Search Results (1,651)

Background/Objectives: The purpose of this study was the chemical design, synthesis, and evaluation of the antimicrobial and antibiofilm potentials of 20 novel thiazolyl-methylthio-thiadiazole hybrid compounds (6a–j and 8a–j). Methods: The compounds were designed as structural analogues of halicin with two points of variation and were synthesized through a process with multiple condensation steps. The compounds were evaluated in vitro through MIC determinations for the antimicrobial activity and percentage of biofilm inhibition, and in silico, respectively, through molecular docking, druggability, and ADMETox prediction. A 2D-QSAR study was conducted for antimicrobial activity using the Free-Wilson model. Results: In terms of antibacterial activity, all compounds displayed important activity on the tested strains (MICs = 15.62–250 μg/mL), except against Staphylococcus aureus. Regarding the antifungal activity, the effect against Candida albicans was similar to fluconazole in most cases (MIC = 15.62 μg/mL). With respect to the antibiofilm activity, the most effective activity was registered against the Pseudomonas aeruginosa biofilm. The in vitro results for the antibacterial activity against Escherichia coli were correlated with the observations drawn in the molecular docking study on the ATPase domain of the GyrB subunit of E. coli. The in silico predictions of the molecular properties concluded that all compounds have good druggability properties, while the ADMETox predictions concluded that the compounds could have low gastrointestinal absorption and blood–brain barrier permeation capacity, but raised safety flags (e.g., hepatotoxicity and high acute oral toxicity). The 2D-QSAR study concluded that the thiazolyl-methylthio-thiadiazole scaffold had the highest contribution to antimicrobial activity in almost all cases. Conclusions: The two series of compounds highlight the impact of structural modulations of the scaffold and its substituents on the investigated biological activities. Full article

Porcine epidemic diarrhea virus (PEDV) is the pathogen responsible for porcine epidemic diarrhea, causing significant economic losses to the swine industry. During the replication of PEDV, the genome mutates rapidly, making the effectiveness of commercial vaccines uncertain when facing newly emerging prevalent variants. More importantly, there are currently no safe and effective specific antiviral drugs available. YT1418, a pyrido[1,2-c]pyrimidin-1-one (PPO) compound, exhibited anti-PEDV activity in a previous study. To expand the chemical space of the PPO scaffold and clarify the influence of substituents at different positions on the antiviral activity of the compounds, 36 new compounds were designed and synthesized, and then their abilities to inhibit viral replication in a PEDV-infected cell model were evaluated. Furthermore, the hepatic microsomal metabolic stabilities of compounds with potent antiviral activity were assessed. The results showed that compounds N1 and N2 exhibited antiviral activity (EC₅₀ = 0.32, 0.37 μM, respectively) superior to that of YT1418, with selective index values of 43.78 and 42.89, respectively. Meanwhile, compound J4 demonstrated good hepatic microsomal stability and low cytotoxicity, which requires further investigation. This study identified lead compounds featuring a novel PPO core and established their structure–activity relationships, providing important insights for the development of anti-PEDV drugs. Full article

A series of hexadecylpiperidinium surfactants containing alkyl (PMe-16, PEt-16, PBu-16), benzyl (Benz-16, 1-Benz-3-HP-16, 1-Benz-4-HP-16), and hydroxyl (3-HPMe-16, 4-HPMe-16) substituents in the ring were tested with the nematode Caenorhabditis elegans to investigate the relationship between nematocidal activity and the structural features of surfactants. It was found that increasing the hydrophobicity of the substituent in the surfactant head group reduced the nematocidal activity in the order PMe-16 > PEt-16 > PBu-16 > Benz-16. The lead compound, PMe-16, showed significantly higher activity than the commercial insecticide carbofuran, and was able to induce nearly complete nematode mortality within 24 h at a concentration of 50 μg·mL⁻¹, as well as suppress culture development at concentrations of 25–100 μg·mL⁻¹. All tested piperidinium surfactants inhibited nematode population development at 100 μg·mL⁻¹, while PMe-16 remained effective at concentrations as low as 25 μg·mL⁻¹. The membranotropic properties of the surfactants were evaluated using a turbidimetric method with dipalmitoylphosphatidylcholine (DPPC)-based liposomes as a model of biomembranes. Dynamic light scattering measurements were performed in parallel to assess changes in liposome size and zeta potential as a function of surfactant content, as well as to determine the critical concentration required to induce lipid bilayer destabilization. These results provide indirect evidence of surfactant–membrane interactions. The combinations of piperidinium surfactants and carbofuran showed pronounced synergistic effects, reducing the insecticide dose while maintaining efficacy. Synergy was evaluated using the Bliss independence model and the Highest Single Agent model. The addition of the most active surfactants (PMe-16 and 4-HPMe-16) at 6.25 μg·mL⁻¹ enabled an approximately twofold reduction in the carbofuran dose while maintaining full nematocidal activity. Full article

Three ethynyl-extended benzanthrone derivatives with benzonitrile (Dye A), thiophene (Dye B), and methyl propiolate (Dye C) as substituents were synthesized and investigated to illustrate structure–property relationships governing their nonlinear optical (NLO) behavior. The third-order nonlinear absorption and refractive index of three dyes were studied using open- and closed-aperture z-scan measurements under 532 nm continuous-wave laser excitation. All dyes exhibited reverse saturable absorption dominated by two-photon absorption, with Dye A showing the highest nonlinear absorption coefficient (βeff = 2.3 × 10⁻⁵ cm/W) and two-photon response, attributed to its extended conjugation and smaller HOMO−LUMO gap (6.45 eV). Closed-aperture Z-scans revealed strong nonlinear refraction (n₂), with the thiophene-substituted Dye B displaying the largest n₂ (14.8 × 10⁻⁹ cm²/W) and third-order susceptibility (χ³ = 3.1 × 10⁻⁶ esu). The evaluated optical switching figures of merit met the requirements for all-optical switching and optical limiting. DFT and TDDFT calculations demonstrated that donor substitution and conjugation length govern electronic structure, charge transfer character, and global reactivity descriptors. Enhanced electronic softness and hyperpolarizability in Dye B further support its superior refractive nonlinearity. These results establish clear structure–property correlations and highlight donor engineering as an effective strategy for developing organic nonlinear optical and photonic materials. Full article

Selective inhibition of the tumour-associated carbonic anhydrase (CA) isoforms IX and XII, which are overexpressed in hypoxic tumours, has emerged as a promising strategy for the development of novel anticancer agents. Among the diverse CA inhibitors reported to date, coumarins have attracted particular attention. These chromenone derivatives, widely distributed in phytochemicals, display a broad range of biological activities and are known to act as suicide inhibitors of CAs. Following the tail approach, we designed a series of hybrid compounds combining a coumarin core with an N-arylthioureido scaffold located at the C-7 position and investigated how structural variations—including substituents on the coumarin and aromatic moieties, tether length, and urea/thiourea isosterism—influence their biological properties (CA inhibition and antiproliferative activity). Substituted coumarins at C-3 and C-4 were efficiently prepared via Pechmann condensation, while the thioureido motif was introduced using various aryl isothiocyanates as key synthetic intermediates. The lead compound, featuring a dimethylated coumarin, a pentyl linker, and an N-(p-tolyl)thioureido residue, inhibited the target enzymes in the low- to mid-nanomolar range (K_i = 6.0 and 49.9 nM, respectively), displaying selectivity indexes (S.I.s) surpassing those of the reference drug acetazolamide (AAZ). Moreover, it exhibited potent antiproliferative activity, with GI₅₀ values in the low micromolar range (1.9–3.5 µM) against both drug-sensitive and multidrug-resistant cancer cell lines. Label-free three-dimensional holotomographic microscopy revealed that this compound triggers slow apoptosis, leading to cell death after approximately 20 h of exposure. Full article

Background: Organic cation transporter 2 (OCT2) mediates the renal uptake of cisplatin and is a principal contributor to its dose-limiting nephrotoxicity. Despite reports of OCT2 inhibition by various phytochemicals, the structure–activity relationships (SARs) governing inhibition and their functional implications remain poorly understood. Methods: We systematically evaluated OCT2 inhibitory activity across a structurally diverse library of 146 phytochemicals, including anthraquinones, flavanols, stilbenes, and isoflavones, using Madin–Darby canine kidney (MDCK) cells stably overexpressing OCT2. Structure–activity relationships were analyzed using non-parametric statistics and multivariate logistic regression, and functional relevance was assessed via cisplatin-induced cytotoxicity assays. Results: Inhibitory activity varied widely across the library, with potent inhibitors identified across multiple chemical scaffolds. Non-parametric statistical analyses revealed no significant differences in overall activity distributions among scaffold classes. Notably, chemical substituent patterns, rather than core scaffold identity, were the primary drivers of OCT2 inhibitory potency. Methoxylation was consistently associated with enhanced OCT2 inhibition, particularly within isoflavones, although its impact varied across structural scaffolds. The selected OCT2 inhibitors markedly reduced cisplatin-mediated cell death in OCT2-expressing cells but not in mock-transfected controls, confirming an OCT2-dependent mechanism of protection. Conclusions: This study establishes a structure-guided framework linking phytochemical OCT2 inhibition to nephroprotective potential and identifies methoxylation as a major determinant of OCT2-targeted intervention strategies. Full article

9-Mesitylacridinium salts are widely recognized as efficient organic photoredox catalysts owing to their strong excited-state oxidizing power and stability under visible-light irradiation. In this study, a new mesityl acridinium derivative bearing a di-tert-butylphenyl substituent on the nitrogen atom was synthesized. The introduction of tert-butyl groups on the N-aryl moiety was primarily aimed at improving solubility and chemical stability of the acridinium salt. Starting from a 9(10H)-acridinone precursor, the target compound was obtained in high overall yield through a concise synthetic sequence. The synthesis consists of a copper-catalyzed C–N coupling reaction to install the aryl substituent on the nitrogen atom, followed by a Grignard reaction and subsequent acid treatment to afford the corresponding acridinium salt. All transformations proceeded smoothly, providing efficient access to the desired novel acridinium derivative. This work presents a practical example of the structural modification of mesitylacridinium derivatives directed toward enhanced solubility and stability, and provides a useful synthetic platform for the preparation of structurally diverse acridinium salts. Full article

Pyrazole derivatives have emerged as an important class of heterocyclic compounds in anticancer research due to their structural versatility and broad spectrum of biological activities. This review provides a concise overview of recent advances in the development of pyrazole-based anticancer agents, with emphasis on synthetic strategies, structure–activity relationships, and molecular mechanisms of action. Common synthetic approaches, particularly condensation and cyclization reactions, have enabled the preparation of structurally diverse pyrazole derivatives for biological evaluation. Available evidence indicates that the type and position of substituents within the pyrazole scaffold markedly influence anticancer potency, selectivity, and target affinity. Reported compounds act through multiple mechanisms, including inhibition of cancer-related targets such as tubulin, epidermal growth factor receptor (EGFR), cyclin-dependent kinases (CDKs), Bruton tyrosine kinase (BTK), and deoxyribonucleic acid (DNA)-associated pathways, as well as induction of apoptosis and disruption of cell-cycle progression. Several pyrazole derivatives have shown promising activity in in vitro and in vivo models. Overall, the findings summarized in this review identify the pyrazole scaffold as a valuable platform for the design and optimization of novel anticancer agents and support its continued exploration in medicinal chemistry. Full article

A structural analysis of phenylpropanoids demonstrates that the benzene ring and the propenoic fragment act as two largely independent π-electron systems. This distinctive feature provides a theoretical basis for the rational design of novel compounds obtained through the structural integration of phenylpropanoids with polyene aldehydes and acids. These classes may be combined by elongating the carbon backbone via iterative vinyl group extension, thereby generating an expanded conjugated double-bond system. Alternatively, the structure of polyene aldehydes may be modified by replacing the unreactive methyl group with a benzene ring bearing suitable functional substituents. DFT computational studies performed at the B3LYP/QZVP level of theory indicate that the designed analogs predominantly scavenge radicals through the sequential proton loss electron transfer (SPLET) mechanism in aqueous environments. This pathway involves the initial deprotonation of carboxyl, aldehyde, or phenolic groups, with the hydroxyl moiety exhibiting the greatest propensity for proton dissociation. Carbon chain extension exerts only a minor influence on proton affinity (PA) values but significantly affects electron transfer enthalpy (ETE) parameters. Consequently, increasing the number of conjugated double bonds enhances activation of the second step of the SPLET mechanism, thereby improving overall radical-scavenging activity. Comparison of the calculated chemical reactivity parameters substantiates the conclusions drawn from the thermodynamic analysis. A pronounced enhancement in the reactivity of the modeled compounds, relative to the parent constituents, is observed. Time-dependent density functional theory (TD-DFT) calculations further predict absorption in the visible region, indicating potential applications of the modeled compounds as radical-scavenging dyes in food, pharmaceutical, cosmetic, and dietary supplement formulations. Full article

To investigate the potential of halogen-containing building blocks in the development of artificial carbohydrate receptors, the 1,3,5-trisubstituted 2,4,6-triethylbenzene scaffold with halogenated subunits and classical hydrogen bonding sites was used as a model system. In the first studies, the influence of the presence of halogens on the binding properties of compounds bearing benzamidomethyl units was investigated, whereby the type of halogen and its ring position were varied. The question was whether the presence of halogens could lead to an increase in binding effectivity and whether this increase can be attributed to the formation of halogen bonds (especially for X = Br and I in ortho position) with the sugar substrate or to other effects. The binding studies revealed some interesting relationships between structure and binding affinity for the tested compounds 1–9. For those bearing the halogen substituent in the ortho position to the amide functionality, the binding affinity increases in the expected order 4 (o-F) < 3 (o-Cl) < 2 (o-Br) < 1 (o-I). In the presence of small amounts of water in CDCl₃, an increase in binding strength was observed in comparison to experiments conducted in dry CDCl₃. The present studies aim to provide impulses for the use of halogenated building blocks in the design of artificial carbohydrate receptors. Optimizing the type of halogenated units and the receptor architecture should result in more effective carbohydrate receptors capable of functioning effectively in aqueous media through a combination of different noncovalent interactions. Full article

Seminaphtofluorones (SNAFRs) are a family of benzannulated xanthene dyes that exhibit strong fluorescence in both neutral and anionic states and can reach emission wavelengths in the deep-red to near-infrared region. Their optical response is highly sensitive to regioisomerism and functionalization, making them attractive candidates for systematic structure–property investigations. Here, we computed the photophysical properties of six SNAFR regioisomers for both neutral and anionic species and correlate the calculated results with available experimental data. From the six dyes, we further chose two of them, SNAFR4 and SNAFR6, to further investigate how phenyl-ring functionalization modulates SNAFR properties by introducing methyl (–CH₃) and carboxyl (–COOH) substituents at the ortho (o), meta (m), and para (p) positions. The calculations indicate that substitution induces measurable changes in geometries, as well as in excitation and emission energies, with particularly pronounced effects for the anionic derivatives. Overall, these results provide a computational framework for the rational tuning of SNAFRs’ optical properties and the design of derivatives with tailored optical characteristics for fluorescence imaging and applications in photodynamic therapy. Full article

Phenetole derivatives with dual ethoxy substituents exhibit rich conformational diversity and complex vibronic characteristics, making them important model compounds for understanding substituent effects on molecular structure and spectroscopy. In this work, we systematically investigated the stable rotamers, vibronic spectra, and cationic ground-state features of p-diethoxybenzene (PDEB) using resonance-enhanced multiphoton ionization (REMPI), UV-UV hole-burning (HB), and mass-analyzed threshold ionization (MATI) spectroscopies, combined with density functional theory (DFT) calculations. The ground-state potential energy surface (PES) of PDEB was calculated at the B3LYP/6-311++G(d,p) level, identifying eight rotamers with distinct statistical weights and relative energies. Hole-burning spectroscopy resolved two dominant rotamers (cis/up–up and trans/up–down) in the supersonic molecular beam, with their S₁←S₀ transition origins determined as 33,824 cm⁻¹ and 33,613 cm⁻¹, respectively. Franck-Condon simulations of the vibronic transitions showed excellent agreement with the experimental REMPI spectra, enabling precise assignment of substituent and benzene ring vibrational modes. MATI experiments yielded accurate adiabatic ionization energies (AIEs) of the cis and trans rotamers as 59,629 ± 5 cm⁻¹ and 59,432 ± 5 cm⁻¹, respectively, and identified active cationic vibrational modes in the D₀ state. Geometric parameters of PDEB in the S₀, S₁, and D₀ states were calculated at the B3PW91/aug-cc-pVTZ, TD-B3PW91/aug-cc-pVTZ, and UB3PW91/aug-cc-pVTZ levels, revealing structural evolution during electronic excitation and ionization. The effects of ethoxy substituent orientation on molecular energy, vibrational frequencies, and ionization energy are discussed, and differences in spectral characteristics between PDEB and its meta isomer (MDEB) are compared. This work provides a comprehensive spectral and structural database for p-diethoxybenzene and deepens the understanding of structure–property relationships in diethoxybenzene isomers. Full article

Bidentate ligands, derived from the 1,3-dicarbonyl framework, play a central role in coordination chemistry, catalysis, and materials science due to their tuneable donor properties and structural versatility. This review examines and compares three closely related ligand classes, β-diketones (O,O′ donors), imino-β-diketones or enaminones (N,O donors), and di-imino-β-diketones or β-diketiminates (N,N′ donors), to elucidate how systematic substitution of oxygen by nitrogen affects structure and properties. The discussion integrates spectroscopic data (NMR and IR), crystallographic findings, electrochemical measurements, and density functional theory (DFT) calculations reported in the literature. Across these systems, tautomerism plays a decisive role, with conjugation-stabilized enol or enamine forms generally preferred in solution and the solid state. Frontier molecular orbital analyses show extensive delocalization over the chelate backbone and, when present, aromatic substituents. Electrochemical studies reveal consistent correlations between experimental reduction potentials and calculated LUMO energies for O,O′-, N,O-, and N,N′-bidentate ligands. Overall, the comparison demonstrates that donor atom substitution within a conserved conjugated scaffold provides a systematic approach to tuning acidity, coordination behaviour, and redox properties, offering a coherent framework for understanding structure–property relationships in 1,3-dicarbonyl-derived chelating ligands. Full article

The objective of this study was to design and evaluate π-extended 1,8-naphthalimide derivatives as photoinduced electron transfer (PET) optical sensors for protons and metal cations, with emphasis on the role of heterocyclic annulation and receptor–chromophore electronic matching. Benzofuran- and benzodioxin-annulated naphthalimides bearing either a dimethylaminoethyl receptor or a non-donating alkyl substituent at the imide nitrogen were synthesized using tailored synthetic strategies. Their photophysical properties were investigated by absorption and fluorescence spectroscopy, while sensing performance was evaluated by fluorescence titrations. Quantum chemistry calculations were employed to rationalize experimental observations. Benzofuran-annulated derivatives exhibit structured π–π* absorption bands and strong fluorescence, whereas introduction of the receptor induces efficient fluorescence quenching via reductive PET. Protonation or metal ion coordination suppresses PET and leads to pronounced fluorescence enhancement, particularly in the presence of Cu(II) and Sn(II). In contrast, benzodioxin-annulated derivatives display intramolecular charge-transfer absorption bands, large Stokes shifts, and low fluorescence quantum yields in polar media, resulting in a negligible sensing response. Computational results attribute this behavior to an unfavorable energy arrangement of the donor–acceptor orbitals. Overall, the study demonstrates that heterocyclic annulation critically governs the electronic structure and sensing performance of naphthalimide fluorophores, providing guidelines for the rational design of PET-based optical sensors. Full article

Ruthenocene (Rc) and its derivatives form a structurally versatile class of metallocenes with unique and multifunctional applicability. This review presents a detailed analysis of Rc chemistry including the structural comparison with ferrocene, its redox behavior, and substituent effects. We also discuss its applications in sensing, energy storage, photochemistry, and biomedicine. Rc exhibits unique conformational and adaptive electronic properties based on one and two-electron oxidation processes. Electrochemical investigations of Rc to date indicate that its redox behavior is strongly dependent on the electrolyte system, exhibiting quasi-Nernstian characteristics, the formation of stabilized dimeric species [Rc₂]²⁺, and interconversion among Ru(II), Ru(III), and Ru(IV) oxidation states. Rc-based systems exhibit superior performance as redox mediators and labels in electrochemical sensing systems in terms of electron-transfer kinetics, signal amplification, and surface immobilization. In the field of energy storage, Rc decreases the charging overpotential and increases the cycle life of Li-O₂ batteries. Rc further acts as a photoinitiator via charge-transfer-to-solvent and efficient photoinduced electron transfer in metalloporphyrin and fullerene dyads. In biomedical research, Rc derivatives as well as bioconjugates possess promising anticancer activities, displaying reactive oxygen species generation, topoisomerase inhibition, thioredoxin reductase inhibition, receptor-mediated uptake, and target peptide conjugation. Given its flexible ligand design, electrolyte driven redox behaviors, and antiproliferative properties, Rc exhibits a very adaptive molecular scaffold for next generation electrochemical technologies as well as metallodrug design. Full article