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1.

001-es BibID:	BIBFORM005174
035-os BibID:	(scopus)38349044364 (wos)000253278400023
Első szerző:	Barok Márk (biofizikus)
Cím:	Trastuzumab decreases the number of circulating and disseminated tumor cells despite trastuzumab resistance of the primary tumor / Márk Barok, Margit Balázs, Péter Nagy, Zsuzsa Rákosy, Andrea Treszl, Enikő Tóth, István Juhász, John W. Park, Jorma Isola, György Vereb, János Szöllősi
Dátum:	2008
ISSN:	304-3835 (Print)
Megjegyzések:	We have recently shown that despite of the fact that the ErbB2-positive JIMT-1 human breast cancer cells intrinsically resistant to trastuzumab in vitro, trastuzumab inhibited the outgrowth of early phase JIMT-1 xenografts in SCID mice via antibody-dependent cellular cytotoxicity (ADCC). Here we show that trastuzumab significantly reduces the number of circulating and disseminated tumor cells (CTCs and DTCs) in this xenograft model system at a time when the primary tumor is already unresponsive to trastuzumab. This observation suggests that ErbB2 positive CTCs and DTCs might be sensitive to trastuzumab-mediated ADCC even if when the primary tumor is already non-responsive. Thus, trastuzumab treatment might also be beneficial in the case of patients with breast cancer that is already trastuzumab resistant.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk analysis Animals antagonists and inhibitors Antibodies Antibodies, Monoclonal Antigens Antigens, CD45 Antineoplastic Agents article Biophysics blood Bone Marrow Breast Neoplasms Cell Line, Tumor Cells Chromosomes, Human,X drug effects Drug Resistance, Neoplasm drug therapy EGFR Epidermal Growth Factor ErbB2 Female genetics Histocompatibility Antigens Histocompatibility Antigens Class I Human Humans Hungary Immunohistochemistry immunology In Situ Hybridization,Fluorescence In Vitro metabolism Mice Mice, Scid mouse Neoplasm Circulating Cells Neoplasm Metastasis pathology pharmacology Receptor, Epidermal Growth Factor Research Research Support Support therapeutic use Time Factors Trastuzumab resistance Xenograft Model Antitumor Assays egyetemen (Magyarországon) készült közlemény
Megjelenés:	Cancer Letters. - 260 : 1-2 (2008), p. 198-208. -
További szerzők:	Balázs Margit (1952-) (sejtbiológus, molekuláris genetikus) Nagy Péter (1971-) (biofizikus) Rákosy Zsuzsa (1978-) (sejtbiológus, molekuláris biológus, genetikus) Treszl Andrea (1974-) (molekuláris biológus) Tóth Enikő Juhász István (1956-) (bőrgyógyász, bőrsebész, kozmetológus, klinikai onkológus) Park, John W. Isola, Jorma Vereb György (1965-) (biofizikus, orvos) Szöllősi János (1953-) (biofizikus)
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2.

001-es BibID:	BIBFORM001053
035-os BibID:	(scopus)34447298092 (wos)000248154300017
Első szerző:	Barok Márk (biofizikus)
Cím:	Trastuzumab causes antibody-dependent cellular cytotoxicity-mediated growth inhibition of submacroscopic JIMT-1 breast cancer xenografts despite intrinsic drug resistance / Barok M., Isola J., Pályi-Krekk Zs., Nagy P., Juhász I., Vereb Gy., Kauraniemi P., Kapanen A., Tanner M., Vereb Gy., Szöllősi J.
Dátum:	2007
Megjegyzések:	Trastuzumab is a recombinant antibody drug that is widely used for the treatment of breast cancer. Despite encouraging clinical results, some cancers are primarily resistant to trastuzumab, and a majority of those initially responding become resistant during prolonged treatment. The mechanisms of trastuzumab resistance have not been fully understood. We examined the role of antibody-dependent cellular cytotoxicity (ADCC) using JIMT-1 cells that are ErbB2 positive but intrinsically resistant to trastuzumab in vitro. Unexpectedly, in experiments mimicking adjuvant therapy of submacroscopic disease in vivo (JIMT-1 cells inoculated s.c. in severe combined immunodeficiency mice), trastuzumab was able to inhibit the outgrowth of macroscopically detectable xenograft tumors for up to 5-7 weeks. The effect is likely to be mediated via ADCC because trastuzumab-F(ab')(2) was ineffective in this model. Moreover, in vitro ADCC reaction of human leukocytes was equally strong against breast cancer cells intrinsically sensitive (SKBR-3) or resistant (JIMT-1) to trastuzumab or even against a subline of JIMT-1 that was established from xenograft tumors growing despite trastuzumab treatment. These results suggest that ADCC may be the predominant mechanism of trastuzumab action on submacroscopic tumor spread. Thus, measuring the ADCC activity of patient's leukocytes against the tumor cells may be a relevant predictor of clinical trastuzumab responsiveness in vivo.
Tárgyszavak:	Orvostudományok Természettudományok Elméleti orvostudományok Biológiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk ErbB2 receptor trastuzumab breast cancer antibody therapy
Megjelenés:	Molecular Cancer Therapeutics. - 6 : 7 (2007), p. 2065-2072. -
További szerzők:	Isola, Jorma Pályiné Krekk Zsuzsanna (1974-) (molekuláris biológus) Nagy Péter (1971-) (biofizikus) Juhász István (1956-) (bőrgyógyász, bőrsebész, kozmetológus, klinikai onkológus) Vereb György (1938-) (biokémikus, sejtbiológus) Kauraniemi, Päivikki Kapanen, Anita I. Tanner, Minna Vereb György (1965-) (biofizikus, orvos) Szöllősi János (1953-) (biofizikus)
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3.

001-es BibID:	BIBFORM071657
035-os BibID:	(Cikkazonosító)157 (WOS)000419659600038 (Scopus)85040525540
Első szerző:	Batta Gyula (biológus)
Cím:	Alterations in the properties of the cell membrane due to glycosphingolipid accumulation in a model of Gaucher disease / Gyula Batta, Lilla Soltész, Tamás Kovács, Tamás Bozó, Zoltán Mészár, Miklós Kellermayer, János Szöllősi, Peter Nagy
Dátum:	2018
ISSN:	2045-2322
Megjegyzések:	Gaucher disease is a lysosomal storage disease characterized by the malfunction of glucocerebrosidaseresulting in the accumulation of glucosylceramide and other sphingolipids in certain cells. Althoughthe disease symptoms are usually attributed to the storage of undigested substrate in lysosomes,here we show that glycosphingolipids accumulating in the plasma membrane cause profound changesin the properties of the membrane. The fluidity of the sphingolipid-enriched membrane decreasedaccompanied by the enlargement of raft-like ordered membrane domains. The mobility of non-raftproteins and lipids was severely restricted, while raft-resident components were only mildly affected.The rate of endocytosis of transferrin receptor, a non-raft protein, was significantly retarded in Gauchercells, while the endocytosis of the raft-associated GM1 ganglioside was unaffected. Interferon-?-induced STAT1 phosphorylation was also significantly inhibited in Gaucher cells. Atomic forcemicroscopy revealed that sphingolipid accumulation was associated with a more compliant membranecapable of producing an increased number of nanotubes. The results imply that glycosphingolipidaccumulation in the plasma membrane has significant effects on membrane properties, which may beimportant in the pathogenesis of Gaucher disease.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk
Megjelenés:	Scientific Reports. - 8 : 1 (2018), p. 157. -
További szerzők:	Soltész Lilla (1994-) (orvos) Kovács Tamás (1985-) (általános orvos) Bozó Tamás Mészár Zoltán Mihály (1977-) (agrármérnök) Kellermayer Miklós Szöllősi János (1953-) (biofizikus) Nagy Péter (1971-) (biofizikus)
Pályázati támogatás:	K120302 OTKA K109480 OTKA K124966 OTKA GINOP-2.3.2-15-2016-00020 GINOP GINOP-2.3.2-15-2016-00044 GINOP
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4.

001-es BibID:	BIBFORM077632
035-os BibID:	(cikkazonosító)1062 (scopus)85063627035 (wos)000462542300061
Első szerző:	Costea, Teodora
Cím:	Molecular Mechanisms and Bioavailability of Polyphenols in Prostate Cancer / Teodora Costea, Péter Nagy, Constanța Ganea, János Szöllősi, Maria-Magdalena Mocanu
Dátum:	2019
ISSN:	1661-6596 1422-0067
Megjegyzések:	: Prostate cancer is the one of the most frequently diagnosed cancers among men over the age of 50. Several lines of evidence support the observation that polyphenols have preventive and therapeutic effects in prostate cancer. Moreover, prostate cancer is ideal for chemoprevention due to its long latency. We propose here an equilibrated lifestyle with a diet rich in polyphenols as prophylactic attempts to slow down the progression of localized prostate cancer or prevent the occurrence of the disease. In this review, we will first summarize the molecular mechanisms of polyphenols in prostate cancer with a focus on the antioxidant and pro-oxidant effects, androgen receptors (AR), key molecules involved in AR signaling and their transactivation pathways, cell cycle, apoptosis, angiogenesis, metastasis, genetic aspects, and epigenetic mechanisms. The relevance of the molecular mechanisms is discussed in light of current bioavailability data regarding the activity of polyphenols in prostate cancer. We also highlight strategies for improving the bioavailability of polyphenols. We hope that this review will lead to further research regarding the bioavailability and the role of polyphenols in prostate cancer prevention and treatment.
Tárgyszavak:	Orvostudományok Klinikai orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban dietary polyphenols bioavailability molecular mechanisms prostate cancer
Megjelenés:	International Journal of Molecular Sciences. - 20 : 5 (2019), p. 1-39. -
További szerzők:	Nagy Péter (1971-) (biofizikus) Ganea, Constanta Szöllősi János (1953-) (biofizikus) Mocanu, Maria-Magdalena
Pályázati támogatás:	GINOP-2.3.2-15-2016-00020 GINOP GINOP-2.3.2-15-2016-00044 GINOP GINOP-2.3.3-15-2016-00003 GINOP K120302 Egyéb
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5.

001-es BibID:	BIBFORM004705
035-os BibID:	(scopus)18544371851 (wos)000173421300040
Első szerző:	Dornan, Saffron
Cím:	Differential association of CD45 isoforms with CD4 and CD8 regulates the actions of specific pools of p56lck tyrosine kinase in T cell antigen receptor signal transduction / Dornan, S., Sebestyen, Z., Gamble, J., Nagy, P., Bodnar, A., Alldridge, L., Doe, S., Holmes, N., Goff, L. K., Beverley, P., Szollosi, J., Alexander, D. R.
Dátum:	2002
Megjegyzések:	An investigation into the role of CD45 isoforms in T cell antigen receptor signal transduction was carried out by transfecting CD45-negative CD4(+)CD8(+) HPB-ALL T cells with the CD45R0, CD45RBC, and CD45RABC isoforms. Fluorescence resonance energy transfer analysis showed that the CD45R0 isoform, but not the CD45RBC or CD45RABC isoforms, was found as homodimers and also preferentially associated with CD4 and CD8 at the cell-surface. A comparison was therefore made of T cell antigen receptor signaling between sub-clones expressing either CD45R0 or CD45RBC. Under basal conditions CD4-associated p56(lck) tyrosine kinase activity and cellular protein tyrosine phosphorylation levels were higher in the CD45R0(+) than in the CD45RBC(+) sub-clones. Upon CD3-CD4 ligation, TCR-zeta phosphorylation, ZAP-70 recruitment to the p21/p23 TCR-zeta phosphoisomers, ZAP-70 phosphorylation, as well as p56(lck), c-Cbl and Slp-76 phosphorylation, were all markedly increased in CD45R0(+) compared with CD45RBC(+) cells. T cell antigen receptor (TCR) stimulation alone also promoted c-Cbl phosphorylation in CD45R0(+) but not in CD45RBC(+) cells. Our results are consistent with a model in which association of CD45R0 with CD4 generates a more active pool of CD4-associated p56(lck) kinase molecules. Upon CD3-CD4 co-ligation, the active p56(lck) increases the intensity of T cell antigen receptor signal transduction coupling by promoting TCR-zeta chain phosphorylation and ZAP-70 recruitment.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk analysis Antigens,CD4 Antigens,CD45 Antigens,CD8 Energy Transfer Fluorescence Human immunology Lymphocyte Specific Protein Tyrosine Kinase p56(lck) metabolism Phosphorylation Receptors,Antigen,T-Cell Signal Transduction Support,Non-U.S.Gov't
Megjelenés:	The Journal of Biological Chemistry. - 277 : 3 (2002), p. 1912-1918. -
További szerzők:	Sebestyén Zsolt Gamble, John Nagy Péter (1971-) (biofizikus) Dóczy-Bodnár Andrea (1970-) (biofizikus) Alldridge, Lou Doe, Senam Holmes, Nick Goff, Lindsey K. Beverley, Peter Szöllősi János (1953-) (biofizikus) Alexander, Denis R.
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6.

001-es BibID:	BIBFORM042481
035-os BibID:	(scopus)40049093067 (wos)000253576200006
Első szerző:	Fazekas Zsolt (biofizikus)
Cím:	Two-sided fluorescence resonance energy transfer for assessing molecular interactions of up to three distinct species in confocal microscopy / Zsolt Fazekas, Miklós Petrás, Ákos Fábián, Zsuzsanna Pályi-Krekk, Péter Nagy, Sándor Damjanovich, György Vereb, János Szöllősi
Dátum:	2008
ISSN:	1552-4922 1552-4930
Megjegyzések:	The role of the expression patterns of proteins involved in oncogenesis can be understood after characterizing their multimolecular interactions. Conventional FRET methods permit the analysis of interaction between two molecular species at the most, which necessitates the introduction of new approaches for studying multicomponent signaling complexes. Flow cytometric as well as microscopic donor (dbFRET) and acceptor (abFRET) photobleaching FRET measurements were performed to determine the association states of ErbB2, b1-integrin, and CD44 receptors. Based on consecutively applied abFRET and dbFRET methods (two-sided FRET), the relationship of b1-integrin?ErbB2 heteroassociation to ErbB2 homoassociation and of b1-integrin?ErbB2 heteroassociation to ErbB2?CD44 heteroassociation was studied by correlating pixel-by-pixel FRET values of the corresponding abFRET and dbFRET images in contour plots. Anticorrelation was observed between b1-integrin?ErbB2 heteroassociation and ErbB2 homoassociation on trastuzumab sensitive N87 and SK-BR-3 cells, while modest positive correlation was found between b1-integrin?ErbB2 and ErbB2?CD44 heteroassociationon trastuzumab resistant MKN-7 cells. The FRET efficiency values of b1-integrin?ErbB2 heteroassociation were markedly higher at the focal adhesion regions on attachedcells than those measured by flow cytometry on detached cells. In conclusion, we implemented an experimental set-up termed two-sided FRET for correlating two pairwiseinteractions of three arbitrarily chosen molecular species. On the basis of our results, we assume that the homoassociation state of ErbB2 is dynamically modulated by its interaction with b1-integrins.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk beta1-integrin abFRET analysis Biophysics Carcinoma CD44 Cell Adhesion Cell Adhesion Molecules Cell Line Cells Cholera Toxin Confocal Confocal microscopy cytology dbFRET Energy Transfer ErbB2 Flow Cytometry Fluorescein Fluorescence fluorescence microscopy Fluorescence Resonance Energy Transfer FRET Hiv-1 Human Hungary Image Cytometry Image Processing Kinetics Laser scanning confocal microscopy Luminescence methods Microscopy Photobleaching Protein-protein interactions Proteins Receptor tyrosine kinase Research Signal Transduction Software therapy Trastuzumab resistance tsFRET Tyrosine egyetemen (Magyarországon) készült közlemény
Megjelenés:	Cytometry Part A. - 73 : 3 (2008), p. 209-219. -
További szerzők:	Petrás Miklós (1977-) (orvos) Fábián Ákos István (1982-) (aneszteziológus) Pályiné Krekk Zsuzsanna (1974-) (molekuláris biológus) Nagy Péter (1971-) (biofizikus) Damjanovich Sándor (1936-2017) (biofizikus) Vereb György (1965-) (biofizikus, orvos) Szöllősi János (1953-) (biofizikus)
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7.

001-es BibID:	BIBFORM074167
Első szerző:	Filippi, Alexandru
Cím:	Epigallocatechin-3-gallate alleviates the malignant phenotype in A-431 epidermoid and SK-BR-3 breast cancer cell lines / Filippi Alexandru, Picot Tiphanie, Aanei Carmen Mariana, Nagy Péter, Szöllősi János, Campos Lydia, Ganea Constanţa, Mocanu Maria-Magdalena
Dátum:	2018
ISSN:	0963-7486
Megjegyzések:	In this study, we evaluated the effects of epigallocatechin-3-O-gallate (EGCG) in two cancer cell lines, A-431 overexpressing ErbB1 and SK-BR-3, overexpressing ErbB2. EGCG treatment showed dose-dependent collapse of mitochondrial membrane potential (??m), increase in reactive oxygen species (ROS) production, changes in nuclear morphology and reduced viability. Flow cytometry data indicated that EGCG partially decreases the phosphorylation of several proteins involved in cell proliferation and survival: pErbB1(Y1173, Y1068), pAkt(S473) and pERK(Y204). EGCG affected the clonogenic growth in both cell lines with an EC50 of 2.5 and 5.4??M for A-431 and SK-BR-3, respectively. Wound scratch assay demonstrated that EGCG inhibited the healing in dose-dependent manner and the effect was correlated with partial reduction in phosphorylation of pFAK(S910). Our data suggest that EGCG administration might reduce the unfavourable traits, particularly associated with ErbB1/EGFR overexpression.
Tárgyszavak:	Természettudományok Biológiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
Megjelenés:	International Journal Of Food Sciences And Nutrition. - 69 : 5 (2018), p. 584-597. -
További szerzők:	Picot, Tiphanie Aanei, Carmen Mariana Nagy Péter (1971-) (biofizikus) Szöllősi János (1953-) (biofizikus) Campos, Lydia Ganea, Constanta Mocanu, Maria-Magdalena
Pályázati támogatás:	K120302 OTKA K103906 OTKA GINOP-2.3.2-15-2016-00020 GINOP GINOP-2.3.2-15-2016-00050 GINOP
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8.

001-es BibID:	BIBFORM004864
035-os BibID:	(scopus)26444452209 (wos)000232299300016
Első szerző:	Friedländer Elza (biofizikus)
Cím:	Signal transduction of erbB receptors in trastuzumab (Herceptin) sensitive and resistant cell lines : local stimulation using magnetic microspheres as assessed by quantitative digital microscopy / Friedlander, E., Arndt-Jovin, D. J., Nagy, P., Jovin, T. M., Szollosi, J., Vereb, G.
Dátum:	2005
ISSN:	1552-4922
Megjegyzések:	ErbB2 (HER-2), a member of the epidermal growth factor (EGF) receptor family, is a class I transmembrane receptor tyrosine kinase. Although erbB2 has no known physiologic ligand, it can form complexes with other members of the family and undergo transactivation of its very potent kinase activity, thereby initiating downstream signaling and cell proliferation. ErbB2 is a frequent pathologic marker in ductal invasive breast carcinomas and is targeted by using a specific humanized monoclonal antibody, trastuzumab (Herceptin). The antibody is effective in only 20% to 50% of erbB2-positive tumors, and this resistance, as yet poorly understood, constitutes a major therapeutic challenge. METHODS: Magnetic microspheres coated with ligands or antibodies are widely used for separation of proteins and cells and allow localized, high intensity, and precisely timed stimulation of cells. We used EGF- and trastuzumab-covered paramagnetic microspheres, quantitative confocal laser scanning microscopy, and digital image processing to investigate the (trans)activation of and local signal propagation from erbB1 and erbB2 on trastuzumab sensitive and resistant carcinoma cell lines expressing these receptors at high levels. RESULTS: On A431 cells expressing high levels of endogenous erbB1 and transfected erbB2-mYFP (A4-erbB2-mYFP F4 cell line), EGF-coupled-microspheres activated erbB1 and transactivated erbB2-mYFP. In two other cell lines with comparable erbB2 expression but lower levels of erbB1, EGF microspheres transactivated erbB2 less efficiently. Trastuzumab in solution activated erbB2 on A4-erbB2-mYFP and the trastuzumab sensitive SKBR-3 cells, but only negligibly on the resistant JIMT-1 cells that showed a 10 times higher K(d) for the antibody. Nevertheless, pronounced erbB2 activation and tyrosine phosphorylation could be detected after stimulation with trastuzumab-coupled microspheres in all cell lines, although transactivation of erbB1 was negligible. Receptor phosphorylation was restricted to the immediate proximity of the microspheres, i.e., receptor clusters external to these locations remained inactive. CONCLUSION: ErbB1 ligand and erbB2 specific antibody attached to magnetic microspheres are efficient tools in assessing erbB activation, localized signal propagation, and erbB heterodimer formation. Trastuzumab coupled to microspheres is more efficient at accessing erbB2 and activating it than trastuzumab in solution
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk Animals Antibodies Antibodies,Monoclonal Biophysics Carcinoma Cell Line Cell Line,Tumor Cell Proliferation Cells chemistry drug effects Drug Resistance,Neoplasm Epidermal Growth Factor genetics Humans Hungary Ligands Magnetics metabolism methods Microscopy Microspheres pharmacology Phosphorylation Proteins Receptor,erbB-2 Research Signal Transduction Solubility Support Trans-Activation (Genetics)
Megjelenés:	Cytometry. Part A. - 67 : 2 (2005), p. 161-171. -
További szerzők:	Arndt-Jovin, Donna J. Nagy Péter (1971-) (biofizikus) Jovin, Thomas M. Szöllősi János (1953-) (biofizikus) Vereb György (1965-) (biofizikus, orvos)
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9.

001-es BibID:	BIBFORM087409
Első szerző:	Hajdu Tímea (biomérnök)
Cím:	Comprehensive Model for Epidermal Growth Factor Receptor Ligand Binding Involving Conformational States of the Extracellular and the Kinase Domains / Tímea Hajdu, Tímea Váradi, István Rebenku, Tamás Kovács, János Szöllösi, Péter Nagy
Dátum:	2020
ISSN:	2296-634X
Megjegyzések:	The epidermal growth factor (EGF) receptor (EGFR) undergoes ligand-dependent dimerization to initiate transmembrane signaling. Although crystallographic structures of the extracellular and kinase domains are available, ligand binding has not been quantitatively analyzed taking the influence of both domains into account. Here, we developed a model explicitly accounting for conformational changes of the kinase and extracellular domains, their dimerizations and ligand binding to monomeric and dimeric receptor species. The model was fitted to ligand binding data of suspended cells expressing receptors with active or inactive kinase conformations. Receptor dimers with inactive, symmetric configuration of the kinase domains exhibit positive cooperativity and very weak binding affinity for the first ligand, whereas dimers with active, asymmetric kinase dimers are characterized by negative cooperativity and subnanomolar binding affinity for the first ligand. The homodimerization propensity of EGFR monomers with active kinase domains is _100-times higher than that of dimers with inactive kinase domains. Despite this fact, constitutive, ligand-independent dimers are mainly generated from monomers with inactive kinase domains due to the excess of such monomers in the membrane. The experimental finding of increased positive cooperativity at high expression levels of EGFR was recapitulated by the model. Quantitative prediction of ligand binding to different receptor species revealed that EGF binds to receptor monomers and dimers in an expression-level dependent manner without significant recruitment of monomers to dimers upon EGF stimulation below the phase transition temperature of the membrane. Results of the fitting offer unique insight into the workings of the EGFR.
Tárgyszavak:	Természettudományok Biológiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk EGF EGFR
Megjelenés:	Frontiers in Cell and Developmental Biology. - 8 (2020), p. 1-53. -
További szerzők:	Váradi Tímea (1973-) (biológus) Rebenku István Kovács Tamás (1985-) (általános orvos) Szöllősi János (1953-) (biofizikus) Nagy Péter (1971-) (biofizikus)
Pályázati támogatás:	GINOP-2.3.2-15-2016-00020 GINOP GINOP-2.2.1-15-2017-00044 GINOP NKFIH K120302 Egyéb
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10.

001-es BibID:	BIBFORM004665
035-os BibID:	(scopus)0034033048 (wos)000086686100012
Első szerző:	Hederer, Rosemarie A.
Cím:	The CD45 tyrosine phosphatase regulates Campath-1H (CD52)-induced TCR-dependent signal transduction in human T cells / Hederer, R. A., Guntermann, C., Miller, N., Nagy, P., Szollosi, J., Damjanovich, S., Hale, G., Alexander, D. R.
Dátum:	2000
Megjegyzések:	Campath-1H, a humanized mAb undergoing clinical trials for treatment of leukemia, transplantation and autoimmune diseases, produces substantial lymphocyte depletion in vivo.The antibody binds to CD52, a highly glycosylated molecule attached to the membrane by a glycosylphosphatidylinositol anchor. Cross-linked Campath-1H is known to activate T cells in vitro. We have investigated the molecular basis for these effects by comparing the protein tyrosine phosphorylation signals induced by Campath-1H and the CD3 mAb OKT3 in primary T cells, and in CD45(+)TCR(+), CD45(-)TCR(+) and CD45(+)TCR(-) Jurkat subclones transfected with CD52. Our results show that Campath-1H triggers similar tyrosine phosphorylation events as OKT3 in both primary T cells and in the CD45(+)TCR(+) Jurkat sub-clone, albeit at quantitatively lower levels. However, no phospholipase C gamma 1 activation nor calcium signals were detected in response to CD52 ligation. The CD52-mediated induction of protein tyrosine phosphorylation was absolutely dependent upon the expression of both the TCR and the CD45 phosphotyrosine phosphatase at the cell surface. Cross-linking of Campath-1H was essential for signal transduction in all cells investigated. Fluorescence resonance energy transfer was used to demonstrate CD52 homo-association at the cell surface in Jurkat T cells in a TCR- and CD45-independent manner, and CD52-TCR association in CD45(+)TCR(+) cells. We propose a model to explain the activating effects of Campath-1H in which CD52 mAb cross-linking causes the trapping of TCR polypeptides within molecular complexes at the cell surface, thereby inducing signals via the TCR by a process which depends on the CD45-mediated regulation of the p56(lck) and p59(fyn) tyrosine kinases.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk Antibodies, Monoclonal Antibodies, Neoplasm Antigens, CD Antigens, CD45 Calcium Calcium Signaling Cells, Cultured Comparative Study Energy Transfer enzymology Fluorescence genetics Glycoproteins Human immunology In Vitro Inositol 1,4,5-Trisphosphate Isoenzymes Jurkat Cells metabolism Phospholipase C physiology Receptors, Antigen, T-Cell Signal Transduction Support, Non-U.S.Gov't T-Lymphocytes Transfection
Megjelenés:	International Immunology. - 12 : 4 (2000), p. 505-516. -
További szerzők:	Guntermann, Christine Miller, Nigel Nagy Péter (1971-) (biofizikus) Szöllősi János (1953-) (biofizikus) Damjanovich Sándor (1936-2017) (biofizikus) Hale, Geoffrey Alexander, Denis R.
Internet cím:	DOI elektronikus változat
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11.

001-es BibID:	BIBFORM050047
Első szerző:	Király Anna
Cím:	Hypoxia reduces the efficiency of elisidepsin by inhibiting hydroxylation and altering the structure of lipid rafts / Anna Király, Tímea Váradi, Tímea Hajdu, Ralph Rühl, Carlos M. Galmarini, János Szöllősi, Peter Nagy
Dátum:	2013
Megjegyzések:	The mechanism of action of elisidepsin (PM02734, Irvalec(R)) is assumed to involve membrane permeabilization via attacking lipid rafts and hydroxylated lipids. Here we investigate the role of hypoxia in the mechanism of action of elisidepsin. Culturing under hypoxic conditions increased the half-maximal inhibitory concentration and decreased the drug's binding to almost all cell lines which was reversed by incubation of cells with 2-hydroxy palmitic acid. The expression of fatty acid 2-hydroxylase was strongly correlated with the efficiency of the drug and inversely correlated with the effect of hypoxia. Number and brightness analysis and fluorescence anisotropy experiments showed that hypoxia decreased the clustering of lipid rafts and altered the structure of the plasma membrane. Although the binding of elisidepsin to the membrane is non-cooperative, its membrane permeabilizing effect is characterized by a Hill coefficient of ~3.3. The latter finding is in agreement with elisidepsin-induced clusters of lipid raft-anchored GFP visualized by confocal microscopy. We propose that the concentration of elisidepsin needs to reach a critical level in the membrane above which elisidepsin induces the disruption of the cell membrane. Testing for tumor hypoxia or the density of hydroxylated lipids could be an interesting strategy to increase the efficiency of elisidepsin
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban analysis Anisotropy article Biophysics cell biology Cell Line Cell Membrane Cells Confocal Confocal microscopy EXPRESSION Fluorescence FLUORESCENCE ANISOTROPY Hungary lipid raft LIPID RAFTS Lipids Microscopy Research Research Support Support
Megjelenés:	Marine Drugs. - 11 : 12 (2013), p. 4858-4875. -
További szerzők:	Váradi Tímea (1982-) (okleveles vegyész) Hajdu Tímea (1991-) (biomérnök) Rühl, Ralph (1969-) (vegyész) Galmarini, Carlos M. Szöllősi János (1953-) (biofizikus) Nagy Péter (1971-) (biofizikus)
Internet cím:	DOI Szerző által megadott URL Intézményi repozitóriumban (DEA) tárolt változat
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12.

001-es BibID:	BIBFORM005185
035-os BibID:	(scopus)46449085498 (wos)000257176000003
Első szerző:	Kiss Endre (Budapest)
Cím:	Cytometry of raft and caveola membrane microdomains : from flow and imaging techniques to high throughput screening assays / Kiss, E., Nagy, P., Balogh, A., Szollosi, J., Matko, J.
Dátum:	2008
ISSN:	552-4930 (Electronic)
Megjegyzések:	The evolutionarily developed microdomain structure of biological membranes has gained more and more attention in the past decade. The caveolin-free "membrane rafts," the caveolin-expressing rafts (caveolae), as well as other membrane microdomains seem to play an essential role in controlling and coordinating cell-surface molecular recognition, internalization/endocytosis of the bound molecules or pathogenic organisms and in regulation of transmembrane signal transduction processes. Therefore, in many research fields (e.g. neurobiology and immunology), there is an ongoing need to understand the nature of these microdomains and to quantitatively characterize their lipid and protein composition under various physiological and pathological conditions. Flow and image cytometry offer many sophisticated and routine tools to study these questions. In this review, we give an overview of the past efforts to detect and characterize these membrane microdomains by the use of classical cytometric technologies, and finally we will discuss the results and perspectives of a new line of raft cytometry, the "high throughput screening assays of membrane microdomains," based on "lipidomic" and "proteomic" approaches.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban folyóiratcikk Animals article Caveolae Cell Membrane chemistry Detergents Flow Cytometry Fluorescence Resonance Energy Transfer Humans Hungary Image Cytometry immunology Lipids Membrane Lipids Membrane Microdomains metabolism methods pharmacology Protein Structure, Tertiary Proteomics Research Research Support Signal Transduction Support
Megjelenés:	Cytometry. Part A. - 73A : 7 (2008), p. 599-614. -
További szerzők:	Nagy Péter (1971-) (biofizikus) Balogh Andrea Szöllősi János (1953-) (biofizikus) Matkó János (1952-) (biológus)
Internet cím:	DOI elektronikus változat
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