samples from human glioma in combination with expression data from 289 LGG samples available in the database of The Cancer Genome Atlas. Vascular protein expression was examined by immunohistochemistry in human brain tumor tissue microarrays (TMAs) representing WHO grades II–IV gliomas and nonmalignant brain samples. Regulation of gene expression was examined in primary endothelial cells in vitro.ResultsGene expression analysis of WHO grade II glioma indicated an intermediate stage of vascular abnormality, less severe than that of glioblastoma vessels but distinct from normal vessels. Enhanced expression of laminin subunit alpha 4 (LAMA4) and angiopoietin 2 (ANGPT2) in WHO grade II glioma was confirmed by staining of human TMAs. IDH wild-type LGGs displayed a specific angiogenic gene expression signature, including upregulation of ANGPT2 and serpin family H (SERPINH1), connected to enhanced endothelial cell migration and matrix remodeling. Transcription factor analysis indicated increased transforming growth factor beta (TGFβ) and hypoxia signaling in IDH wild-type LGGs. A subset of genes specifically induced in IDH wild-type LGG vessels was upregulated by stimulation of endothelial cells with TGFβ2, vascular endothelial growth factor, or cobalt chloride in vitro.ConclusionIDH wild-type LGG vessels are molecularly distinct from the vasculature of IDH-mutated LGGs. TGFβ and hypoxia-related signaling pathways may be potential targets for anti-angiogenic therapy of IDH wild-type LGG.

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Section: Resultsmentioning

confidence: 90%

“…For each sample, the standardized values of all 456 vascular enriched genes were added to yield a microvasculature (MV) signature score (an MV score), as described. 24 …”

Section: Methodsmentioning

confidence: 99%

IDH mutation status is associated with distinct vascular gene expression signatures in lower-grade gliomas

Zhang

Lugano

et al. 2018

Neuro-Oncology

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“…The study is designed such that 190 breast cancer patients that developed distant metastatic disease (cases) were selected from a consecutive series of individuals, and each closely matched by adjuvant therapy, age, and calendar period at diagnosis with three patients free from metastasis (controls) 28 . The gene signature for vCAFs correlated strongly to an endothelial metagene 27 and a microvasculature signature 29 within the dataset from the case–control study, whereas mCAFs instead were highly associated with a stroma-derived invasion signature 30 and a stroma-related treatment-predictive signature 31 (Fig. 5i ).…”

Section: Resultsmentioning

confidence: 96%

“…Six gene expression signatures were explored for their correlation with the CAF populations. These included endothelial/microvasculature signatures 27 , 29 , stroma-related signatures 27 , 30 , 31 , and a proliferation signature 32 . Gene signature scores were derived as the weighted averages of the expression values of the constituent signature genes, where the weight for each gene is +1 or −1 depending on the direction with the phenotype in the original publication.…”

Section: Methodsmentioning

confidence: 99%

Spatially and functionally distinct subclasses of breast cancer-associated fibroblasts revealed by single cell RNA sequencing

et al. 2018

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Cancer-associated fibroblasts (CAFs) are a major constituent of the tumor microenvironment, although their origin and roles in shaping disease initiation, progression and treatment response remain unclear due to significant heterogeneity. Here, following a negative selection strategy combined with single-cell RNA sequencing of 768 transcriptomes of mesenchymal cells from a genetically engineered mouse model of breast cancer, we define three distinct subpopulations of CAFs. Validation at the transcriptional and protein level in several experimental models of cancer and human tumors reveal spatial separation of the CAF subclasses attributable to different origins, including the peri-vascular niche, the mammary fat pad and the transformed epithelium. Gene profiles for each CAF subtype correlate to distinctive functional programs and hold independent prognostic capability in clinical cohorts by association to metastatic disease. In conclusion, the improved resolution of the widely defined CAF population opens the possibility for biomarker-driven development of drugs for precision targeting of CAFs.

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“…In this study, we extended previous work of exploiting gene expression profiling approach for accurate detection of VEGF downstream biological activity, and designed a more stringent analytical protocol to identify and validate a reliable VEGF-dependent gene signature in preclinical tumor models and in human patients. Although the VDGs overlapped with previously developed VEGF-related signatures in general 22 26 , the refined gene list presented here was physiologically relevant on the basis of suitable in vivo models and integration of gene profiling results from two independent microarray platforms. Furthermore, we presented a detailed analysis of the VDGs in ovarian cancer by systematically interrogating TCGA HGS-OvCa expression data and four additional genome-wide transcriptome cohorts in the public domain.…”

Section: Discussionmentioning

confidence: 97%

A VEGF-dependent gene signature enriched in mesenchymal ovarian cancer predicts patient prognosis

Yin

Wang

Shen

et al. 2016

Sci Rep

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We have previously reported surrogate biomarkers of VEGF pathway activities with the potential to provide predictive information for anti-VEGF therapies. The aim of this study was to systematically evaluate a new VEGF-dependent gene signature (VDGs) in relation to molecular subtypes of ovarian cancer and patient prognosis. Using microarray profiling and cross-species analysis, we identified 140-gene mouse VDGs and corresponding 139-gene human VDGs, which displayed enrichment of vasculature and basement membrane genes. In patients who received bevacizumab therapy and showed partial response, the expressions of VDGs (summarized to yield VDGs scores) were markedly decreased in post-treatment biopsies compared with pre-treatment baselines. In contrast, VDGs scores were not significantly altered following bevacizumab treatment in patients with stable or progressive disease. Analysis of VDGs in ovarian cancer showed that VDGs as a prognostic signature was able to predict patient outcome. Correlation estimation of VDGs scores and molecular features revealed that VDGs was overrepresented in mesenchymal subtype and BRCA mutation carriers. These findings highlighted the prognostic role of VEGF-mediated angiogenesis in ovarian cancer, and proposed a VEGF-dependent gene signature as a molecular basis for developing novel diagnostic strategies to aid patient selection for VEGF-targeted agents.

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An Endothelial Gene Signature Score Predicts Poor Outcome in Patients with Endocrine-Treated, Low Genomic Grade Breast Tumors

Cited by 8 publications

References 45 publications

IDH mutation status is associated with distinct vascular gene expression signatures in lower-grade gliomas

IDH mutation status is associated with distinct vascular gene expression signatures in lower-grade gliomas

Spatially and functionally distinct subclasses of breast cancer-associated fibroblasts revealed by single cell RNA sequencing

A VEGF-dependent gene signature enriched in mesenchymal ovarian cancer predicts patient prognosis

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