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1.

001-es BibID:BIBFORM110272
035-os BibID:(cikkazonosító)1477 (WoS)000930056200001 (Scopus)85147892443
Első szerző:Bíró Linda (vegyész)
Cím:Interaction between [(eta(6)-p-cym)M(H2O)(3)](2+) (M-II = Ru, Os) or [(eta(5)-Cp*)M(H2O)(3)](2+) (M-III = Rh, Ir) and Phosphonate Derivatives of Iminodiacetic Acid: A Solution Equilibrium and DFT Study / Linda Bíró, Botond Tóth, Norbert Lihi, Etelka Farkas, Péter Buglyó
Dátum:2023
ISSN:1420-3049
Megjegyzések:The pH-dependent binding strengths and modes of the organometallic [(eta(6)-p-cym)M(H2O)(3)](2+) (M-II = Ru, Os; p-cym = 1-methyl-4-isopropylbenzene) or [(eta(5)-Cp*)M(H2O)(3)](2+) (M-III = Rh, Ir; Cp* = pentamethylcyclopentadienyl anion) cations towards iminodiacetic acid (H(2)Ida) and its biorelevant mono- and diphosphonate derivatives N-(phosphonomethyl)-glycine (H(3)IdaP) and iminodi(methylphosphonic acid) (H(4)Ida2P) was studied in an aqueous solution. The results showed that all three of the ligands form 1:1 complexes via the tridentate (O,N,O) donor set, for which the binding mode was further corroborated by the DFT method. Although with IdaP(3-) and Ida2P(4-) in mono- and bis-protonated species, where H+ might also be located at the non-coordinating N atom, the theoretical calculations revealed the protonation of the phosphonate group(s) and the tridentate coordination of the phosphonate ligands. The replacement of one carboxylate in Ida(2-) by a phosphonate group (IdaP(3-)) resulted in a significant increase in the stability of the metal complexes; however, this increase vanished with Ida2P(4-), which was most likely due to some steric hindrance upon the coordination of the second large phosphonate group to form (5 + 5) joined chelates. In the phosphonate-containing systems, the neutral 1:1 complexes are the major species at pH 7.4 in the millimolar concentration range that is supported by both NMR and ESI-TOF-MS.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
IDA-based
phosphonates
organoruthenium
organorhodium
solution equilibrium
complex
Megjelenés:Molecules. - 28 : 3 (2023), p. 1-17-. -
További szerzők:Tóth Botond Lihi Norbert (1990-) (vegyész) Farkas Etelka (1948-) (vegyész) Buglyó Péter (1965-) (vegyész)
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2.

001-es BibID:BIBFORM107731
035-os BibID:(cikkazonosító)4667 (WOS)000831832500001 (Scopus)85135135260
Első szerző:Bíró Linda (vegyész)
Cím:Pd(II) Binding Strength of a Novel Ambidentate Dipeptide-Hydroxypyridinonate Ligand : A Solution Equilibrium Study / Linda Bíró, András Ozsváth, Réka Kapitány, Péter Buglyó
Dátum:2022
ISSN:1420-3049
Megjegyzések:A novel ambidentate dipeptide conjugate (H(L1)) containing N-donor atoms of the peptide part and an (O,O) chelate at the hydroxypyridinone (HP) ring is synthesized and characterized. It is hoped that this chelating ligand can be useful to obtain multitargeted Co(III)/Pt(II) dinuclear complexes with anticancer potential. The Pd(II) (as a Pt(II) model but with faster ligand exchange reactions) binding strength of the ligand was studied in an aqueous solution with the combined use of pH-potentiometry and NMR. In an equimolar solution, (L1)(-) was found to bind Pd(II) via the terminal amino and increasing number of peptide nitrogens of the peptide backbone over a wide pH range. At a 2:1 Pd(II) to ligand ratio, the presence of [Pd2H-x(L1)] (x = 1-4) species, with high stability and with the coordination of the (O,O) chelating set of the ligand, was detected. The reaction of H(L1) with [Co(tren)](3+) (tren = tris(2-aminoethyl)amine) indicated the exclusive binding of (L1)(-) via its (O,O) donor atoms to the metal unit, while treatment of the resulting Co-complex with Pd(II) afforded the formation of a Co/Pd heterobimetallic complex in solution with an (NH2, N-amide) coordination of Pd(II). Shortening the peptide backbone in H(L1) by one peptide unit compared to the structurally similar ambidentate chelator consisting of three peptide bonds resulted in the slightly more favorable formation of the N-coordinated Pd(II) species, allowing the tailoring of the coordination properties.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
multitargeted
palladium
anticancer
speciation
stability constant
ambidentate
hydroxypyridinone
Megjelenés:Molecules. - 27 : 14 (2022), p. 1-13. -
További szerzők:Ozsváth András (1992-) (vegyész) Kapitány Réka Buglyó Péter (1965-) (vegyész)
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3.

001-es BibID:BIBFORM100515
035-os BibID:(cikkazonosító)669 (WoS)000760234200001 (Scopus)85123114917
Első szerző:Bíró Linda (vegyész)
Cím:Diversity in the Interaction of Amino Acid- and Peptide-Based Hydroxamic Acids with Some Platinum Group Metals in Solution / Bíró Linda, Buglyó Péter, Farkas Etelka
Dátum:2022
ISSN:1420-3049
Megjegyzések:Complexes that incorporate both ligand(s) and metal(s) exhibiting cytotoxic activity can especially be interesting to develop multifunctional drug molecules with desired activities. In this review, the limited number of solution results collected in our laboratory on the complexes of Pd(II) and two other platinum group metals-the half-sandwich type, [(6-p-cym)Ru(H2O)3]2+, and [(5-Cp*)Rh(H2O)3]2+-with hydroxamic acid derivatives of three amino acids, two imidazole analogues, and four small peptides are summarized and evaluated. Unlike the limited number of coordination sites of these metal ions (four and three for Pd(II) and the organometallic cations, respectively), the ligands discussed here offer a relatively high number of donor atoms as well as variation in their position within the ligands, resulting in a large versatility of the likely coordination modes. The review, besides presenting the solution equilibrium results, also discusses the main factors, such as (N,N) versus (O,O) chelate; size of chelate; amino-N versus imidazole-N; primary versus secondary hydroxamic function; differences between hydrolytic ability of the metal ions studied; and hydrolysis of the coordinated peptide hydroxamic acids in their Pd(II) complexes, which all determine the coordination modes present in the complexes formed in measurable concentrations in these systems. The options for the quantitative evaluation of metal binding effectivity and selectivity of the various ligands and the comparison with each other by using solution equilibrium data are also discussed.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Megjelenés:Molecules. - 27 : 3 (2022), p. 1-27. -
További szerzők:Buglyó Péter (1965-) (vegyész) Farkas Etelka (1948-) (vegyész)
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Intézményi repozitóriumban (DEA) tárolt változat
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4.

001-es BibID:BIBFORM100915
035-os BibID:(cikkazonosító)542 (WoS)000615421600001 (Scopus)85100478135
Első szerző:Illyés Tünde Zita (kémia-fizika szakos tanár)
Cím:Synthesis of Tetravalent Thio- and Selenogalactoside-Presenting Galactoclusters and Their Interactions with Bacterial Lectin PA-IL from Pseudomonas aeruginosa / Tünde Zita Illyés, Lenka Malinovská, Erzsébet Rőth, Boglárka Tóth, Bence Farkas, Marek Korsák, Michaela Wimmerová, Katalin E. Kövér, Magdolna Csávás
Dátum:2021
ISSN:1420-3049
Megjegyzések:Synthesis of tetravalent thio- and selenogalactopyranoside-containing glycoclusters using azide-alkyne click strategy is presented. Prepared compounds are potential ligands of Pseudomonas aeruginosa lectin PA-IL. P. aeruginosa is an opportunistic human pathogen associated with cystic fibrosis, and PA-IL is one of its virulence factors. The interactions of PA-IL and tetravalent glycoconjugates were investigated using hemagglutination inhibition assay and compared with mono- and divalent galactosides (propargyl 1-thio- and 1-seleno-?-d-galactopyranoside, digalactosyl diselenide and digalactosyl disulfide). The lectin-carbohydrate interactions were also studied by saturation transfer difference NMR technique. Both thio- and seleno-tetravalent glycoconjugates were able to inhibit PA-IL significantly better than simple d-galactose or their intermediate compounds from the synthesis.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
selenoglycosides
galactoclusters
Pseudomonas aeruginosa
PA-IL lectin
multivalency
Megjelenés:Molecules. - 26 : 3 (2021), p. 1-11. -
További szerzők:Malinovská, Lenka Rőth Erzsébet (1957-) (vegyész) Tóth Boglárka Farkas Bence Korsák, Marek Wimmerová, Michaela Kövér Katalin, E. (1956-2023) (vegyész) Csávás Magdolna (1977-) (szénhidrátkémikus, vegyész)
Pályázati támogatás:K119509
OTKA
K128368
OTKA
GINOP-2.3.2-15-2016-00008
GINOP
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Intézményi repozitóriumban (DEA) tárolt változat
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5.

001-es BibID:BIBFORM110065
035-os BibID:(cikkazonosító)3058 (Scopus)85152786486 (WoS)000969830000001
Első szerző:Kacsir István (vegyész)
Cím:Half-sandwich type platinum-group metal complexes of C-Glucosaminyl azines : syntheses, antineoplastic and antimicrobial activities / Kacsir I., Sipos A., Major E., Bajusz N., Bényei A., Buglyó P., Somsák L., Kardos G., Bai P., Bokor É.
Dátum:2023
ISSN:1420-3049
Tárgyszavak:Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Megjelenés:Molecules. - 28 : 7 (2023), p. 1-55. -
További szerzők:Sipos Adrienn (1984-) (biológus, biotechnológus) Major Evelin (1992-) Bajusz Nikolett Bényei Attila (1962-) (vegyész) Buglyó Péter (1965-) (vegyész) Somsák László (1954-) (vegyész) Kardos Gábor (1974-) (szakorvos, klinikai mikrobiológus) Bai Péter (1976-) (biokémikus) Bokor Éva (1982-) (vegyész)
Pályázati támogatás:TKP2020-IKA-04
Egyéb
TKP2021-EGA-19
Egyéb
TKP2021-EGA-20
Egyéb
Post-Covid2021-33
Egyéb
Internet cím:Intézményi repozitóriumban (DEA) tárolt változat
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6.

001-es BibID:BIBFORM098615
035-os BibID:(cikkazonosító)5902 (WoS)000706517100001 (Scopus)85116118060
Első szerző:Nagy Cynthia (1994-)
Cím:Development of an In-Line Enzyme Reactor Integrated into a Capillary Electrophoresis System / Nagy Cynthia, Szabo Ruben, Gaspar Attila
Dátum:2021
ISSN:1420-3049
Megjegyzések:The goal of this paper was to develop an in-line immobilized enzyme reactor (IMER) integrated into a capillary electrophoresis platform. In our research, we created the IMER by adsorbing trypsin onto the inner surface of a capillary in a short section. Enzyme immobilization was possible due to the electrostatic attraction between the oppositely charged fused silica capillary surface and trypsin. The reactor was formed by simply injecting and removing trypsin solution from the capillary inlet (similar to 1-2 cms). We investigated the factors affecting the efficiency of the reactor. The main advantages of the proposed method are the fast, cheap, and easy formation of an IMER with in-line protein digestion capability. Human tear samples were used to test the efficiency of the digestion in the microreactor.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Megjelenés:Molecules. - 26 : 19 (2021), p. 1-14. -
További szerzők:Szabó Ruben (1998-) Gáspár Attila (1970-) (vegyész, kémikus)
Pályázati támogatás:K127931
Egyéb
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Intézményi repozitóriumban (DEA) tárolt változat
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7.

001-es BibID:BIBFORM099415
035-os BibID:(cikkazonosító)3586 (WoS)000666566100001 (Scopus)85108329799
Első szerző:Nagy Sándor (vegyész)
Cím:Donor Atom Preference of Organoruthenium and Organorhodium Cations on the Interaction with Novel Ambidentate (N,N) and (O,O) Chelating Ligands in Aqueous Solution / Nagy Sándor, Ozsváth András, Bényei Attila Cs., Farkas Etelka, Buglyó Péter
Dátum:2021
ISSN:1420-3049
Megjegyzések:Two novel, pyridinone-based chelating ligands containing separated (O,O) and (Namino,Nhet) chelating sets (Namino = secondary amine; Nhet = pyrrole N for H(L3) (1-(3-(((1H-pyrrole-2-yl)methyl)-amino)propyl)-3-hydroxy-2-methylpyridin-4(1H)-one) or pyridine N for H(L5) (3-hydroxy-2-methyl-1-(3-((pyridin-2-ylmethyl)amino)propyl)pyridin-4(1H)-one)) were synthesized via reduction of the appropriate imines. Their proton dissociation processes were explored, and the molecular structures of two synthons were assessed by X-ray crystallography. These ambidentate chelating ligands are intended to develop Co(III)/PGM (PGM = platinum group metal) heterobimetallic multitargeted complexes with anticancer potential. To explore their metal ion binding ability, the interaction with Pd(II), [(?6-p-cym)Ru]2+ and [(?5-Cp*)Rh]2+ (p-cym = 1-methyl-4-isopropylbenzene, Cp* = pentamethyl-cyclopentadienyl anion) cations was studied in aqueous solution with the combined use of pH-potentiometry, NMR and HR ESI-MS. In general, organorhodium was found to form more labile complexes over ruthenium, while complexation of the (N,N) chelating set was slower than the processes of the pyridinone unit with (O,O) coordination. Formation of the organoruthenium complexes starts at lower pH (higher thermodynamic stabilities of the corresponding complexes) than for [(?5-Cp*)Rh]2+ but, due to the higher affinity of [?6-p-cym)Ru]2+ towards hydrolysis, the complexed ligands are capable of competing with hydroxide ion in a lesser extent than for the rhodium systems. As a result, under biologically relevant conditions, the rhodium binding effectivity of the ligands becomes comparable or even slightly higher than their effectivity towards ruthenium. Our results indicate that H(L3) is a less efficient (N,N) chelator for these metal ions than H(L5). Similarly, due to the relative effectivity of the (O,O) and (N,N) chelates at a 1:1 metal-ion-to-ligand ratio, H(L5) coordinates in a (N,N) manner to both cations in the whole pH range studied while, for H(L3), the complexation starts with (O,O) coordination. At a 2:1 metal-ion-to-ligand ratio, H(L3) cannot hinder the intensive hydrolysis of the second metal ion, although a small amount of 2:1 complex with [(?5-Cp*)Rh]2+ can also be detected.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
ruténium
ródium
komplex
piridinon
maltol
Megjelenés:Molecules. - 26 : 12 (2021), p. 1-23. -
További szerzők:Ozsváth András (1992-) (vegyész) Bényei Attila (1962-) (vegyész) Farkas Etelka (1948-) (vegyész) Buglyó Péter (1965-) (vegyész)
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8.

001-es BibID:BIBFORM074773
035-os BibID:(WoS)000447365100107 (Scopus)85052664471
Első szerző:Nagy Tamás Milán (vegyész, nmr)
Cím:Photochemical and structural studies on cyclic peptide models / Tamás Milán Nagy, Krisztina Knapp, Eszter Illyés, István Timári, Gitta Schlosser, Gabriella Csík, Attila Borics, Zsuzsa Majer, Katalin E. Kövér
Dátum:2018
ISSN:1420-3049
Megjegyzések:UV irradiation has a significant impact on the structure and function of proteins that is supposed to be in relationship with the tryptophan-mediated photolysis of disulfide bonds. To investigate the correlation between the photoexcitation of Trp residues in polypeptides and the associated reduction of disulfide bridges, a series of small, cyclic oligopeptide models were analyzed in this work. Average distances between the aromatic side chains and the disulfide bridge were determined following molecular mechanics (MM) geometry optimizations. In this way, the possibility of cation-pi interactions was also investigated. Molecular mechanics calculations revealed that the shortest distance between the side chain of the Trp residues and the disulfide bridge is approximately 5 A in the cyclic pentapeptide models. Based on this, three tryptophan-containing cyclopeptide models were synthesized and analyzed by NMR spectroscopy. Experimental data and detailed molecular dynamics (MD) simulations were in good agreement with MM geometry calculations. Selected model peptides were subjected to photolytic degradation to study the correlation of structural features and the photolytic cleavage of disulfide bonds in solution. Formation of free sulfhydryl groups upon illumination with near UV light was monitored by fluorescence spectroscopy after chemical derivatization with 7-diethylamino-3-(4-maleimidophenyl)-4-methylcoumarin (CPM) and mass spectrometry. LC-MS measurements indicated the presence of multiple photooxidation products (e.g. dimers, multimers and other oxidated products), suggesting that besides the photolysis of disulfide bonds secondary photolytic processes take place.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
cyclopeptides
UV-irradiation
photolysis
disulfide bridges
NMR
MD
Megjelenés:Molecules. - 23 : 9 (2018), p. 1-20. -
További szerzők:Knapp Krisztina Illyés Eszter Timári István (1989-) (vegyész) Schlosser Gitta Csík Gabriella Borics Attila Májer Zsuzsa Kövér Katalin, E. (1956-2023) (vegyész)
Pályázati támogatás:GINOP-2.3.2-15-2016-00008
GINOP
GINOP-2.3.3-15-2016-00004
GINOP
NN 128368
OTKA
Internet cím:Intézményi repozitóriumban (DEA) tárolt változat
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Szerző által megadott URL
Borító:

9.

001-es BibID:BIBFORM098762
035-os BibID:(cikkazonosító)3632 (WoS)000667382100001 (Scopus)85110387344
Első szerző:Najóczki Ferenc
Cím:Synthesis and Characterization of 1,10-Phenanthroline-mono-N-oxides / Najóczki Ferenc, Szabó Mária, Lihi Norbert, Udvardy Antal, Fábián István
Dátum:2021
ISSN:1420-3049
Megjegyzések:N-oxides of N-heteroaromatic compounds find widespread applications in various fields of chemistry. Although the strictly planar aromatic structure of 1,10-phenanthroline (phen) is expected to induce unique features of the corresponding N-oxides, so far the potential of these compounds has not been explored. In fact, appropriate procedure has not been reported for synthesizing these derivatives of phen. Now, we provide a straightforward method for the synthesis of a series of mono-N-oxides of 1,10-phenanthrolines. The parent compounds were oxidized by a green oxidant, peroxomonosulfate ion in acidic aqueous solution. The products were obtained in high quality and at good to excellent yields. A systematic study reveals a clear-cut correlation between the basicity of the compounds and the electronic effects of the substituents on the aromatic ring. The UV spectra of these compounds were predicted by DFT calculations at the TD-DFT/TPSSh/def2-TZVP level of theory.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
density functional calculation
N-oxide; oxidation
peroxomonosulfate ion
X-ray diffraction
Megjelenés:Molecules. - 26 : 12 (2021), p. 1-19. -
További szerzők:Szabó Mária (1991-) (vegyész) Lihi Norbert (1990-) (vegyész) Udvardy Antal (1981-) (vegyész) Fábián István (1956-) (vegyész)
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Intézményi repozitóriumban (DEA) tárolt változat
Borító:

10.

001-es BibID:BIBFORM087177
035-os BibID:(cikkazonosító)3941 (WoS)000498055500130 (Scopus)85074330646
Első szerző:Ozsváth András (vegyész)
Cím:Trends and Exceptions in the Interaction of Hydroxamic Acid Derivatives of Common Di- and Tripeptides with Some 3d and 4d Metal Ions in Aqueous Solution / András Ozsváth, Linda Bíró, Eszter Márta Nagy, Péter Buglyó, Daniele Sanna, Etelka Farkas
Dátum:2019
ISSN:1420-3049
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Megjelenés:Molecules. - 24 : 21 (2019), p. 1-25. -
További szerzők:Bíró Linda (1985-) (vegyész) Nagy Eszter Márta (1976-) (vegyész) Buglyó Péter (1965-) (vegyész) Sanna, Daniele (1956-) (vegyész) Farkas Etelka (1948-) (vegyész)
Pályázati támogatás:GINOP-2.3.2-15-2016-00008
GINOP
OTKA K112317
OTKA
Internet cím:DOI
Intézményi repozitóriumban (DEA) tárolt változat
Borító:

11.

001-es BibID:BIBFORM101155
035-os BibID:(cikkazonosító)1966 (Wos)000774452400001 (Scopus)85127134499
Első szerző:Santos, M. Amélia
Cím:Hydroxypyridinone-Based Metal Chelators towards Ecotoxicity: Remediation and Biological Mechanisms / M. Amélia Santos, Anna Irto, Péter Buglyó, Sílvia Chaves
Dátum:2022
ISSN:1420-3049
Megjegyzések:Hydroxypyridinones (HPs) are recognized as excellent chemical tools for engineering a diversity of metal chelating agents, with high affinity for hard metal ions, exhibiting a broad range of activities and applications, namely in medical, biological and environmental contexts. They are easily made and functionalizable towards the tuning of their pharmacokinetic properties or the improving of their metal complex thermodynamic stabilities. In this review, an analysis of the recently published works on hydroxypyridinone-based ligands, that have been mostly addressed for environmental applications, namely for remediation of hard metal ion ecotoxicity in living beings and other biological matrices is carried out. In particular, herein the most recent developments in the design of new chelating systems, from bidentate mono-HP to polydentate multi-HP derivatives, with a structural diversity of soluble or solid-supported backbones are outlined. Along with the ligand design, an analysis of the relationship between their structures and activities is presented and discussed, namely associated with the metal affinity and the thermodynamic stability of the corresponding metal complexes.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Megjelenés:Molecules. - 27 : 6 (2022), p. 1-26. -
További szerzők:Irto, Anna Buglyó Péter (1965-) (vegyész) Chaves, Silvia
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Borító:

12.

001-es BibID:BIBFORM106975
035-os BibID:(cikkazonosító)4540 (WoS)000833614900001 (Scopus)85137331295
Első szerző:Szabó Ruben
Cím:Determination of Phenolic Compounds by Capillary Zone Electrophoresis-Mass Spectrometry / Ruben Szabo, Attila Gaspar
Dátum:2022
ISSN:1420-3049
Megjegyzések:A CZE-MS method was developed for the determination of several phenolic compounds (phenolic acids, flavonoids). Since the analysis of these components necessitates the application of basic conditions for CZE separation and negative ionization mode for MS detection, the simplest choice was to use 0.5 M NH4OH and IPA:water (1:1 v/v%) as the background electrolyte and sheath liquid, respectively. The LOD values ranged between 0.004-1.9 mg/L showing that there are relatively large differences in the ionization (and chemical) features of these compounds. The precision data were better than 0.75 RSD% for migration times and were between 5-8 RSD% for peak areas. In order to test the applicability of the developed method, a honey sample was analyzed.
Tárgyszavak:Természettudományok Kémiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Megjelenés:Molecules. - 27 : 14 (2022), p. 1-12. -
További szerzők:Gáspár Attila (1970-) (vegyész, kémikus)
Pályázati támogatás:K127931
OTKA
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