Fibroblast activation protein alpha is expressed by transformed and stromal cells and is associated with mesenchymal features in glioblastoma

Bušek, Petr; Balážiová, Eva; Matrasova, Ivana; Hilser, Marek; Tomáš, Robert; Syrůček, Martin; Zemanová, Zuzana; Kr̆epela, E; Běláček, Jaromír; Šedo, Aleksi

doi:10.1007/s13277-016-5274-9

Cited by 74 publications

(91 citation statements)

References 74 publications

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“…There was a wide intertumoral variability in the expression of both molecules, possibly reflecting their differential expression in individual molecular subtypes of glioblastoma (ref. 12 and our unpublished data) and our unpublished data. FAP immunopositivity was detectable by WB in most of the high-grade glioma samples, but was absent in the DPP-IV negative gliomas.…”

supporting

confidence: 59%

“…Both proteases are involved in the regulation of cell differentiation, adhesion and migration by their proteolytic activity and also non-hydrolytic interactions 9,10 . Our previous reports demonstrated that the expression DPP-IV and FAP is increased in glioblastomas 11,12 . The data on their pathogenetic role in brain tumors is limited-DPP-IV inhibits glioma cell growth, in large part independently of its enzymatic activity 13 , and FAP likely influences the interaction of glioma cells with the surrounding extracellular matrix (our unpublished results and ref.…”

Section: Introductionmentioning

confidence: 92%

“…Brain tissue samples were collected from 51 patients undergoing astrocytic tumor resection, non-tumorous brain specimens were obtained from 15 patients in whom brain surgery was performed for drug-resistant temporal lobe epilepsy 12 . Written informed consent was obtained from the patients before their entry into the study according to the guidelines of institutional Ethics Committee conducted in accordance with the Declaration of Helsinki.…”

Section: Brain Tissue Samplesmentioning

confidence: 99%

“…Interestingly, the isoforms detected in glioblastoma tissues exhibited more alkaline pI compared to the glioma cell lines. Similarly to DPP-IV, these isoforms may originate from the stromal cells expressing FAP in glioblastomas 12 or reflect the differences in FAP isoforms expressed by glioma cells in vitro and in situ.…”

mentioning

confidence: 99%

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Heterogeneity of molecular forms of dipeptidyl peptidase-IV and fibroblast activation protein in human glioblastomas

Matrasova

Bušek

Balážiová

et al. 2017

Biomed Pap Med Fac Univ Palacky Olomouc Czech Repub

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Background and Aims. Proteolytic enzymes contribute to the progression of various cancers. We previously reported increased expression of the proline specific peptidases dipeptidyl peptidase-IV (DPP-IV) and its closest paralogue fibroblast activation protein (FAP) in human glioblastomas. Here we analyze the molecular heterogeneity of DPP-IV and FAP in glioblastomas. Methods. ELISA, isoelectric focusing, 1D and 2D electrophoresis followed by WB or enzyme overlay assay were utilized to analyze DPP-IV and FAP isoforms. Cell fractionation using a Percoll gradient and deglycosylation with PNGase F were performed to analyze the possible basis of DPP-IV and FAP microheterogeneity. Results. Molecular forms of DPP-IV with an estimated molecular weight of 140-160 kDa and a pI predominantly 5.8 were detected in human glioblastoma; in some tumors additional isoforms with a more acidic (3.5-5.5) as well as alkaline (8.1) pI were revealed. Using 2D electrophoresis, two to three molecular forms of FAP with an alkaline (7.0-8.5) pI and an estimated MW of 120-140 kDa were identified in glioblastoma tissues. In glioma cell lines in vitro, several isoforms of both enzymes were expressed, however the alkalic forms present in glioblastoma tissues were not detected. Removal of N-linked oligosaccharides decreased the estimated molecular weight of both enzymes; the overall pattern of molecular forms nevertheless remained unchanged. Conclusion. Several isoforms of DPP-IV and FAP are present in glioblastoma tissue. The absence of alkaline isoforms of both enzymes in glioma cell lines however suggests that isoforms from other, most likely stromal, cell types contribute to the overall pattern seen in glioblastoma tissues.

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supporting

confidence: 59%

Section: Introductionmentioning

confidence: 92%

Section: Brain Tissue Samplesmentioning

confidence: 99%

mentioning

confidence: 99%

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Heterogeneity of molecular forms of dipeptidyl peptidase-IV and fibroblast activation protein in human glioblastomas

Matrasova

Bušek

Balážiová

et al. 2017

Biomed Pap Med Fac Univ Palacky Olomouc Czech Repub

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“…Human cancer FAP expression is reported to correlate to higher tumor grade and worse survival across a worldwide range(11),like cancer on the breast, colon, stomach, etc(12–15). Some studies(15, 16) indicated that FAP can induce EMT.…”

Section: Introductionmentioning

confidence: 99%

FAP overexpression induce Epithelial-Mesenchymal Transition (EMT) in oral squamous cell carcinoma by down-regulating DPP9 gene

Zhao

Huang

et al. 2019

Preprint

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17FAP acts as a tumor promoter via epithelial-mesenchymal transition (EMT) in 18 human oral squamous cell carcinoma (OSCC). The present study was designed to 19 investigate the interaction proteins with FAP and explore the precise mechanism 20 of FAP promoting EMT in OSCC. IP-MS analysis confirmed that DPP9 was an 21 interacting protein of FAP. DPP9 was down-regulated in OSCC tissue samples 22 compared with MNT using immunohistochemistry and quantitative-PCR detection. 23Lower DPP9 was correlated with unfavorable overall survival of patients with OSCC. 24Repressing DPP9 accelerates the proliferation of OSCC cells in vitro and in vivo. 25 Mechanistically, overexpression of FAP downregulate the expression of the DPP9 26 and the effect of FAP on OSCC proliferation, migration, invasion and EMT could be 27 reversed by up-regulated DPP9. Our study suggests that FAP could induce EMT 28 and promote carcinogenesis in oral squamous cell carcinoma by down-regulating 29 DPP9 gene. That will hint different dimension on therapy for patients with OSCC.30 31 Keyword 32 OSCC, FAP, DPP9, EMT, Oral cancer 33 34 Abbreviations 35 FAP: fibroblast activation protein 36 OSCC: Oral squamous cell carcinoma 37 IP: Immunoprecipitation 38 MS: Mass spectrometry 39 qPCR: Quantitative real-time PCR 40 EMT: Epithelial-mesenchymal transition 41 42 43 Introduction 44 Cancer of the oral cavity is one of the most common malignancies and an important 45 cause of morbidity and death(1). OSCC accounts for more than 90% of all oral 46 cancers with the main factors of consumption of tobacco and/or alcohol and chewing 47 areca. In spite of major advances in diagnosis and treatment, the prognosis of OSCC 48 is poor due to invasion, metastasis, and recurrence. Although the oral cavity is easily 49 examined, yet up to 60% of OSCC cases are undiagnosed in the clinical stage. At 50 histopathological level, OSCC is characterized squamous differentiation, nuclear 51 pleomorphisms, invasive growth and metastasis(2). The biomarkers(3) for early 52 diagnosis of OSCC is therefore key to improving patient prognosis and survival rates. 53 FAP is a member of the dipeptidyl peptidase (DPP) family with around 50% homology 54 with DPP4(4). FAP is expressed during development, and in the context of cancer, it is 55 highly expressed and can be a marker of cancer-associated fibroblasts(CAFs), and 56 itself has been demonstrated to have pro-tumorigenic activity(5). Structurally, FAP 57 consists of a 6 amino acid cytoplasmic tail, a single 20 amino acid transmembrane 58 domain, and a 734 amino acid extracellular domain(4) and FAP have both post-59 proline exopeptidase activity and gelatinase activity (6). FAP plays its role in cancer 60 promotion both by enzymatic effects and non-enzymatic effects. Its dual enzymatic 61 activity gives it a range of putative substrates, and many different types of substrates 62 had been reported (7). Although many studies (7) suggested that FAP can enhance 63 various carcinogenesis process, it is still not clear whether that is based on its ...

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Improved prognostication of glioblastoma beyond molecular subtyping by transcriptional profiling of the tumor microenvironment

et al. 2020

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Glioblastoma (GBM), the most aggressive form of brain cancer, is characterized by a high level of molecular heterogeneity, and infiltration by various immune and stromal cell populations. Important advances have been made in deciphering the microenvironment of GBMs, but its association with existing molecular subtypes and its potential prognostic role remain elusive. We have investigated the abundance of infiltrating immune and stromal cells in silico, from gene expression profiles. Two cohorts, including in-house normal brain and glioma samples (n = 70) and a large sample set from TCGA (n = 393), were combined into a single exploratory dataset. A third independent cohort (n = 124) was used for validation. Tumors were clustered based on their microenvironment infiltration profiles, and associations with known GBM molecular subtypes and patient outcome were tested a posteriori in a multivariable setting. We identified a subset of GBM samples with significantly higher abundances of most immune and stromal cell populations. This subset showed increased expression of both immune suppressor and immune effector genes compared to other GBMs and was enriched for the mesenchymal molecular subtype. Survival analyses suggested that tumor microenvironment infiltration pattern was an independent prognostic factor for GBM patients. Among all, patients with the mesenchymal subtype with low immune and stromal infiltration had the poorest survival. By combining molecular subtyping with gene expression measures of tumor infiltration, the present work contributes with improving prognostic models in GBM.

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Fibroblast activation protein alpha is expressed by transformed and stromal cells and is associated with mesenchymal features in glioblastoma

Cited by 74 publications

References 74 publications

Heterogeneity of molecular forms of dipeptidyl peptidase-IV and fibroblast activation protein in human glioblastomas

Heterogeneity of molecular forms of dipeptidyl peptidase-IV and fibroblast activation protein in human glioblastomas

FAP overexpression induce Epithelial-Mesenchymal Transition (EMT) in oral squamous cell carcinoma by down-regulating DPP9 gene

Improved prognostication of glioblastoma beyond molecular subtyping by transcriptional profiling of the tumor microenvironment

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