Your search keyword '"Eva Juhasz"' showing total 19 results

1. Expression of Growth Hormone-Releasing Hormone and Its Receptor Splice Variants in Primary Human Endometrial Carcinomas: Novel Therapeutic Approaches

Author

Zsuzsanna Szabo, Eva Juhasz, Andrew V. Schally, Balazs Dezso, Sandor Huga, Zoltan Hernadi, Gabor Halmos, and Csongor Kiss

Subjects

GHRH, receptors for GHRH, splice variants, human endometrial carcinoma, Organic chemistry, QD241-441

Abstract

Antagonists of growth hormone-releasing hormone (GHRH) inhibit the growth of various tumors, including endometrial carcinomas (EC). However, tumoral receptors that mediate the antiproliferative effects of GHRH antagonists in human ECs have not been fully characterized. In this study, we investigated the expression of mRNA for GHRH and splice variants (SVs) of GHRH receptors (GHRH-R) in 39 human ECs and in 7 normal endometrial tissue samples using RT-PCR. Primers designed for the PCR amplification of mRNA for the full length GHRH-R and SVs were utilized. The PCR products were sequenced, and their specificity was confirmed. Nine ECs cancers (23%) expressed mRNA for SV1, three (7.7%) showed SV2 and eight (20.5%) revealed mRNA for SV4. The presence of SVs for GHRH-Rs could not be detected in any of the normal endometrial tissue specimens. The presence of specific, high affinity GHRH-Rs was also demonstrated in EC specimens using radioligand binding studies. Twenty-four of the investigated thirty-nine tumor samples (61.5%) and three of the seven corresponding normal endometrial tissues (42.9%) expressed mRNA for GHRH ligand. Our findings suggest the possible existence of an autocrine loop in EC based on GHRH and its tumoral SV receptors. The antiproliferative effects of GHRH antagonists on EC are likely to be exerted in part by the local SVs and GHRH system.

Published

2022

2. Expression of Somatostatin Receptor Subtypes (SSTR-1–SSTR-5) in Pediatric Hematological and Oncological Disorders

Author

Kristof Harda, Zsuzsanna Szabo, Eva Juhasz, Balazs Dezso, Csongor Kiss, Andrew V. Schally, and Gabor Halmos

Subjects

hematological-oncological disorders in children, somatostatin receptors, somatostatin analogs, Organic chemistry, QD241-441

Abstract

Hematological and oncological disorders represent leading causes of childhood mortality. Neuropeptide somatostatin (SST) has been previously demonstrated in various pediatric tumors, but limited information exists on the expression and characteristics of SST receptors (SSTR) in hematological and oncological disorders of children. We aimed to investigate the expression of mRNA for SSTR subtypes (SSTR-1–5) in 15 pediatric hematological/oncological specimens by RT-PCR. The presence and binding characteristics of SSTRs were further studies by ligand competition assay. Our results show that the pediatric tumor samples highly expressed mRNA for the five SSTR subtypes with various patterns. The mRNA for SSTR-2 was detected in all specimens independently of their histological type. A Hodgkin lymphoma sample co-expressed mRNA for all five SSTR subtypes. SSTR-3 and SSTR-5 were detected only in malignant specimens, such as rhabdomyosarcoma, Hodgkin lymphoma, acute lymphoblastic leukemia, and a single nonmalignant condition, hereditary spherocytosis. The incidence of SSTR-1 and SSTR-4 was similar (60%) in the 15 specimens investigated. Radioligand binding studies demonstrated the presence of specific SSTRs and high affinity binding of SST analogs in pediatric solid tumors investigated. The high incidence of SSTRs in hematological and oncological disorders in children supports the merit of further investigation of SSTRs as molecular targets for diagnosis and therapy.

Published

2020

3. Ileoanal Pouches - Is Mucosectomy Essential?

Author

Roger R Dozios and Eva Juhasz

Subjects

Diseases of the digestive system. Gastroenterology, RC799-869

Published

1993

4. Expression of Growth Hormone-Releasing Hormone and Its Receptor Splice Variants in Primary Human Endometrial Carcinomas: Novel Therapeutic Approaches

Author

Kiss, Zsuzsanna Szabo, Eva Juhasz, Andrew V. Schally, Balazs Dezso, Sandor Huga, Zoltan Hernadi, Gabor Halmos, and Csongor

Subjects

endocrine system, GHRH, receptors for GHRH, splice variants, human endometrial carcinoma, hormones, hormone substitutes, and hormone antagonists

Abstract

Antagonists of growth hormone-releasing hormone (GHRH) inhibit the growth of various tumors, including endometrial carcinomas (EC). However, tumoral receptors that mediate the antiproliferative effects of GHRH antagonists in human ECs have not been fully characterized. In this study, we investigated the expression of mRNA for GHRH and splice variants (SVs) of GHRH receptors (GHRH-R) in 39 human ECs and in 7 normal endometrial tissue samples using RT-PCR. Primers designed for the PCR amplification of mRNA for the full length GHRH-R and SVs were utilized. The PCR products were sequenced, and their specificity was confirmed. Nine ECs cancers (23%) expressed mRNA for SV1, three (7.7%) showed SV2 and eight (20.5%) revealed mRNA for SV4. The presence of SVs for GHRH-Rs could not be detected in any of the normal endometrial tissue specimens. The presence of specific, high affinity GHRH-Rs was also demonstrated in EC specimens using radioligand binding studies. Twenty-four of the investigated thirty-nine tumor samples (61.5%) and three of the seven corresponding normal endometrial tissues (42.9%) expressed mRNA for GHRH ligand. Our findings suggest the possible existence of an autocrine loop in EC based on GHRH and its tumoral SV receptors. The antiproliferative effects of GHRH antagonists on EC are likely to be exerted in part by the local SVs and GHRH system.

Published

2022

5. Potential Teratogenicity Effects of Metals on Avian Embryos

Author

Rita Szabó, Péter Budai, Éva Juhász, László Major, and József Lehel

Subjects

cadmium, copper, lead, developmental abnormalities, mortality, environmental safety, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Agricultural areas can provide sources of food and hiding and nesting places for wild birds. Thus, the chemical load of potentially toxic elements (Cd, Cu, Pb) due to industrial and agricultural activities can affect not only the adult birds but also the embryos developing in the egg. The toxic effects of heavy metals applied alone were investigated on chicken embryos in the early and late stages of embryonic development using injection and immersion treatment methods. On day 3 of incubation, permanent preparations were made from the embryos to study the early development stage. There were no significant differences observed in embryo deaths and developmental abnormalities in this stage. On day 19 of incubation, the number of embryonic deaths, the body weight of the embryos, and the type of developmental abnormalities were examined. The embryonic mortality was statistically higher in the groups treated with cadmium and lead in the case of the injection treatment. A significant increase in developmental disorders was observed in the copper-treated group using the immersion application. The body weight significantly decreased in the cadmium- and lead-treated group using both treatment methods. However, a significant change in the body weight in the copper-treated group was only realized due to the injection method.

Published

2024

6. Contributors

Author

Marah Armouti, John A. Arnott, Kushal Bakshi, Natalie J. Bales, Mary Beth Bauer, Nathan A. Berger, Daniel J. Bernard, Mark Blostein, M. Luisa Bonet, Amanda P. Borrow, Gregory A. Brent, Emilie Brûlé, Max H. Cake, Giulia Cantini, Ayano Chiba, George P. Chrousos, Sila Cocciolillo, R. Comaposada-Baró, Kevin P.M. Currie, Pierre De Meyts, Ilaria Dicembrini, Clark W. Distelhorst, Nikoletta Dobos, David E. Fisher, M.L. Franco, Gabor Halmos, Robert J. Handa, Elie Hobeika, Eva Juhasz, Hamsini Sudheer Kala, Lajos V. Kemeny, Ruth A. Keri, Haruka Kobayashi, Christopher S. Kovacs, Kalman Kovacs, Pierre J. Lefèbvre, Carole Le Henaff, P.R. Le Tissier, Gerald Litwack, Yan-Yun Liu, null Sonia Lobo, Michaela Luconi, David J. Lyons, Rong Ma, Robert T. Mallet, Edoardo Mannucci, Anna Milanesi, Naoki Mochizuki, J.F. Murray, Nicolas C. Nicolaides, Kostas Pantopoulos, Nicola C. Partridge, Doodipala Samba Reddy, Lina M. Restrepo, Joan Ribot, Allison J. Richard, Ana M. Rodríguez, Nicola Romanò, Fabio Rotondo, Andrew V. Schally, Giada Sebastiani, Carlos A. Serna, Nima Sharifi, null Michael J. Shipston, Jacqueline M. Stephens, Carlos Stocco, Sally A. Stover, Luis V. Syro, Zsuzsanna Szabo, Martina Trabucco, M. Vilar, David E. Volk, Helge Waldum, Richard J. Wurtman, George C.T. Yeoh, Yue Yu, and Eleonora Zakharian

Published

2020

7. Hypothalamic Releasing Hormones

Author

Gabor Halmos, Eva Juhasz, Andrew V. Schally, Nikoletta Dobos, and Zsuzsanna Szabó

Subjects

endocrine system, medicine.medical_specialty, Thyrotropin-releasing hormone, Biology, Corticotropin-releasing hormone, Endocrinology, medicine.anatomical_structure, Somatostatin, Hypothalamic Hormones, Anterior pituitary, Hypothalamus, Internal medicine, medicine, Luteinizing hormone, Hormone

Abstract

Neurohormones produced in the hypothalamus and transported by the hypophyseal portal vessels to the anterior pituitary gland control its secretion of trophic hormones adrenocorticotropic hormone, thyroid-stimulating hormone, follicle-stimulating hormone, luteinizing hormone, growth hormone, and prolactin. Hypothalamic hormones regulate various bodily functions such as growth, reproduction, lactation, metabolism, gastrointestinal function, and response to stress, as well as pathologic processes including tumorigenesis through the adenohypophyseal hormones and the hormones secreted by the target glands. The effects exerted are covered in books of physiology, medical endocrinology, oncology, pharmacology, and drug therapy. It is not within the scope of this review to survey all the available findings. This chapter consists of brief sections reviewing the current knowledge on each of the hypothalamic hormones, thyrotropin releasing hormone, corticotropin releasing hormone, luteinizing hormone-releasing hormone/gonadotropin-releasing hormone, somatostatin, growth hormone-releasing hormone, and prolactin-releasing factors, and listing their structures, evolution, receptors, signaling pathways, and physiologic functions. The status of potent synthetic analogs of hypothalamic peptides as promising drug candidates for the treatment of various diseases and conditions, especially endocrine disorders and cancer, and their applications in current clinical therapies are also summarized.

Published

2020

8. Expression of Growth Hormone-Releasing Hormone and Its Receptor Splice Variants in a Cohort of Hungarian Pediatric Patients with Hematological and Oncological Disorders: A Pilot Study

Author

Éva Juhász, Zsuzsanna Szabó, Andrew V. Schally, József Király, Petra Fodor, Gábor Kónya, Balázs Dezső, Erzsébet Szabó, Gábor Halmos, and Csongor Kiss

Subjects

hematological-oncological disorders in children, GHRH, GHRH receptor, splice variant, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Hematological and oncological diseases are still among the leading causes of childhood mortality. Expression of growth hormone-releasing hormone (GHRH) and its receptors (GHRH-R) has been previously demonstrated in various human tumors, but very limited findings are available about the presence and potential function of GHRH-Rs in oncological and hematological disorders of children. In this study, we aimed to investigate the expression of mRNA for GHRH and splice variant 1 (SV) of GHRH-R in 15 pediatric hematological/oncological specimens by RT-PCR. The presence and binding characteristics of GHRH-R protein were also studied by Western blot and ligand competition assays. Of the fifteen specimens studied, eleven pediatric samples (73%) showed the expression of mRNA for GHRH. These eleven samples also expressed mRNA for GHRH receptor SV1. GHRH-R protein was found to be expressed in two benign tumor samples and five malignant tumors examined by Western blot. The presence of specific, high affinity binding sites on GHRH-R was demonstrated in all of the seven human pediatric solid tumor samples investigated. Our results show that the expression of GHRH and SV1 of GHRH-R in hemato-oncological diseases in children can pave the way for further investigation of GHRH-Rs as potential molecular targets for diagnosis and therapy.

Published

2024

9. Axillary dissection versus no axillary dissection in patients with breast cancer and sentinel-node micrometastases (IBCSG 23-01): 10-year follow-up of a randomised, controlled, phase 3 trial

Author

Achim Fleischmann, Cindy Mak, Jane Hill, David Littlejohn, Andreas Veronesi, Holger Moch, Stefano Zurrida, L Perey, Nirmala Pathmanathan, Carlo Tondini, Giancarlo Pruneri, Viviana Galimberti, Christian Oehlschlegel, Christoph Rageth, Jack Hoffmann, Richard D. Gelber, John J. Collins, Angelo Recalcati, Marisa Donatella Magri, Andrée Rorive, Bruno Späti, Dimitri Sarlos, Zsuzsanna Varga, Rolf A. Stahel, Mattia Intra, Charlotte Lanng, P. Smart, L. Tan, Anna Cardillo, Francesco Coran, James French, Rudolf Maibach, Manuela Rabaglio, Marco Colleoni, Emilia Montagna, Elisabeth Saurenmann, Elisabeth Elder, Michael Knauer, Samuele Massarut, Mauro Arcicasa, Karin Ribi, Julie Craik, Theresa Zielinski, Wendy Jeanneret Sozzi, Sandro Morassut, Tiziana Rusca, Paul Chin, Elgene Lim, Frances M. Boyle, Richard West, Patrizia Dell'Orto, Umberto Veronesi, Marie-Christine Mathieu, Jean-Remi Garbay, Katrina Moore, Marisa Cristina Leonardi, Gregory Bruce Mann, Donatella Santini, Mario Roncadin, Joëlle Collignon, Michael D. Green, David Moon, Oreste Gentilini, Petere G. Gill, Stephen Allpress, Giulia Peruzzotti, Elga Majdic, Caitlin Mahoney, Karen N. Price, Craig Murphy, Lori Hayes, Melissa Bochner, Lynette Mann, Christoph Tausch, Otto Schiltknecht, Antonino Carbone, Aron Goldhirsch, Giuseppe Cancello, Anand Murugasu, John F. Forbes, Erica Piccoli, Luca Mazzucchelli, Alberto Gianatti, Lucien Zaman, Jose Manuel Cotrina, Per Karlsson, Janez Zgajnar, Diana Crivellari, Birgitte Bruun Rasmussen, Elisabetta Candiago, Manuela Sargenti, Robert Whitfield, Silvia Dellapasqua, R. Ghisini, Meredith M. Regan, Michael Müller, Tiziana Perin, M. Thorburn, Stamatina Fournarakou, Monika Bamert, Malcolm Buchanan, Allison Jones, Gerhard Ries, Andreas Ehrsam, Hugh Carmalt, István Láng, Jürg Bernhard, Guy Jerusalem, Manuela Lagrassa, S. Fiona Bonar, Mario Mileto, Jurij Lindtner, P. Jeal, Fereshte Farshidi, Bernard F. Cole, John Hoerby, James Kollias, Privato Fenaroli, Giovanni Mazzarol, Richard Dyer, Angelo Buonadonna, Heidi Roschitzki, Stefania Andrighetto, Robert Macindoe, Martin F. Fey, Ingrid Kössler, Olivia Pagani, Anita Hiltbrunner, Camelia Chifu, William Ross, Rachele Volpe, Linda Leidi, Barbara Ruepp, Giorgio Caccia, Philippe Delvenne, Susanne Gerred, Tara Scolese, Mario Taffurelli, Paola Baratella, Jean Francois Delaloye, Richard Harman, A. Michael Bilous, Ian G. Campbell, Franco Nolè, Maryse Fiche, Ute Lorenz, Susanne Roux, Roberto Orecchia, Mark Sywak, Aashit Shah, Assia Treboux, Laura Cattaneo, Martina Egli-Tupaj, Rosmarie Caduff, Paolo Veronesi, Linda Madigan, Elena Kralidis, Maj-Lis Moeller Talman, Roswitha Kammler, Michael Töpfer, Eva Juhasz, Peer Schousen, Michele Ghielmini, Snjezana Frkovic-Grazio, Hanne Galatius, Elisabeth Rippy, Sylvie Maweja, Lynette Blacher, Stefan Aebi, D.F. Preece, Gilles Berclaz, Daniel Wyss, D. F. Lindsay, Andreas Günthert, Frederick Mayall, Lucia Bronz, Paul McKenzie, Andrew J. Spillane, Giuseppe Viale, Sandra Lippert, Alberto Luini, Virginia Howard, Giuseppe Curigliano, Rainer Grobholz, Robert Millar, Julio Abugattas, Hans-Anton Lehr, Maria Emanuela Limonta, Monica Iorfida, Elisa Vicini, Helle Holtveg, Angelo Di Leo, Giuseppe Renne, Alan S. Coates, Ezio Candiani, Karolyn Scott, Mauro G. Mastropasqua, Paolo Tricomi, Thomas Gyr, Karen Briscoe, and Viviana Galimberti, Bernard F Cole, Giuseppe Viale, Paolo Veronesi, Elisa Vicini, Mattia Intra, Giovanni Mazzarol, Samuele Massarut, Janez Zgajnar, Mario Taffurelli, David Littlejohn, Michael Knauer, Carlo Tondini, Angelo Di Leo, Marco Colleoni, Meredith M Regan, Alan S Coates, Richard D Gelber, Aron Goldhirsch

Subjects

0301 basic medicine, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Population, Breast Neoplasms, Disease-Free Survival, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Risk Factors, Clinical endpoint, Medicine, Humans, education, Mastectomy, education.field_of_study, business.industry, Sentinel Lymph Node Biopsy, Hazard ratio, Sentinel node, medicine.disease, Breast cancer, axillary dissection, IBCSG 23-01, follow up, Surgery, Clinical trial, Axilla, 030104 developmental biology, medicine.anatomical_structure, Oncology, Neoplasm Micrometastasis, 030220 oncology & carcinogenesis, Lymphatic Metastasis, Disease Progression, Lymph Node Excision, Female, Sentinel Lymph Node, business

Abstract

Summary Background We previously reported the 5-year results of the phase 3 IBCSG 23-01 trial comparing disease-free survival in patients with breast cancer with one or more micrometastatic (≤2 mm) sentinel nodes randomly assigned to either axillary dissection or no axillary dissection. The results showed no difference in disease-free survival between the groups and showed non-inferiority of no axillary dissection relative to axillary dissection. The current analysis presents the results of the study after a median follow-up of 9·7 years (IQR 7·8–12·7). Methods In this multicentre, randomised, controlled, open-label, non-inferiority, phase 3 trial, participants were recruited from 27 hospitals and cancer centres in nine countries. Eligible women could be of any age with clinical, mammographic, ultrasonographic, or pathological diagnosis of breast cancer with largest lesion diameter of 5 cm or smaller, and one or more metastatic sentinel nodes, all of which were 2 mm or smaller and with no extracapsular extension. Patients were randomly assigned (1:1) before surgery (mastectomy or breast-conserving surgery) to no axillary dissection or axillary dissection using permuted blocks generated by a web-based congruence algorithm, with stratification by centre and menopausal status. The protocol-specified primary endpoint was disease-free survival, analysed in the intention-to-treat population (as randomly assigned). Safety was assessed in all randomly assigned patients who received their allocated treatment (as treated). We did a one-sided test for non-inferiority of no axillary dissection by comparing the observed hazard ratios (HRs) for disease-free survival with a margin of 1·25. This 10-year follow-up analysis was not prespecified in the trial's protocol and thus was not adjusted for multiple, sequential testing. This trial is registered with ClinicalTrials.gov, number NCT00072293. Findings Between April 1, 2001, and Feb 8, 2010, 6681 patients were screened and 934 randomly assigned to no axillary dissection (n=469) or axillary dissection (n=465). Three patients were ineligible and were excluded from the trial after randomisation. Disease-free survival at 10 years was 76·8% (95% CI 72·5–81·0) in the no axillary dissection group, compared with 74·9% (70·5–79·3) in the axillary dissection group (HR 0·85, 95% CI 0·65–1·11; log-rank p=0·24; p=0·0024 for non-inferiority). Long-term surgical complications included lymphoedema of any grade in 16 (4%) of 453 patients in the no axillary dissection group and 60 (13%) of 447 in the axillary dissection group, sensory neuropathy of any grade in 57 (13%) in the no axillary dissection group versus 85 (19%) in the axillary dissection group, and motor neuropathy of any grade (14 [3%] in the no axillary dissection group vs 40 [9%] in the axillary dissection group). One serious adverse event (postoperative infection and inflamed axilla requiring hospital admission) was attributed to axillary dissection; the event resolved without sequelae. Interpretation The findings of the IBCSG 23-01 trial after a median follow-up of 9·7 years (IQR 7·8–12·7) corroborate those obtained at 5 years and are consistent with those of the 10-year follow-up analysis of the Z0011 trial. Together, these findings support the current practice of not doing an axillary dissection when the tumour burden in the sentinel nodes is minimal or moderate in patients with early breast cancer. Funding International Breast Cancer Study Group.

Published

2018

10. Targeting the Melanocortin 1 Receptor in Melanoma: Biological Activity of α-MSH–Peptide Conjugates

Author

Ildikó Szabó, Beáta Biri-Kovács, Balázs Vári, Ivan Ranđelović, Diána Vári-Mező, Éva Juhász, Gábor Halmos, Szilvia Bősze, József Tóvári, and Gábor Mező

Subjects

α-MSH, melanoma, peptide–drug conjugates, in vitro antiproliferative effect, in vivo antitumor activity, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Malignant melanoma is one of the most aggressive and resistant tumor types, with high metastatic properties. Because of the lack of suitable chemotherapeutic agents for treatment, the 5-year survival rate of melanoma patients with regional and distant metastases is lower than 10%. Targeted tumor therapy that provides several promising results might be a good option for the treatment of malignant melanomas. Our goal was to develop novel melanoma-specific peptide–drug conjugates for targeted tumor therapy. Melanocortin-1-receptor (MC1R) is a cell surface receptor responsible for melanogenesis and it is overexpressed on the surface of melanoma cells, providing a good target. Its native ligand, α-MSH (α-melanocyte-stimulating hormone) peptide, or its derivatives, might be potential homing devices for this purpose. Therefore, we prepared three α-MSH derivative–daunomycin (Dau) conjugates and their in vitro and in vivo antitumor activities were compared. Dau has an autofluorescence property; therefore, it is suitable for preparing conjugates for in vitro (e.g., cellular uptake) and in vivo experiments. Dau was attached to the peptides via a non-cleavable oxime linkage that was applied efficiently in our previous experiments, resulting in conjugates with high tumor growth inhibition activity. The results indicated that the most promising conjugate was the compound in which Dau was connected to the side chain of Lys (Ac-SYSNleEHFRWGK(Dau=Aoa)PV-NH2). The highest cellular uptake by melanoma cells was demonstrated using the compound, with the highest tumor growth inhibition detected both on mouse (38.6% on B16) and human uveal melanoma (55% on OMC-1) cells. The effect of the compound was more pronounced than that of the free drug.

Published

2024

11. Flap thickness in femtosecond laser

Author

Eva, Juhasz

Subjects

Corneal Stroma, Keratomileusis, Laser In Situ, Humans, Lasers, Excimer, Surgical Flaps

Published

2015

12. Shikonin Causes an Apoptotic Effect on Human Kidney Cancer Cells through Ras/MAPK and PI3K/AKT Pathways

Author

József Király, Erzsébet Szabó, Petra Fodor, Zsolt Fejes, Béla Nagy, Éva Juhász, Anna Vass, Mahua Choudhury, Gábor Kónya, Gábor Halmos, and Zsuzsanna Szabó

Subjects

shikonin, human renal cancer, CAKI-2, A-498, apoptosis, Ras/MAPK and PI3K/AKT pathways, Organic chemistry, QD241-441

Abstract

(1) Background: Shikonin, the main ingredient in Chinese herbal medicine, is described as a novel angiogenesis inhibitor, and its anticancer effects have already been studied. Shikonin and its derivatives induce apoptosis and suppress metastasis, which further enhance the effectiveness of chemotherapy. However, their mechanism of function has not been completely elucidated on human renal cancer cells. (2) Methods: In our study, CAKI-2 and A-498 cells were treated with increasing concentrations (2.5–40 µM) of shikonin, when colony formation ability and cytotoxic activity were tested. The changes in the expression of the main targets of apoptotic pathways were measured by RT-qPCR and Western blot. The intracellular levels of miR-21 and miR-155 were quantified by RT-qPCR. (3) Results: Shikonin exerted a dose-dependent effect on the proliferation of the cell lines examined. In 5 µM concentration of shikonin in vitro elevated caspase-3 and -7 levels, the proteins of the Ras/MAPK and PI3K/AKT pathways were activated. However, no significant changes were detected in the miR-21 and miR-155 expressions. (4) Conclusions: Our findings indicated that shikonin causes apoptosis of renal cancer cells by activating the Ras/MAPK and PI3K/AKT pathways. These effects of shikonin on renal cancer cells may bear important potential therapeutic implications for the treatment of renal cancer.

Published

2023

13. Assessment of Visual Quality Improvement as a Result of Spectacle Personalization

Author

Fruzsina Benyó, Lilla István, Huba Kiss, Andrea Gyenes, Gábor Erdei, Éva Juhász, Natalia Vlasak, Claudia Unger, Tamás Andorfi, Kata Réz, Illés Kovács, and Zoltán Zsolt Nagy

Subjects

personalized spectacle, visual quality, progressive addition lens, Science

Abstract

Personalized spectacles customized according to an individual’s facial anatomy were developed to provide enhanced visual performance and overall comfort when compared to standard spectacles. In this comparative crossover trial, each subject was randomly assigned to wear either personalized spectacles or standard spectacles for two weeks and then tried the second pair for another two weeks. Visual acuity and reading speed were measured, and visual quality and comfort were assessed using specific questionnaires. The correlation of the wearing parameters with the subjects’ satisfaction was calculated. According to our results, the subjects wearing personalized glasses reported significantly less experience of swaying and significantly higher overall satisfaction compared to those wearing the control spectacles. At the end of the study, 62% of subjects preferred the personalized spectacles, and visual quality was the primary reason for their spectacle preference followed by wearing comfort. The difference from the ideal cornea–vertex distance was significantly lower when wearing the personalized spectacles compared to the control frames. In addition, the absolute value of the difference from the ideal cornea–vertex distance was significantly correlated with patient satisfaction. These results suggest that personalized spectacles, customized according to an individual’s facial anatomy for the ideal wearing parameters, result in both visual and comfort advantages for wearers.

Published

2023

14. First Synthesis of 3-Glycopyranosyl-1,2,4-Triazines and Some Cycloadditions Thereof

Author

Éva Bokor, Attila Ferenczi, Mahir Hashimov, Éva Juhász-Tóth, Zsófia Götz, Alshimaa Ibrahim Zaki, and László Somsák

Subjects

C-glycosyl compound, 1,2,4-triazine, amidrazone, IEDDA, pyridine, Organic chemistry, QD241-441

Abstract

C-glycopyranosyl derivatives of six-membered heterocycles are scarcely represented in the chemical literature and the title 3-glycopyranosyl-1,2,4-triazines are completely unknown. In this paper, the first synthesis of this compound class is accomplished by the cyclocondensation of C-glycosyl formamidrazones and 1,2-dicarbonyl derivatives. In addition, the synthesis of C-glycopyranosyl 1,2,4-triazin-5(4H)-ones was also carried out by the transformation of the above formamidrazones with α-keto-carboxylic esters. Inverse electron demand Diels–Alder reactions of 3-glycopyranosyl-1,2,4-triazines with a bicyclononyne derivative yielded the corresponding annulated 2-glycopyranosyl pyridines.

Published

2022

15. Development and Biochemical Characterization of Self-Immolative Linker Containing GnRH-III-Drug Conjugates

Author

Sabine Schuster, Éva Juhász, Gábor Halmos, Ines Neundorf, Cesare Gennari, and Gábor Mező

Subjects

targeted cancer therapy, drug delivery system, gonadotropin releasing hormone, daunorubicin, paclitaxel, peptide-drug conjugates, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The human gonadotropin releasing hormone (GnRH-I) and its sea lamprey analogue GnRH-III specifically bind to GnRH receptors on cancer cells and can be used as targeting moieties for targeted tumor therapy. Considering that the selective release of drugs in cancer cells is of high relevance, we were encouraged to develop cleavable, self-immolative GnRH-III-drug conjugates which consist of a p-aminobenzyloxycarbonlyl (PABC) spacer between a cathepsin B-cleavable dipeptide (Val-Ala, Val-Cit) and the classical anticancer drugs daunorubicin (Dau) and paclitaxel (PTX). Alongside these compounds, non-cleavable GnRH-III-drug conjugates were also synthesized, and all compounds were analyzed for their antiproliferative activity. The cleavable GnRH-III bioconjugates revealed a growth inhibitory effect on GnRH receptor-expressing A2780 ovarian cancer cells, while their activity was reduced on Panc-1 pancreatic cancer cells exhibiting a lower GnRH receptor level. Moreover, the antiproliferative activity of the non-cleavable counterparts was strongly reduced. Additionally, the efficient cleavage of the Val-Ala linker and the subsequent release of the drugs could be verified by lysosomal degradation studies, while radioligand binding studies ensured that the GnRH-III-drug conjugates bound to the GnRH receptor with high affinity. Our results underline the high value of GnRH-III-based homing devices and the application of cathepsin B-cleavable linker systems for the development of small molecule drug conjugates (SMDCs).

Published

2022

16. Glycogen phosphorylase inhibitor, 2,3-bis[(2E)-3-(4-hydroxyphenyl)prop-2-enamido] butanedioic acid (BF142), improves baseline insulin secretion of MIN6 insulinoma cells.

Author

Lilla Nagy, Ferenc Béke, László Juhász, Tünde Kovács, Éva Juhász-Tóth, Tibor Docsa, Attila Tóth, Pál Gergely, László Somsák, and Péter Bai

Subjects

Medicine, Science

Abstract

Type 2 diabetes mellitus (T2DM), one of the most common metabolic diseases, is characterized by insulin resistance and inadequate insulin secretion of β cells. Glycogen phosphorylase (GP) is the key enzyme in glycogen breakdown, and contributes to hepatic glucose production during fasting or during insulin resistance. Pharmacological GP inhibitors are potential glucose lowering agents, which may be used in T2DM therapy. A natural product isolated from the cultured broth of the fungal strain No. 138354, called 2,3-bis(4-hydroxycinnamoyloxy)glutaric acid (FR258900), was discovered a decade ago. In vivo studies showed that FR258900 significantly reduced blood glucose levels in diabetic mice. We previously showed that GP inhibitors can potently enhance the function of β cells. The purpose of this study was to assess whether an analogue of FR258900 can influence β cell function. BF142 (Meso-Dimethyl 2,3-bis[(E)-3-(4-acetoxyphenyl)prop-2-enamido]butanedioate) treatment activated the glucose-stimulated insulin secretion pathway, as indicated by enhanced glycolysis, increased mitochondrial oxidation, significantly increased ATP production, and elevated calcium influx in MIN6 cells. Furthermore, BF142 induced mTORC1-specific phosphorylation of S6K, increased levels of PDX1 and insulin protein, and increased insulin secretion. Our data suggest that BF142 can influence β cell function and can support the insulin producing ability of β cells.

Published

2020

17. Prenylation inhibition-induced cell death in melanoma: reduced sensitivity in BRAF mutant/PTEN wild-type melanoma cells.

Author

Tamás Garay, István Kenessey, Eszter Molnár, Éva Juhász, Andrea Réti, Viktória László, Anita Rózsás, Judit Dobos, Balázs Döme, Walter Berger, Walter Klepetko, József Tóvári, József Tímár, and Balázs Hegedűs

Subjects

Medicine, Science

Abstract

While targeted therapy brought a new era in the treatment of BRAF mutant melanoma, therapeutic options for non-BRAF mutant cases are still limited. In order to explore the antitumor activity of prenylation inhibition we investigated the response to zoledronic acid treatment in thirteen human melanoma cell lines with known BRAF, NRAS and PTEN mutational status. Effect of zoledronic acid on proliferation, clonogenic potential, apoptosis and migration of melanoma cells as well as the activation of downstream elements of the RAS/RAF pathway were investigated in vitro with SRB, TUNEL and PARP cleavage assays and videomicroscopy and immunoblot measurements, respectively. Subcutaneous and spleen-to-liver colonization xenograft mouse models were used to evaluate the influence of zoledronic acid treatment on primary and disseminated tumor growth of melanoma cells in vivo. Zoledronic acid more efficiently decreased short-term in vitro viability in NRAS mutant cells when compared to BRAF mutant and BRAF/NRAS wild-type cells. In line with this finding, following treatment decreased activation of ribosomal protein S6 was found in NRAS mutant cells. Zoledronic acid demonstrated no significant synergism in cell viability inhibition or apoptosis induction with cisplatin or DTIC treatment in vitro. Importantly, zoledronic acid could inhibit clonogenic growth in the majority of melanoma cell lines except in the three BRAF mutant but PTEN wild-type melanoma lines. A similar pattern was observed in apoptosis induction experiments. In vivo zoledronic acid did not inhibit the subcutaneous growth or spleen-to-liver colonization of melanoma cells. Altogether our data demonstrates that prenylation inhibition may be a novel therapeutic approach in NRAS mutant melanoma. Nevertheless, we also demonstrated that therapeutic sensitivity might be influenced by the PTEN status of BRAF mutant melanoma cells. However, further investigations are needed to identify drugs that have appropriate pharmacological properties to efficiently target prenylation in melanoma cells.

Published

2015

18. Evaluation of intereye corneal asymmetry in patients with keratoconus. A scheimpflug imaging study.

Author

Lóránt Dienes, Kinga Kránitz, Eva Juhász, Andrea Gyenes, Agnes Takács, Kata Miháltz, Zoltán Z Nagy, and Illés Kovács

Subjects

Medicine, Science

Abstract

PURPOSE: To assess the correlation between keratoconus severity and intereye asymmetry of pachymetric data and posterior elevation values and to evaluate their combined accuracy in discriminating normal corneas from those with keratoconus. METHODS: This study included 97 patients: 65 subjects with bilateral normal corneas (NC) and 32 with keratoconus (KC). Central corneal thickness (CCT), thinnest corneal thickness (ThCT) and posterior elevation (PE) at the thinnest point of the cornea were measured in both eyes using Scheimpflug imaging. Intereye asymmetry and its correlation with keratoconus severity were calculated for each variable. The area under the receiver operating characteristic curve (AUROC) was used to compare predictive accuracy of different variables for keratoconus. RESULTS: In normal eyes, intereye differences were significantly lower compared with the keratoconus eyes (p

Published

2014

19. MRSA Transmission between Cows and Humans

Author

Éva Juhász-Kaszanyitzky, Szilárd Jánosi, Pál Somogyi, Ádám Dán, Linda vanderGraaf van Bloois, Engeline van Duijkeren, and Jaap A. Wagenaar

Subjects

Methicillin-resistant Staphylococcus aureus, cows, mastitis, zoonosis, phage types, PFGE, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

We isolated methicillin-resistant Staphylococcus aureus (MRSA) from cows with subclinical mastitis and from a person who worked with these animals. The bovine and human strains were indistinguishable by phenotyping and genotyping methods and were of a low frequency spa type. To our knowledge, this finding indicates the first documented case of direct transmission of MRSA between cows and humans.

Published

2007