Your search keyword '"Péterfia, Bálint"' showing total 11 results

1. A recurrent NTRK1 tyrosine kinase domain mutation pair is characteristic in a subset of dedifferentiated liposarcomas.

Author

Lippai, Zoltán, Péterfia, Bálint, Papp, Gergő, Dezső, Katalin, Bedics, Gábor, Pápai, Zsuzsanna, Lamers, Meindert H., Kuin, Rosan CM, Szuhai, Károly, and Sápi, Zoltán

Subjects

*IN vitro studies, *CELLULAR signal transduction, *TUMOR markers, *LIPOSARCOMA, *GENE expression, *IMMUNOHISTOCHEMISTRY, *FIBROBLASTS, *CELL lines, *PROTEIN-tyrosine kinases, *GENETIC mutation

Abstract

Dedifferentiated liposarcoma (DDLPS) is a common form of liposarcoma with challenging treatment modalities. Pan-TRK immunopositivity can be often observed without NTRK gene fusion in soft tissue sarcomas with myogenic differentiation. Expression and the role of NTRK in DDLPS are under-studied. We sought to identify activating mutations of the NTRK genes. 131 DDLPS patients were selected for pan-TRK immunohistochemistry and positive cases were analyzed by Sanger sequencing for NTRK1, NTRK2 and NTRK3 genes. Functional assays were performed using a lentiviral transduction system to study the effect of NTRK variants in fibroblast, immortalized fibroblast, and dedifferentiated liposarcoma cell lines. Out of the 131 DDLPS cases, 75 immunohistochemical staining positive cases, 46 were successfully Sanger sequenced. A recurrent somatic mutation pair in cis position (NGS) of the NTRK1 c.1810C>T (p.H604Y) and c.1838G>T (p.G613V) was identified in six cases (13%) that have never been reported in DDLPS. NTRK fusions were excluded in all six cases by FISH and NGS. The phospho-AKT immunopositivity among the six mutated cases suggested downstream activation of the NTRK signaling pathway. Functional assays showed no transforming effects, but resistance to first- and second-line TRK inhibitors of the p.G613V and p.H604Y variant. We detected (de novo/somatic) missense mutation variants in cis position of the NTRK1 gene in a subset of DDLPS indicating modifying mutations that may contribute to tumorigenesis in a subset of DDLPS. These variants beget resistance to TRK inhibitors indicating an interesting biomarker for other studies with TRK inhibitors. • A subset of dedifferentiated liposarcomas harbour an NTRK1 mutation pair • NTRK1 p.H604Y and p.G613V are somatic mutations, in cis position • Activated downstream pathway can be observed in the double mutant cases • In vitro cell line model did not show transformative potential of the mutations • The mutation pair begets resistance to first- and second-line TRK inhibitors in vitro [ABSTRACT FROM AUTHOR]

Published

2024

2. Syndecan-1 Enhances Proliferation, Migration and Metastasis of HT-1080 Cells in Cooperation with Syndecan-2.

Author

Péterfia, Bálint, Füle, Tibor, Baghy, Kornélia, Szabadkai, Krisztina, Fullár, Alexandra, Dobos, Katalin, Fang Zong, Dobra, Katalin, Hollósi, Péter, Jeney, András, Paku, Sándor, and Kovalszky, Ilona

Subjects

*SYNDECANS, *HEPARAN sulfate proteoglycans, *FIBROSARCOMA, *CANCER cells, *METASTASIS, *CELL proliferation, *GENE expression, *CELL migration

Abstract

Syndecans are transmembrane heparan sulphate proteoglycans. Their role in the development of the malignant phenotype is ambiguous and depends upon the particular type of cancer. Nevertheless, syndecans are promising targets in cancer therapy, and it is important to elucidate the mechanisms controlling their various cellular effects. According to earlier studies, both syndecan-1 and syndecan-2 promote malignancy of HT-1080 human fibrosarcoma cells, by increasing the proliferation rate and the metastatic potential and migratory ability, respectively. To better understand their tumour promoter role in this cell line, syndecan expression levels were modulated in HT-1080 cells and the growth rate, chemotaxis and invasion capacity were studied. For in vivo testing, syndecan-1 overexpressing cells were also inoculated into mice. Overexpression of full length or truncated syndecan-1 lacking the entire ectodomain but containing the four juxtamembrane amino acids promoted proliferation and chemotaxis. These effects were accompanied by a marked increase in syndecan-2 protein expression. The pro-migratory and pro-proliferative effects of truncated syndecan-1 were not observable when syndecan-2 was silenced. Antisense silencing of syndecan-2, but not that of syndecan-1, inhibited cell migration. In vivo, both full length and truncated syndecan-1 increased tumour growth and metastatic rate. Based on our in vitro results, we conclude that the tumour promoter role of syndecan-1 observed in HT-1080 cells is independent of its ectodomain; however, in vivo the presence of the ectodomain further increases tumour proliferation. The enhanced migratory ability induced by syndecan-1 overexpression is mediated by syndecan-2. Overexpression of syndecan-1 also leads to activation of IGF1R and increased expression of Ets-1. These changes were not evident when syndecan-2 was overexpressed. These findings suggest the involvement of IGF1R and Ets-1 in the induction of syndecan-2 synthesis and stimulation of proliferation by syndecan-1. This is the first report demonstrating that syndecan-1 enhances malignancy of a mesenchymal tumour cell line, via induction of syndecan-2 expression. [ABSTRACT FROM AUTHOR]

Published

2012

3. Gene promoter and exon DNA methylation changes in colon cancer development - mRNA expression and tumor mutation alterations.

Author

Molnár, Béla, Galamb, Orsolya, Péterfia, Bálint, Wichmann, Barnabás, Csabai, István, Bodor, András, Kalmár, Alexandra, Szigeti, Krisztina Andrea, Barták, Barbara Kinga, Nagy, Zsófia Brigitta, Valcz, Gábor, Patai, Árpád V., Igaz, Péter, and Tulassay, Zsolt

Subjects

*GENETICS of colon cancer, *PROMOTERS (Genetics), *DNA methylation, *MESSENGER RNA, *GENETIC mutation

Abstract

Background: DNA mutations occur randomly and sporadically in growth-related genes, mostly on cytosines. Demethylation of cytosines may lead to genetic instability through spontaneous deamination. Aims were whole genome methylation and targeted mutation analysis of colorectal cancer (CRC)-related genes and mRNA expression analysis of TP53 pathway genes.Methods: Long interspersed nuclear element-1 (LINE-1) BS-PCR followed by pyrosequencing was performed for the estimation of global DNA metlyation levels along the colorectal normal-adenoma-carcinoma sequence. Methyl capture sequencing was done on 6 normal adjacent (NAT), 15 adenomatous (AD) and 9 CRC tissues. Overall quantitative methylation analysis, selection of top hyper/hypomethylated genes, methylation analysis on mutation regions and TP53 pathway gene promoters were performed. Mutations of 12 CRC-related genes (APC, BRAF, CTNNB1, EGFR, FBXW7, KRAS, NRAS, MSH6, PIK3CA, SMAD2, SMAD4, TP53) were evaluated. mRNA expression of TP53 pathway genes was also analyzed.Results: According to the LINE-1 methylation results, overall hypomethylation was observed along the normal-adenoma-carcinoma sequence. Within top50 differential methylated regions (DMRs), in AD-N comparison TP73, NGFR, PDGFRA genes were hypermethylated, FMN1, SLC16A7 genes were hypomethylated. In CRC-N comparison DKK2, SDC2, SOX1 genes showed hypermethylation, while ERBB4, CREB5, CNTN1 genes were hypomethylated. In certain mutation hot spot regions significant DNA methylation alterations were detected. The TP53 gene body was addressed by hypermethylation in adenomas. APC, TP53 and KRAS mutations were found in 30, 15, 21% of adenomas, and in 29, 53, 29% of CRCs, respectively. mRNA expression changes were observed in several TP53 pathway genes showing promoter methylation alterations.Conclusions: DNA methylation with consecutive phenotypic effect can be observed in a high number of promoter and gene body regions through CRC development. [ABSTRACT FROM AUTHOR]

Published

2018

4. Colorectal adenoma and cancer detection based on altered methylation pattern of SFRP1, SFRP2, SDC2 , and PRIMA1 in plasma samples.

Author

Barták, Barbara Kinga, Kalmár, Alexandra, Péterfia, Bálint, Patai, Árpád V., Galamb, Orsolya, Valcz, Gábor, Spisák, Sándor, Wichmann, Barnabás, Nagy, Zsófia Brigitta, Tóth, Kinga, Tulassay, Zsolt, Igaz, Péter, and Molnár, Béla

Published

2017

5. Aberrant DNA methylation of WNT pathway genes in the development and progression of CIMP-negative colorectal cancer.

Author

Galamb, Orsolya, Kalmár, Alexandra, Péterfia, Bálint, Csabai, István, Bodor, András, Ribli, Dezső, Krenács, Tibor, Patai, Árpád V., Wichmann, Barnabás, Barták, Barbara Kinga, Tóth, Kinga, Valcz, Gábor, Spisák, Sándor, Tulassay, Zsolt, and Molnár, Béla

Published

2016

6. Occurrence of Ordered and Disordered Structural Elements in Postsynaptic Proteins Supports Optimization for Interaction Diversity.

Author

Kiss-Tóth, Annamária, Dobson, Laszlo, Péterfia, Bálint, Ángyán, Annamária F., Ligeti, Balázs, Lukács, Gergely, and Gáspári, Zoltán

Subjects

*AMINO acid sequence, *STRUCTURAL bioinformatics, *PROTEIN-protein interactions, *PROTEINS

Abstract

The human postsynaptic density is an elaborate network comprising thousands of proteins, playing a vital role in the molecular events of learning and the formation of memory. Despite our growing knowledge of specific proteins and their interactions, atomic-level details of their full three-dimensional structure and their rearrangements are mostly elusive. Advancements in structural bioinformatics enabled us to depict the characteristic features of proteins involved in different processes aiding neurotransmission. We show that postsynaptic protein-protein interactions are mediated through the delicate balance of intrinsically disordered regions and folded domains, and this duality is also imprinted in the amino acid sequence. We introduce Diversity of Potential Interactions (DPI), a structure and regulation based descriptor to assess the diversity of interactions. Our approach reveals that the postsynaptic proteome has its own characteristic features and these properties reliably discriminate them from other proteins of the human proteome. Our results suggest that postsynaptic proteins are especially susceptible to forming diverse interactions with each other, which might be key in the reorganization of the postsynaptic density (PSD) in molecular processes related to learning and memory. [ABSTRACT FROM AUTHOR]

Published

2019

7. Comprehensive DNA Methylation Analysis Reveals a Common Ten-Gene Methylation Signature in Colorectal Adenomas and Carcinomas.

Author

Patai, Árpád V., Valcz, Gábor, Hollósi, Péter, Kalmár, Alexandra, Péterfia, Bálint, Patai, Árpád, Wichmann, Barnabás, Spisák, Sándor, Barták, Barbara Kinga, Leiszter, Katalin, Tóth, Kinga, Sipos, Ferenc, Kovalszky, Ilona, Péter, Zoltán, Miheller, Pál, Tulassay, Zsolt, and Molnár, Béla

Subjects

*COLON cancer diagnosis, *GENETICS of colon cancer, *BIOPSY, *DNA methylation, *MICROARRAY technology, *GENETIC mutation

Abstract

Microarray analysis of promoter hypermethylation provides insight into the role and extent of DNA methylation in the development of colorectal cancer (CRC) and may be co-monitored with the appearance of driver mutations. Colonic biopsy samples were obtained endoscopically from 10 normal, 23 adenoma (17 low-grade (LGD) and 6 high-grade dysplasia (HGD)), and 8 ulcerative colitis (UC) patients (4 active and 4 inactive). CRC samples were obtained from 24 patients (17 primary, 7 metastatic (MCRC)), 7 of them with synchronous LGD. Field effects were analyzed in tissues 1 cm (n = 5) and 10 cm (n = 5) from the margin of CRC. Tissue materials were studied for DNA methylation status using a 96 gene panel and for KRAS and BRAF mutations. Expression levels were assayed using whole genomic mRNA arrays. SFRP1 was further examined by immunohistochemistry. HT29 cells were treated with 5-aza-2’ deoxycytidine to analyze the reversal possibility of DNA methylation. More than 85% of tumor samples showed hypermethylation in 10 genes (SFRP1, SST, BNC1, MAL, SLIT2, SFRP2, SLIT3, ALDH1A3, TMEFF2, WIF1), whereas the frequency of examined mutations were below 25%. These genes distinguished precancerous and cancerous lesions from inflamed and healthy tissue. The mRNA alterations that might be caused by systematic methylation could be partly reversed by demethylation treatment. Systematic changes in methylation patterns were observed early in CRC carcinogenesis, occuring in precursor lesions and CRC. Thus we conclude that DNA hypermethylation is an early and systematic event in colorectal carcinogenesis, and it could be potentially reversed by systematic demethylation therapy, but it would need more in vitro and in vivo experiments to support this theory. [ABSTRACT FROM AUTHOR]

Published

2015

8. Myofibroblast-Derived SFRP1 as Potential Inhibitor of Colorectal Carcinoma Field Effect.

Author

Valcz, Gábor, Patai, Árpád V., Kalmár, Alexandra, Péterfia, Bálint, Fűri, István, Wichmann, Barnabás, Műzes, Györgyi, Sipos, Ferenc, Krenács, Tibor, Mihály, Emese, Spisák, Sándor, Molnár, Béla, and Tulassay, Zsolt

Subjects

*MYOFIBROBLASTS, *COLON cancer prevention, *EPIGENETICS, *EPITHELIAL cells, *CELL communication, *GENE expression

Abstract

Epigenetic changes of stromal-epithelial interactions are of key importance in the regulation of colorectal carcinoma (CRC) cells and morphologically normal, but genetically and epigenetically altered epithelium in normal adjacent tumor (NAT) areas. Here we demonstrated retained protein expression of well-known Wnt inhibitor, secreted frizzled-related protein 1 (SFRP1) in stromal myofibroblasts and decreasing epithelial expression from NAT tissues towards the tumor. SFRP1 was unmethylated in laser microdissected myofibroblasts and partially hypermethylated in epithelial cells in these areas. In contrast, we found epigenetically silenced myofibroblast-derived SFRP1 in CRC stroma. Our results suggest that the myofibroblast-derived SFRP1 protein might be a paracrine inhibitor of epithelial proliferation in NAT areas and loss of this signal may support tumor proliferation in CRC. [ABSTRACT FROM AUTHOR]

Published

2014

9. Lack of Matrilin-2 Favors Liver Tumor Development via Erk1/2 and GSK-3β Pathways In Vivo.

Author

Fullár, Alexandra, Baghy, Kornélia, Deák, Ferenc, Péterfia, Bálint, Zsák, Yvonne, Tátrai, Péter, Schaff, Zsuzsa, Dudás, József, Kiss, Ibolya, and Kovalszky, Ilona

Subjects

*LIVER regeneration, *MATRILINS, *EXTRACELLULAR matrix, *ADAPTOR proteins, *RETINOBLASTOMA protein, *GASTROINTESTINAL tumors

Abstract

Matrilin-2 (Matn2) is a multidomain adaptor protein which plays a role in the assembly of extracellular matrix (ECM). It is produced by oval cells during stem cell-driven liver regeneration. In our study, the impact of Matn2 on hepatocarcinogenesis was investigated in Matn2-/- mice comparing them with wild-type (WT) mice in a diethylnitrosamine (DEN) model. The liver tissue was analyzed macroscopically, histologically and immunohistochemically, at protein level by Proteome Profiler Arrays and Western blot analysis. Matn2-/- mice exhibited higher susceptibility to hepatocarcinogenesis compared to wild-type mice. In the liver of Matn2-/- mice, spontaneous microscopic tumor foci were detected without DEN treatment. After 15 μg/g body weight DEN treatment, the liver of Matn2-/- mice contained macroscopic tumors of both larger number and size than the WT liver. In contrast with the WT liver, spontaneous phosphorylation of EGFR, Erk1/2 GSK-3α/β and retinoblastoma protein (p-Rb), decrease in p21/CIP1 level, and increase in β-Catenin protein expression were detected in Matn2-/- livers. Focal Ki-67 positivity of these samples provided additional support to our presumption that the lack of Matn2 drives the liver into a pro-proliferatory state, making it prone to tumor development. This enhanced proliferative capacity was further increased in the tumor nodules of DEN-treated Matn2-/- livers. Our study suggests that Matn2 functions as a tumor suppressor in hepatocarcinogenesis, and in this process activation of EGFR together with that of Erk1/2, as well as inactivation of GSK-3β, play strategic roles. [ABSTRACT FROM AUTHOR]

Published

2014

10. Initial Genomics of the Human Nucleolus.

Author

Németh, Attila, Conesa, Ana, Santoyo-Lopez, Javier, Medina, Ignacio, Montaner, David, Péterfia, Bálint, Solovei, Irina, Cremer, Thomas, Dopazo, Joaquin, and Längst, Gernot

Subjects

*GENETIC research, *GENOMICS, *NUCLEOLUS, *EUKARYOTIC cells, *CHROMATIN, *BIOINFORMATICS

Abstract

We report for the first time the genomics of a nuclear compartment of the eukaryotic cell. 454 sequencing and microarray analysis revealed the pattern of nucleolus-associated chromatin domains (NADs) in the linear human genome and identified different gene families and certain satellite repeats as the major building blocks of NADs, which constitute about 4% of the genome. Bioinformatic evaluation showed that NAD-localized genes take part in specific biological processes, like the response to other organisms, odor perception, and tissue development. 3D FISH and immunofluorescence experiments illustrated the spatial distribution of NAD-specific chromatin within interphase nuclei and its alteration upon transcriptional changes. Altogether, our findings describe the nature of DNA sequences associated with the human nucleolus and provide insights into the function of the nucleolus in genome organization and establishment of nuclear architecture. [ABSTRACT FROM AUTHOR]

Published

2010

11. Syndecan-1 Promotes Hepatocyte-Like Differentiation of Hepatoma Cells Targeting Ets-1 and AP-1.

Author

Hollósi, Péter, Váncza, Lóránd, Karászi, Katalin, Dobos, Katalin, Péterfia, Bálint, Tátrai, Enikő, Tátrai, Péter, Szarvas, Tibor, Paku, Sándor, Szilák, László, and Kovalszky, Ilona

Subjects

*CELL differentiation, *HEPARAN sulfate, *CELL membranes, *REPORTER genes, *HEPATOCELLULAR carcinoma

Abstract

Syndecan-1 is a transmembrane heparan sulfate proteoglycan which is indispensable in the structural and functional integrity of epithelia. Normal hepatocytes display strong cell surface expression of syndecan-1; however, upon malignant transformation, they may lose it from their cell surfaces. In this study, we demonstrate that re-expression of full-length or ectodomain-deleted syndecan-1 in hepatocellular carcinoma cells downregulates phosphorylation of ERK1/2 and p38, with the truncated form exerting an even stronger effect than the full-length protein. Furthermore, overexpression of syndecan-1 in hepatoma cells is associated with a shift of heparan sulfate structure toward a highly sulfated type specific for normal liver. As a result, cell proliferation and proteolytic shedding of syndecan-1 from the cell surface are restrained, which facilitates redifferentiation of hepatoma cells to a more hepatocyte-like phenotype. Our results highlight the importance of syndecan-1 in the formation and maintenance of differentiated epithelial characteristics in hepatocytes partly via the HGF/ERK/Ets-1 signal transduction pathway. Downregulation of Ets-1 expression alone, however, was not sufficient to replicate the phenotype of syndecan-1 overexpressing cells, indicating the need for additional molecular mechanisms. Accordingly, a reporter gene assay revealed the inhibition of Ets-1 as well as AP-1 transcription factor-induced promoter activation, presumably an effect of the heparan sulfate switch. [ABSTRACT FROM AUTHOR]

Published

2020