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19 results on '"Spengler, Gabriella"'

1. Modulation of the bacterial virulence and resistance by well-known European medicinal herbs

Author

Křížkovská Bára, Hoang Lan, Brdová Daniela, Klementová Kristýna, Szemerédi Nikoletta, Loučková Anna, Kronusová Olga, Spengler Gabriella, Kaštánek Petr, Hajšlová Jana, Viktorová Jitka, and Lipov Jan

Subjects
Multidrug resistance, Herbs, Medicinal plants, Quorum sensing, Biofilm, Efflux pump inhibitors
Abstract

Our research is focused on adjuvants that inhibit the mechanism of antibiotic resistance or modulate bacterial virulence. Based on a preliminary screening of 52 European herbs, which commonly appear as part of tea blends or poultice. Six of them were selected for their ability to revert the resistant phenotype of nosocomial bacterial strains.

Published
2023

2. Indolo[2,3-e]benzazocines and indolo[2,3-f]benzazonines and their copper(II) complexes as microtubule destabilizing agents

Author

Wittmann Christopher, Dömötör Orsolya, Kuznetcova Irina, Spengler Gabriella, Reynisson Jóhannes, Holder Lauren, Miller Gavin J., Enyedy Éva Anna, Bai Ruoli, Hamel Ernest, and Vladimir Arion

Subjects
01.04. Kémiai tudományok, 01.06. Biológiai tudományok
Abstract

A series of four indolo[2,3-e]benzazocines HL1–HL4 and two indolo[2,3-f]benzazonines HL5–and HL6, as well as their respective copper(II) complexes 1–6 were synthesized and characterized by 1H and 13C NMR spectroscopy, ESI...

Published
2023

4. The Release of a Highly Cytotoxic Paullone Bearing a TEMPO Free Radical from the HSA Hydrogel: An EPR Spectroscopic Characterization

Author

Vesković, Ana, Nakarada, Đura, Vasiljević, Olga, Dobrov, Anatolie, Spengler, Gabriella, Enyedy, Éva A., Arion, Vladimir B., and Popović Bijelić, Ana

Subjects
spin labeling, paullones, Pharmaceutical Science, cytotoxic ligand, drug release, EPR spectroscopy and imaging, HSA hydrogel
Abstract

This study shows the potential of a thermally induced human serum albumin (HSA) hydrogel to serve as a drug depot for sustained release of a highly cytotoxic modified paullone ligand bearing a TEMPO free radical (HL). The binding of HL to HSA was studied by electron paramagnetic resonance (EPR) spectroscopy and imaging. The EPR protocol was also implemented for the study of matrix degradation, and ligand diffusion rate, in two additional spin-labeled hydrogels, containing 5-doxylstearate and 3-carbamoyl-proxyl. The results showed that the hydrogel is an efficient HL reservoir as it retained 60% of the ligand during 11 days of dialysis in physiological saline. Furthermore, upon incubation with Colo 205 human colon adenocarcinoma cells for 3 days, the HL/HSA hydrogel did not exhibit cytotoxic activity, demonstrating that it is also an efficient ligand depot in the presence of living cells. It was observed that the percentage of HL release is independent of its initial concentration in the hydrogel, suggesting that HSA possesses a specific binding site for the ligand, most likely Sudlow site 2, as predicted by molecular docking. The intrinsic property of albumin to bind and transport various substances, including hydrophobic drugs, may be fine-tuned by appropriate physical/chemical hydrogel preparation procedures, providing optimal drug delivery.

Published
2022
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5. Solution Equilibrium Studies on Salicylidene Aminoguanidine Schiff Base Metal Complexes: Impact of the Hybridization with L-Proline on Stability, Redox Activity and Cytotoxicity

Author

Dömötör, Orsolya, May, Nóra V., Gál, G. Tamás, Spengler, Gabriella, Dobrova, Aliona, Arion, Vladimir B., and Enyedy, Éva A.

Subjects
Proline, Organic Chemistry, Pharmaceutical Science, Crystallography, X-Ray, Ligands, aminoguanidine, anticancer, Ferric Compounds, Guanidines, Analytical Chemistry, stability constants, thiosemicarbazone, EPR spectroscopy, Coordination Complexes, Chemistry (miscellaneous), Drug Discovery, Humans, Molecular Medicine, Ferrous Compounds, Physical and Theoretical Chemistry, Oxidation-Reduction, Schiff Bases
Abstract

The proton dissociation processes of two tridentate salicylidene aminoguanidine Schiff bases (SISC, Pro-SISC-Me), the solution stability and electrochemical properties of their Cu(II), Fe(II) and Fe(III) complexes were characterized using pH-potentiometry, cyclic voltammetry and UV-visible, 1H NMR and electron paramagnetic resonance spectroscopic methods. The structure of the proline derivative (Pro-SISC-Me) was determined by X-ray crystallography. The conjugation of L-proline to the simplest salicylidene aminoguanidine Schiff base (SISC) increased the water solubility due to its zwitterionic structure in a wide pH range. The formation of mono complexes with both ligands was found in the case of Cu(II) and Fe(II), while bis complexes were also formed with Fe(III). In the complexes these tridentate ligands coordinate via the phenolato O, azomethine N and the amidine N, except the complex [Fe(III)L2]+ of Pro-SISC-Me in which the (O,N) donor atoms of the proline moiety are coordinated beside the phenolato O, confirmed by single crystal X-ray crystallographic analysis. This binding mode yielded a stronger Fe(III) preference for Pro-SISC-Me over Fe(II) in comparison to SISC. This finding is also reflected in the lower redox potential value of the iron-Pro-SISC-Me complexes. The ligands alone were not cytotoxic against human colon cancer cell lines, while complexation of SISC with Cu(II) resulted in moderate activity, unlike the case of its more hydrophilic counterpart.

Published
2022
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7. Selenocompounds evaluation as novel MDR-reversing anticancer agents

Author

Domínguez-Álvarez, Enrique, González-Prádena, Ana, Rácz, Bálint, Szemerédi, Nikoletta, Malgorzata, Mar, and Spengler, Gabriella

Abstract

Nine symmetrical selenocompounds, comprising 6 selenodiesters and 3 selenotriesters, were synthesized and evaluated novel anticancer and MDR-reversing agents. According to results, the most active ones showed submicromolar IC50 values in cancer cells, as well as ability to inhibit efflux pumps. Thus, there are novel promising anticancer compounds.

Published
2021

12. Coumarin-Based Triapine Derivatives and Their Copper(II) Complexes: Synthesis, Cytotoxicity and mR2 RNR Inhibition Activity

Author

Stepanenko, Iryna, Babak, Maria V., Spengler, Gabriella, Hammerstad, Marta, Popovic-Bijelic, Ana, Shova, Sergiu, Büchel, Gabriel E., Darvasiova, Denisa, Rapta, Peter, and Arion, Vladimir B.

Subjects
Models, Molecular, antiproliferative activity, Molecular Structure, Pyridines, thiosemicarbazones, Antineoplastic Agents, Crystallography, X-Ray, Microbiology, coumarin, QR1-502, Article, Mice, Structure-Activity Relationship, electrochemistry, Coordination Complexes, Coumarins, Cell Line, Tumor, triapine, Animals, Humans, tyrosyl radical reduction, copper(II), Copper, Cell Proliferation
Abstract

A series of thiosemicarbazone-coumarin hybrids (HL1-HL3 and H2L4) has been synthesised in 12 steps and used for the preparation of mono- and dinuclear copper(II) complexes, namely Cu(HL1)Cl2 (1), Cu(HL2)Cl2 (2), Cu(HL3)Cl2 (3) and Cu2(H2L4)Cl4 (4), isolated in hydrated or solvated forms. Both the organic hybrids and their copper(II) and dicopper(II) complexes were comprehensively characterised by analytical and spectroscopic techniques, i.e., elemental analysis, ESI mass spectrometry, 1D and 2D NMR, IR and UV–vis spectroscopies, cyclic voltammetry (CV) and spectroelectrochemistry (SEC). Re-crystallisation of 1 from methanol afforded single crystals of copper(II) complex with monoanionic ligand Cu(L1)Cl, which could be studied by single crystal X-ray diffraction (SC-XRD). The prepared copper(II) complexes and their metal-free ligands revealed antiproliferative activity against highly resistant cancer cell lines, including triple negative breast cancer cells MDA-MB-231, sensitive COLO-205 and multidrug resistant COLO-320 colorectal adenocarcinoma cell lines, as well as in healthy human lung fibroblasts MRC-5 and compared to those for triapine and doxorubicin. In addition, their ability to reduce the tyrosyl radical in mouse R2 protein of ribonucleotide reductase has been ascertained by EPR spectroscopy and the results were compared with those for triapine.

Published
2021

15. Efflux pump inhibition by symmetric selenoesters on colon adenocarcinoma cells

Author

Rácz, B., Kincses, Annamária, Benito-Lama, Miguel, González-Prádena, Ana, Domínguez-Álvarez, Enrique, and Spengler, Gabriella

Abstract

The development of resistance to chemotherapy in tumour cells is often due to altered membrane transport, such as the overexpression of ABCB1 (P-glycoprotein). Previously, selenium and its derivatives have been reported as antiproliferative, cytotoxic compounds that can also reduce drug resistance in tumour cells, trigger apoptotic events and enhance synergistically the anticancer activity of chemotherapy drugs such as doxorubicin. This work aims to elucidate how the symmetrical selenoesters exert their anticancer effect on sensitive and resistant human colon adenocarcinoma cells expressing ABCB1 protein. MTT assay was applied to assess both the antiproliferative and cytotoxic effects of the compounds on sensitive and resistant colon adenocarcinoma and normal embryonic lung fibroblast cells. A flow cytometry based assay which determines the accumulation of rhodamine 123 was used to assess the efflux pump inhibitory activity of the tested selenoesters. Finally, annexin V-FITC staining was used to determine the apoptosis-inducing effect of the most promising derivatives. Furthermore, the interaction of the compounds with doxorubicin was assessed by checkerboard combination assay and the type of interaction was calculated by Calcusyn software. Methyl ketone-containing compounds (EDAG-1, -5, -8) showed the most potent antiproliferative and cytotoxic effects. Out of them, EDAG-5 was the one that had the most synergistic interaction with doxorubicin. On the other hand, the methyloxycarbonylmethyl- and the methylcyano selenoesters had a very low cytotoxic activity on the normal MRC-5 fibroblast cell line. Methyl ketone- and methylcyano-selenoesters (EDAG-7, -10, 11) were more potent ABCB1 inhibitors than the reference compound verapamil. Finally, a methyl ketone selenoester (EDAG-1) was an effective inducer of apoptosis in the resistant Colo 320 cell line. The biological activities observed are comparable or higher than the ones determined in previous works. Thus, it seems that the inclusion of symmetric centres in these selenocompounds may favour (or at least retain) the biological activity. Based on these results, it can be concluded that these compounds (or derivatives containing these symmetrical elements) could be interesting scaffolds for future research in medicinal chemistry.

Published
2020

16. Dually Acting Nonclassical 1,4-Dihydropyridines Promote the Anti-Tuberculosis (Tb) Activities of Clofazimine

Author

Lentz, Fabian, Reiling, Norbert, Spengler, Gabriella, Kincses, Annamária, Csonka, Andrea, Molnár, Joseph, and Hilgeroth, Andreas

Subjects
Dihydropyridines, Molecular Structure, synthesis, Communication, Spectrum Analysis, structure–activity, Antitubercular Agents, Drug Synergism, Microbial Sensitivity Tests, Mycobacterium tuberculosis, substituent, Clofazimine, inhibition, lcsh:QD241-441, antibacterial activity, lcsh:Organic chemistry, ATP Binding Cassette Transporter, Subfamily B, Member 1
Abstract

The number of effective antituberculotic drugs is strongly limited to four first-line drugs in standard therapy. In case of resistances second-line antibiotics are used with a poor efficacy and tolerability. Therefore, novel antituberculotic drugs are urgently needed. We synthesized novel nonclassical 1,4-dihydropyridines and evaluated their antituberculotic properties depending on substituent effects. Preferred substituents could be identified. As related classical 1,4-dihydropyridines are known as inhibitors of the transmembrane efflux pump ABCB1 in cancer cells, we wondered whether a use of our compounds may be of favour to enhance the antituberculotic drug efficacy of the second-line antituberculotic drug clofazimine, which is a known substrate of ABCB1 by a suggested inhibition of a corresponding efflux pump in Mycobacterium tuberculosis (Mtb). For this, we determined the ABCB1 inhibiting properties of our compounds in a mouse T-lymphoma cell line model and then evaluated the drug-enhancing properties of selected compounds in a co-application with clofazimine in our Mtb strain. We identified novel enhancers of clofazimine toxicity which could prevent clofazimine resistance development mediated by an efflux pump activity.

Published
2019

17. Efflux pumps as targets to reverse multidrug resistance in bacteria

Author

Spengler, Gabriella, Annamária, Kincses, Márió, Gajdács, Amaral, Leonard, Unidade de Parasitologia e Microbiologia Médicas (UPMM), and Centro de Malária e outras Doenças Tropicais (CMDT)

Subjects
RND pump, Efflux pump inhibitor (EPI), SDG 3 - Good Health and Well-being, Proton motive force, ABC-transporter, Multidrug efflux pump, Multidrug resistance
Abstract

Multidrug resistance (MDR) has appeared in response to selective pressures resulting from the incorrect use of antibiotics and other antimicrobials. This inappropriate application and mismanagement of antibiotics have led to serious problems in the therapy of infectious diseases. Bacteria can develop resistance by various mechanisms and one of the most important factors resulting in MDR is efflux pump-mediated resistance. Because of the importance of the efflux-related multidrug resistance the development of new therapeutic approaches aiming to inhibit bacterial efflux pumps is a promising way to combat bacteria having over-expressed MDR efflux systems. The definition of an efflux pump inhibitor (EPI) includes the ability to render the bacterium increasingly more sensitive to a given antibiotic or even reverse the multidrug resistant phenotype. In the recent years numerous EPIs have been developed, although so far their clinical application has not yet been achieved due to their in vivo toxicity and side effects. In this review, we aim to give a short overview of efflux mediated resistance in bacteria, EPI compounds of plant and synthetic origin, and the possible methods to investigate and screen EPI compounds in bacterial systems. publishersversion published

Published
2017

18. Multidrug resistance reversal by 3-formylchromones in human colon cancer and human mdr1 gene-transfected mouse lymphoma cells

Author

Barath, Zoltan, Radics, Rita, Spengler, Gabriella, Ocsovszki, Imre, Shah, Anamik, and Molnar, Jozsef

Subjects
Formylchromones, multidrug resistance-reversing effect
Abstract

Several new 3-formylchromone derivatives proved to be modifiers of multidrug resistance in mouse lymphoma cells and in human Colo320 colon cancer cells. There is apparently a structure-activity relationship between the antiproliferative multidrug resistance-reversing effect and the chemical structure of the 3-formylchromones. The total polar surface areas and the ground state dipole moments of the molecules are presumed to play a key role in the multidrug resistance-reversing effect. The log P values can provide an adequate explanation for the selective cytotoxicity against cancer cells., 5p.

Published
2006

19. Biological activity of well defined hydantoin derivatives on efflux pump systems of bacteria and cancer cells

Author

EVARISTO, Miguel do Rosário and SPENGLER, Gabriella

Subjects
Terapêutica, Bactérias, Ciências Médicas [Domínio/Área Científica], Biologia molecular, Cancro, Efluxo
Abstract

A multi-resistência a antibióticos e medicamentos usados em quimioterapia é um dos grandes problemas com os quais as instituições de saúde se debatem hoje em dia. A acção provocada por bombas de efluxo é uma das suas causas. Estas bombas têm uma importância fundamental, uma vez que, ao expelirem todo o tipo de tóxicos para o exterior das células, também expelem medicamentos, fazendo com que estes não tenham o efeito desejado dentro delas. As bombas de efluxo são transportadores que se encontram nas membranas de todo o tipo de células. Existem dois grandes tipos de bombas de efluxo: as primárias e as secundárias. As primeiras conferem multi-resistência principalmente em células eucariotas, como as células do cancro em humanos, tendo como função a mediação da repulsa de substâncias tóxicas por intermédio da hidrólise de ATP. A primeira a ser descoberta e mais estudada destas bombas foi a ABCB1 que é o gene que codifica a glicoproteína-P (P de permeabilidade). Enquanto as secundárias, que são a maior fonte de multi-resistência em bactérias, promovem a extrusão de substâncias tóxicas através da força motriz de protões. Neste tipo de bombas são conhecidas quatro famílias principais, das quais uma das mais importantes é a superfamília RND, uma vez que inclui a bomba AcrAB-TolC, que é muito importante no metabolismo xenobiótico de bactérias Gramnegativas, nomeadamente a E.coli. Com o objectivo de reverter a multi-resistência, tanto em células eucariotas como procariotas, têm-se desenvolvido estratégias de combate que envolvem a descoberta de substâncias que inibam as bombas de efluxo. Assim sendo, ao longo dos tempos têm sido descobertas variadas substâncias que cumprem este objectivo. É o caso, por exemplo, dos derivados de fluoroquinolonas usados como inibidores de bombas de efluxo em bactérias ou do Tamoxifen, utilizado na terapia de pacientes com cancro da mama. Um dos grupos de substâncias estudados para o desenvolvimento de possíveis compostos que actuem como reversores de multi-resistência são os compostos derivados de hidantoínas. Estes, são conhecidos por possuírem uma grande variedade de propriedades bioquímicas e farmacológicas, sendo portanto usados para tratarem algumas doenças em humanos, como a epilepsia. Nestes, estão englobados compostos com actividade anti-convulsão que constitui a sua grande mais-valia e, dependente da substituição no anel que os constitui, uma grande variedade de outras propriedades farmacológicas como a anti-fungica, a anti-arritmica, a anti-viral, a anti-diabética ou por exemplo a antagonização de determinados receptores, como os da serotonina. Apesar de pouco usados em estudos experimentais para desenvolver substâncias anti-carcinogénicas, existem alguns estudos com este efeito. Objectivos: O presente projecto envolve o estudo de bombas de efluxo primárias e secundárias, em células eucariotas e procariotas, respectivamente. Em bactérias, foram usados quatro modelos experimentais: Staphylococcus aureus ATCC 25923, Enterococcus faecalis ATCC 29212, E. coli AG 100 e Salmonella Enteritidis NCTC 13349. Em células de cancro foram usadas, células T de linfoma de rato parentais e células T de linfoma de rato transfectadas com o gene humano MDR-1. O principal objectivo deste estudo foi a pesquisa de novos moduladores de bombas de efluxo presentes em bactérias e células do cancro, tentando assim contribuir para o desenvolvimento de novos agentes farmacológicos que consigam reverter a multi-resistência a medicamentos. Assim sendo foram testados trinta compostos derivados de hidantoínas: SZ-2, SZ-7, LL-9, BS-1, JH-63, MN-3, TD-7k, GG-5k, P3, P7, P10, P11, RW-15b, AD-26, RW-13, AD-29, KF-2, PDPH-3, Mor-1, KK-XV, Thioam-1, JHF-1, JHC-2, JHP-1, Fur-2, GL-1, GL-7, GL-14, GL-16, GL-18. Como forma de atingir estes objectivos, a actividade biológica dos trinta compostos derivados de hidantoínas foi avaliada nas quatro estirpes de bactérias da seguinte forma: foram determinadas as concentrações mínimas inibitórias dos trinta compostos como forma de definir as concentrações em que os compostos seriam utilizados. Os compostos foram posteriormente testadas com um método fluorométrico de acumulação de brometo de etídeo, que é um substrato comum em bombas de efluxo bacterianas, desenvolvido por Viveiros et al. A actividade biológica dos compostos derivados de hidantoínas nas células de cancro foi demonstrada por diferentes métodos. O efeito anti-proliferativo e citotóxico dos trinta compostos foi avaliado nas células T de linfoma de rato transfectadas com o gene humano MDR-1 pelo método de thiazolyl de tetrazólio (MTT). Como o brometo de etídeo também é expelido pelos transportadores ABC, estes compostos foram posteriormente testados com um método fluorométrico de acumulação de brometo de etídeo desenvolvido por Spengler et al nos dois diferentes tipos de células eucariotas. Resultados: A maioria dos compostos derivados de hidantoínas foi eficaz na modulação de bombas de efluxo, nas duas estirpes de bactérias Gram-negativas e nos dois diferentes tipos de células T de linfoma. Em contraste com estes resultados, nas duas estirpes de células Gram-positivas, a maioria dos compostos tiveram pouco efeito na inibição de bombas de efluxo ou até nenhum, em muitos dos casos. De uma maneira geral os melhores compostos nas diferentes estirpes de bactérias foram: Thioam-1, SZ-2, P3, Rw-15b, AD-26, AD-29, GL-18, GL-7, KF-2, SZ-7, MN-3, GL-16 e GL- 14. Foram portanto estes os compostos que provocaram maior acumulação de brometo de etídeo, inibindo assim com maior eficácia as bombas de efluxo. No presente estudo, a maioria dos compostos conseguiu inibir a resistência provocada pela bomba de efluxo ABCB1, tanto nas células parentais bem como nas células que sobre-expressam esta bomba, causando a acumulação de brometo de etídeo dentro das células. As células que sobreexpressam a bomba ABCB1 foram posteriormente testadas com citometria de fluxo que é a técnica padrão para pesquisa de inibidores de bombas de efluxo. Os compostos que foram mais efectivos na inibição da bomba ABCB1, causando assim maior acumulação de brometo de etídeo nas células que sobre-expressam esta bomba foram: PDPH-3, GL-7, KK-XV, AD-29, Thioam-1, SZ-7, KF-2, MN-3, RW-13, LL-9, P3, AD-26, JH-63 e RW- 15b. Este facto não corroborou totalmente os resultados da citometria de fluxo uma vez que os moduladores que provocaram maior inibição da bomba ABCB1 foram o MN-3, JH-63 e o BS-1, sendo que o último não foi seleccionado como um bom composto usando o método fluorométrico de acumulação de brometo de etídeo. Conclusão: Os compostos derivados de hidantoínas testados tiveram maior efeito nas estirpes de bactérias Gram-negativas do que nas Gram-positivas. Relativamente às células eucariotas, as estruturas mais activas apresentam substituintes aromáticos bem como alguns fragmentos aminicos terciários.

Published
2010

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