Your search keyword '"György Marko-Varga"' showing total 9 results

1. Proteomic Alterations in Follicular Fluid of Human Small Antral Follicles Collected from Polycystic Ovaries—A Pilot Study

Author

Indira Pla, Aniel Sanchez, Susanne Elisabeth Pors, Stine Gry Kristensen, Roger Appelqvist, K. Barbara Sahlin, György Marko-Varga, Claus Yding Andersen, and Johan Malm

Subjects

follicular fluid, small antral follicles, proteomics, PCOS, PCO, Science

Abstract

Polycystic ovaries (PCO) contain antral follicles that arrest growing around 3–11 mm in diameter, perturbing the dominant follicle’s selection and the subsequent ovulatory process. Proteomic alterations of PCO follicular fluid (FF) (i.e., microenvironment in which the oocyte develops until ovulation) have been studied from large follicles in connection with oocyte pickup during ovarian stimulation. The present study aimed to detect proteomic alterations in FF from unstimulated human small antral follicles (hSAF) obtained from PCO. After performing deep-sequencing label-free proteomics on 10 PCO and 10 non-PCO FF samples from unstimulated hSAF (4.6–9.8 mm), 1436 proteins were identified, of which 115 were dysregulated in PCO FF samples. Pathways and processes related to the immune system, inflammation, and oxidative stress appeared to be upregulated in PCO, while extracellular matrix receptors interactions, the collagens-containing extracellular matrix, and the regulation of signaling were downregulated. The secreted proteins SFRP1, THBS4, and C1QC significantly decreased their expression in PCO FF, and this downregulation was suggested to affect future oocyte competence. In conclusion, our study revealed, for the first time, evidence of proteomic alterations occurring in the FF of PCO hSAF that may be related to the dysfunction of follicular growth and subsequent oocyte competence.

Published

2022

2. Short-Term Effect of Induced Alterations in Testosterone Levels on Fasting Plasma Amino Acid Levels in Healthy Young Men

Author

K. Barbara Sahlin, Indira Pla, Jéssica de Siqueira Guedes, Krzysztof Pawłowski, Roger Appelqvist, György Marko-Varga, Gilberto Barbosa Domont, Fábio César Sousa Nogueira, Aleksander Giwercman, Aniel Sanchez, and Johan Malm

Subjects

testosterone, protein breakdown, gluconeogenesis, Science

Abstract

Long term effect of testosterone (T) deficiency impairs metabolism and is associated with muscle degradation and metabolic disease. The association seems to have a bidirectional nature and is not well understood. The present study aims to investigate the early and unidirectional metabolic effect of induced T changes by measuring fasting amino acid (AA) levels in a human model, in which short-term T alterations were induced. We designed a human model of 30 healthy young males with pharmacologically induced T changes, which resulted in three time points for blood collection: (A) baseline, (B) low T (3 weeks post administration of gonadotropin releasing hormone antagonist) and (C) restored T (2 weeks after injection of T undecanoate). The influence of T on AAs was analyzed by spectrophotometry on plasma samples. Levels of 9 out of 23 AAs, of which 7 were essential AAs, were significantly increased at low T and are restored upon T supplementation. Levels of tyrosine and phenylalanine were most strongly associated to T changes. Short-term effect of T changes suggests an increased protein breakdown that is restored upon T supplementation. Fasting AA levels are able to monitor the early metabolic changes induced by the T fluctuations.

Published

2021

3. Identification and Validation of VEGFR2 Kinase as a Target of Voacangine by a Systematic Combination of DARTS and MSI

Author

Yonghyo Kim, Yutaka Sugihara, Tae Young Kim, Sung Min Cho, Jin Young Kim, Ju Yeon Lee, Jong Shin Yoo, Doona Song, Gyoonhee Han, Melinda Rezeli, Charlotte Welinder, Roger Appelqvist, György Marko-Varga, and Ho Jeong Kwon

Subjects

target identification, target validation, label-free method for drugs, anti-angiogenesis, mechanism of action, receptor tyrosine kinases, Microbiology, QR1-502

Abstract

Although natural products are an important source of drugs and drug leads, identification and validation of their target proteins have proven difficult. Here, we report the development of a systematic strategy for target identification and validation employing drug affinity responsive target stability (DARTS) and mass spectrometry imaging (MSI) without modifying or labeling natural compounds. Through a validation step using curcumin, which targets aminopeptidase N (APN), we successfully standardized the systematic strategy. Using label-free voacangine, an antiangiogenic alkaloid molecule as the model natural compound, DARTS analysis revealed vascular endothelial growth factor receptor 2 (VEGFR2) as a target protein. Voacangine inhibits VEGFR2 kinase activity and its downstream signaling by binding to the kinase domain of VEGFR2, as was revealed by docking simulation. Through cell culture assays, voacangine was found to inhibit the growth of glioblastoma cells expressing high levels of VEGFR2. Specific localization of voacangine to tumor compartments in a glioblastoma xenograft mouse was revealed by MSI analysis. The overlap of histological images with the MSI signals for voacangine was intense in the tumor regions and showed colocalization of voacangine and VEGFR2 in the tumor tissues by immunofluorescence analysis of VEGFR2. The strategy employing DARTS and MSI to identify and validate the targets of a natural compound as demonstrated for voacangine in this study is expected to streamline the general approach of drug discovery and validation using other biomolecules including natural products.

Published

2020

4. Organ Specific Copy Number Variations in Visceral Metastases of Human Melanoma

Author

Sarolta Kárpáti, Jeovanis Gil, József Tímár, Viktória Doma, Orsolya Papp, György Marko-Varga, and Laura Vízkeleti

Subjects

distant organ metastasis, DDR deficiency, HGF/MET autocrine activation, immunogenic mimicry, BRAF and NRAS mutant allele frequency, Cancer Research, Lung, business.industry, Melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Locus (genetics), medicine.disease, Article, Lymphatic system, medicine.anatomical_structure, Oncology, Cancer research, Medicine, Ectopic expression, Copy-number variation, business, Autocrine signalling, Gene, RC254-282

Abstract

Simple Summary Malignant melanoma is a highly metastatic disease disseminating to several distant sites. This potential is also of great clinical impact for patient survival and therapeutic success. Knowledge about melanoma genomics is mainly based on lymphatic or skin metastases derived data, whereas data from distant sites is limited. Therefore, an autopsy-based visceral metastasis biobank was established, and an array-based copy number variation (CNV) analysis was performed, focusing primarily on major organs (brain, lung, and liver) and completed partly by proteomic analysis. A unique picture emerged about organ-specific CNV-type distributions or gene alterations, including the frequent loss of DNA damage error genes in brain metastases, the presence of HGF/MET autocrine loop in brain and lung metastases, the traces of immunogenic mimicry exclusive for lung metastases or the correlation of BRAF copy number and mutant allele frequency, especially in lung metastases. All these above phenomena have a great influence on therapy efficacy or resistance. Abstract Malignant melanoma is one of the most aggressive skin cancers with high potential of visceral dissemination. Since the information about melanoma genomics is mainly based on primary tumors and lymphatic or skin metastases, an autopsy-based visceral metastasis biobank was established. We used copy number variation arrays (N = 38 samples) to reveal organ specific alterations. Results were partly completed by proteomic analysis. A significant increase of high-copy number gains was found in an organ-specific manner, whereas copy number losses were predominant in brain metastases, including the loss of numerous DNA damage response genes. Amplification of many immune genes was also observed, several of them are novel in melanoma, suggesting that their ectopic expression is possibly underestimated. This “immunogenic mimicry” was exclusive for lung metastasis. We also provided evidence for the possible autocrine activation of c-MET, especially in brain and lung metastases. Furthermore, frequent loss of 9p21 locus in brain metastases may predict higher metastatic potential to this organ. Finally, a significant correlation was observed between BRAF gene copy number and mutant allele frequency, mainly in lung metastases. All of these events may influence therapy efficacy in an organ specific manner, which knowledge may help in alleviating difficulties caused by resistance.

Published

2021

5. DNA Polymerase Alpha Subunit B Is a Binding Protein for Erlotinib Resistance in Non-Small Cell Lung Cancer

Author

Jin Young Kim, Jong Shin Yoo, Eun Sun Ji, Ho Jeong Kwon, Tae Young Kim, A. Marcell Szász, Ju Yeon Lee, György Marko-Varga, and Balazs Dome

Subjects

0301 basic medicine, Cancer Research, DNA polymerase, Protein subunit, Drug resistance, NSCLC, lcsh:RC254-282, Article, resistance, 03 medical and health sciences, 0302 clinical medicine, Growth factor receptor, medicine, DARTS LC-MS/MS, Kinase activity, Lung cancer, neoplasms, biology, Chemistry, Binding protein, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, respiratory tract diseases, POLA2, 030104 developmental biology, Oncology, Erlotinib, 030220 oncology & carcinogenesis, Cancer research, biology.protein, medicine.drug

Abstract

Simple Summary Non-small-cell lung carcinoma (NSCLC) covers for almost 85% of all lung cancers and a major contributor to the overall cancer death rate. Erlotinib is used to treat NSCLC via inhibition of epithelial growth factor receptor (EGFR) kinase activity. Despite its high efficacy, recurrence can occur in patients who become resistant to the drug. We performed DARTS LC-MS/MS with SWATH of DIA analysis and identified a novel binding protein of Erlotinib that may underlie NSCLC resistance. Our study indicated that Erlotinib binds POLA2 in addition to EGFR. This was confirmed by DARTS and CETSA results. Importantly, POLA2 expression levels in four NSCLC cell lines were positively correlated with anti-proliferative Erlotinib efficacy (Pearson correlation coefficient, R = 0.9886). These results suggest that POLA2 is a novel complementary target protein of Erlotinib, and could clinically provide validity as a surrogate marker for drug resistance in patients with NSCLC. Abstract Erlotinib inhibits epithelial growth factor receptor (EGFR) kinase activity and is used to treat non-small cell lung cancer (NSCLC). Despite its high efficacy, recurrence can occur in patients who become resistant to the drug. To address the underlying mechanism of Erlotinib resistance, we investigated additional mechanisms related to mode-of-drug-action, by multiple protein-binding interactions, besides EGFR by using drug affinity responsive target stability (DARTS) and liquid chromatography-mass spectrometry (LC-MS/MS) methods with non-labeled Erlotinib. DNA polymerase alpha subunit B (POLA2) was identified as a new Erlotinib binding protein that was validated by the DARTS platform, complemented with cellular thermal shift assays. Genetic knock-down of POLA2 promoted the anti-proliferative effect of the drug in the Erlotinib-resistant cell line H1299 with high POLA2 expression, whereas the overexpression of POLA2 restored anti-proliferative effects in the Erlotinib-sensitive cell line HCC827 with low POLA2 expression. Importantly, POLA2 expression levels in four NSCLC cell lines were positively correlated with anti-proliferative Erlotinib efficacy (Pearson correlation coefficient, R = 0.9886). These results suggest that POLA2 is a novel complementary target protein of Erlotinib, and could clinically provide validity as a surrogate marker for drug resistance in patients with NSCLC.

Published

2020

6. Protein Expression in Metastatic Melanoma and the Link to Disease Presentation in a Range of Tumor Phenotypes

Author

Yonghyo, Kim, Jeovanis, Gil, Indira, Pla, Aniel, Sanchez, Lazaro Hiram, Betancourt, Boram, Lee, Roger, Appelqvist, Christian, Ingvar, Lotta, Lundgren, Håkan, Olsson, Bo, Baldetorp, Ho Jeong, Kwon, Henriett, Oskolás, Melinda, Rezeli, Viktoria, Doma, Sarolta, Kárpáti, A Marcell, Szasz, István Balázs, Németh, Johan, Malm, and György, Marko-Varga

Subjects

clinical trials, combinative treatments, clinical proteogenomics, targeted therapy, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, mitochondrial function, Perspective, metastasis signaling pathways, histopathology, braf mutation, immunotherapy, metastatic melanoma, therapeutic opportunities

Abstract

Malignant melanoma is among the most aggressive skin cancers and it has among the highest metastatic potentials. Although surgery to remove the primary tumor is the gold standard treatment, once melanoma progresses and metastasizes to the lymph nodes and distal organs, i.e., metastatic melanoma (MM), the usual outcome is decreased survival. To improve survival rates and life span, advanced treatments have focused on the success of targeted therapies in the MAPK pathway that are based on BRAF (BRAF V600E) and MEK. The majority of patients with tumors that have higher expression of BRAF V600E show poorer prognosis than patients with a lower level of the mutated protein. Based on the molecular basis of melanoma, these findings are supported by distinct tumor phenotypes determined from differences in tumor heterogeneity and protein expression profiles. With these aspects in mind, continued challenges are to: (1) deconvolute the complexity and heterogeneity of MM; (2) identify the signaling pathways involved; and (3) determine protein expression to develop targeted therapies. Here, we provide an overview of the results from protein expression in MM and the link to disease presentation in a variety of tumor phenotypes and how these will overcome the challenges of clinical problems and suggest new promising approaches in metastatic melanoma and cancer therapy.

Published

2020

7. Identification and Validation of VEGFR2 Kinase as a Target of Voacangine by a Systematic Combination of DARTS and MSI

Author

Ho Jeong Kwon, Ju Yeon Lee, Jong Shin Yoo, Jin Young Kim, Charlotte Welinder, Tae Young Kim, Melinda Rezeli, Roger Appelqvist, György Marko-Varga, Yonghyo Kim, Doona Song, Sung Min Cho, Gyoonhee Han, and Yutaka Sugihara

Subjects

Curcumin, label-free method for drugs, natural products, lcsh:QR1-502, Drug Evaluation, Preclinical, CD13 Antigens, Biochemistry, lcsh:Microbiology, Article, Mass Spectrometry, Receptor tyrosine kinase, Mass spectrometry imaging, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, target identification, Human Umbilical Vein Endothelial Cells, biochemistry, Animals, Humans, Tissue Distribution, Kinase activity, Molecular Biology, Voacangine, 030304 developmental biology, Mice, Inbred BALB C, 0303 health sciences, receptor tyrosine kinases, biology, Drug discovery, Kinase insert domain receptor, Vascular Endothelial Growth Factor Receptor-2, Xenograft Model Antitumor Assays, Molecular Docking Simulation, target validation, chemistry, Docking (molecular), Ibogaine, 030220 oncology & carcinogenesis, biology.protein, anti-angiogenesis, Female, Target protein, Cell culture assays, mechanism of action

Abstract

Although natural products are an important source of drugs and drug leads, identification and validation of their target proteins have proven difficult. Here, we report the development of a systematic strategy for target identification and validation employing drug affinity responsive target stability (DARTS) and mass spectrometry imaging (MSI) without modifying or labeling natural compounds. Through a validation step using curcumin, which targets aminopeptidase N (APN), we successfully standardized the systematic strategy. Using label-free voacangine, an antiangiogenic alkaloid molecule as the model natural compound, DARTS analysis revealed vascular endothelial growth factor receptor 2 (VEGFR2) as a target protein. Voacangine inhibits VEGFR2 kinase activity and its downstream signaling by binding to the kinase domain of VEGFR2, as was revealed by docking simulation. Through cell culture assays, voacangine was found to inhibit the growth of glioblastoma cells expressing high levels of VEGFR2. Specific localization of voacangine to tumor compartments in a glioblastoma xenograft mouse was revealed by MSI analysis. The overlap of histological images with the MSI signals for voacangine was intense in the tumor regions and showed colocalization of voacangine and VEGFR2 in the tumor tissues by immunofluorescence analysis of VEGFR2. The strategy employing DARTS and MSI to identify and validate the targets of a natural compound as demonstrated for voacangine in this study is expected to streamline the general approach of drug discovery and validation using other biomolecules including natural products.

Published

2020

8. The Hidden Story of Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma-Association with Clinical Outcome and Tumor Phenotypes

Author

A. Marcell Szász, György Marko-Varga, Melinda Rezeli, Charlotte Welinder, Lotta Lundgren, Elisabet Wieslander, Magdalena Kuras, Indira Pla, Ho Jeong Kwon, Bo Baldetorp, Kenichi Miharada, Zsolt Horvath, Aniel Sanchez, David Fenyö, Roger Appelqvist, Jimmy Rodriguez Murillo, Tasso Miliotis, Christian Ingvar, Johan Malm, Yutaka Sugihara, Håkan Olsson, István Németh, Jonatan Eriksson, Peter Horvatovich, Lázaro Betancourt, Krzysztof Pawłowski, Jeovanis Gil, Göran Jönsson, Analytical Biochemistry, and Medicinal Chemistry and Bioanalysis (MCB)

Subjects

0301 basic medicine, Cancer Research, malignant melanoma, medicine.disease_cause, Proteomics, Article, 03 medical and health sciences, 0302 clinical medicine, proteomics, Mutant protein, medicine, Mutation, business.industry, Melanoma, BRAF V600E mutation, medicine.disease, mass spectrometry genetics, 030104 developmental biology, MRNA Sequencing, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Cancer research, Immunohistochemistry, prognosis, heterogeneity, business, V600E

Abstract

In comparison to other human cancer types, malignant melanoma exhibits the greatest amount of heterogeneity. After DNA-based detection of the BRAF V600E mutation in melanoma patients, targeted inhibitor treatment is the current recommendation. This approach, however, does not take the abundance of the therapeutic target, i.e., the B-raf V600E protein, into consideration. As shown by immunohistochemistry, the protein expression profiles of metastatic melanomas clearly reveal the existence of inter- and intra-tumor variability. Nevertheless, the technique is only semi-quantitative. To quantitate the mutant protein there is a fundamental need for more precise techniques that are aimed at defining the currently non-existent link between the levels of the target protein and subsequent drug efficacy. Using cutting-edge mass spectrometry combined with DNA and mRNA sequencing, the mutated B-raf protein within metastatic tumors was quantitated for the first time. B-raf V600E protein analysis revealed a subjacent layer of heterogeneity for mutation-positive metastatic melanomas. These were characterized into two distinct groups with different tumor morphologies, protein profiles and patient clinical outcomes. This study provides evidence that a higher level of expression in the mutated protein is associated with a more aggressive tumor progression. Our study design, comprised of surgical isolation of tumors, histopathological characterization, tissue biobanking, and protein analysis, may enable the eventual delineation of patient responders/non-responders and subsequent therapy for malignant melanoma.

Published

2019

9. The Hidden Story on Heterogeneous B-raf V600E Mutation Quantitative Protein Expression in Metastatic Melanoma – Association with Clinical Outcome and Tumor Phenotypes

Author

Melinda Rezeli, Jeovanis Gil, Håkan Olsson, Peter Horvatovich, Zsolt Horvath, David Fenyö, Lázaro Betancourt, Johan Malm, Jonatan Eriksson, Indira Pla, Charlotte Welinder, Jimmy Rodriguez Murillo, Roger Appelqvist, Elisabet Wieslander, Yutaka Sugihara, Magdalena Kuras, Tasso Militois, Göran Jönsson, István Németh, Krzysztof Pawłowski, Kenichi Miharada, György Marko-Varga, Lotta Lundgren, Christian Ingvar, Bo Baldetorp, Aniel Sánchez, Ho Jeong Kwon, and A. Marcell Szász

Subjects

Metastatic melanoma, business.industry, Mutation (genetic algorithm), Cancer research, Medicine, business, Proteomics, Phenotype, Protein expression, V600E, oncology_oncogenics

Abstract

In comparison to other human cancer types, malignant melanoma exhibits the greatest amount of heterogeneity. After DNA-based detection of the BRAF V600E mutation in melanoma patients, targeted inhibitor treatment is the current recommendation. This approach, however, does not take the abundance of the therapeutic target, i.e., the B-raf V600E protein, into consideration. As shown by immunohistochemistry, the protein expression profiles of metastatic melanomas do clearly reveal the existence of inter- and intra-tumor variability. Nevertheless, the technique is only semi-quantitative. To quantitate the mutant protein there is a fundamental need for more precise techniques that are aimed at defining the currently non-existent link between the levels of the target protein and subsequent drug efficacy. Using cutting-edge mass spectrometry combined with DNA and mRNA sequencing, the mutated B-raf protein within metastatic tumors was quantitated for the first time. B-raf V600E protein analysis revealed a subjacent layer of heterogeneity for mutation-positive metastatic melanomas. These were characterized into two distinct groups with different tumor morphologies, protein profiles and patient clinical outcomes. This study provides evidence that a higher level of expression for the mutated protein is associated with a more aggressive tumor progression. Our study design that is comprised of surgical isolation of tumors, histopathological characterization, tissue biobanking, and protein analysis may enable the eventual delineation of patient responders/non-responders and the subsequent therapy of malignant melanoma.

Published

2019