Search Results (852)

Conventional strategies to enhance the hydrophobicity of polyurethane (PU) coatings typically rely on fragile micro/nanostructures or irradiation-induced crosslinking, both of which suffer from poor controllability and often compromise mechanical robustness. Herein, we report a UV-triggered crosslinking strategy based on coumarin chemistry that enables precise, controllable network formation, thereby simultaneously enhancing the hydrophobicity, adhesion strength, and thermal stability of polydimethylsiloxane (PDMS)-based PU coatings. A series of coumarin-functionalized PDMS-PU coatings (HNP-PDMS-PUx) was prepared by blending coumarin-grafted PDMS (HNP) with PDMS-PU elastomers. Upon 365 nm UV irradiation, the coumarin moieties dimerize, forming a dense, chemically crosslinked “brush-like” structure on the coating surface. The optimal coating (HNP-PDMS-PU_3/1) exhibited a significant increase in water contact angle from 108° to 129° on average, reaching a maximum of 134°. The UV-treated coating also showed enhanced adhesion strength (a 45% increase) and improved thermal stability, while maintaining good flexibility (F7 rating) and abrasion resistance (contact angle remained at 126° after 30 cycles). Moreover, the coating demonstrated excellent easy-cleaning performance against both liquid and solid contaminants. This work provides a photochemical strategy that replaces uncontrollable or irreversible crosslinking methods with a controllable UV-triggered approach, enabling synergistic enhancement of multiple properties. Full article

Growth hormone-releasing hormone receptor 1a (GHS-R1a) is a key G protein-coupled receptor (GPCR) governing feeding and energy homeostasis. Accumulating evidence shows that GHS-R1a forms functional heterodimers with multiple metabolic-related GPCRs, including dopamine 2 receptor (D2R), melanocortin 3 receptor (MC3R), 5-hydroxytryptamine 2c receptor (5-HT2cR), orexin receptor 1 (OX1R) and cannabinoid receptor 1 (CB1R). These heterodimers undergo distinct signal transduction reprogramming, generating novel physiological effects that are not observed with individual receptors: for instance, GHS-R1a/D2R mediates an atypical calcium signaling pathway to regulate appetite, while GHS-R1a/5-HT2cR antagonizes ghrelin-induced orexigenic effects. Meanwhile, diverse detection techniques, including co-immunoprecipitation and fluorescence resonance energy transfer, have been developed to identify and validate GHS-R1a heterodimerization, laying a solid foundation for mechanistic research. This review systematically summarizes the molecular mechanisms of GHS-R1a heterodimer formation, the characteristic signal regulation patterns of different heterodimers, and their specific regulatory roles in feeding circuits. Furthermore, we discuss the existing research gaps in this field, such as the lack of in vivo detection methods for heterodimers and the unclear structural basis of dimerization. Finally, we highlight the potential of targeting specific GHS-R1a heterodimers as a novel therapeutic strategy for obesity and anorexia, providing new directions for future pharmaceutical development and clinical translation. Full article

Purpose: Preclinical studies report low-intensity ultraviolet C (UVC) light to be safe and effective in treating murine bacterial keratitis, however, limbal impacts of UVC have yet to be investigated directly. This study evaluated the depth and density of UVC-induced DNA damage in the porcine and human limbus following UVC exposures of varying supratherapeutic dose. Methods: The corneoscleral junction (limbus) of full-thickness porcine corneas was exposed to supratherapeutic doses of UVC light (265 nm, 1.93 mW/cm²) for 5, 10, 15, 30, or 60 min (exposure groups) or remained unexposed for the same durations (control groups), with a sample size of 6 per group. In parallel, human corneal tissue was exposed to UVC for 1 or 5 min and processed identically. Following exposure, all tissues were frozen, dissected, and analysed using immunohistochemistry to detect cyclobutane pyrimidine dimers (CPDs) as markers of DNA damage. CPD distribution, depth, and density were subsequently evaluated. Results: CPDs were localised predominantly in the superficial corneal epithelial layers, irrespective of the UVC dose. The mean ± SD thickness of the corneal epithelium in the UVC-exposed groups was 38.9 ± 18.9 µm, and the average depth of CPD formation was 13.3 ± 8.43 µm. The proportions of cells affected by CPDs within the corneal epithelium (mean ± SD) were 47.8 ± 25.6%, 58.5 ± 16.2%, 39.9 ± 26.4%, 41.3 ± 27.3%, and 38.9 ± 28.3% for exposure durations of 5, 10, 15, 30, and 60 min, respectively (p > 0.05). Human cornea showed similarly limited penetration, with no difference in CPD proportions between the 1 and 5 min UVC exposures (p = 0.70). Conclusions: UVC-induced DNA damage in both species was confined to the superficial cellular layers of the cornea, with no detectable damage observed in deeper tissues, including those where limbal stem cells reside, even after supratherapeutic doses of up to one hour of exposure. Full article

The emergence of clinical resistance to conventional antigiardials underscores the need for compounds with novel mechanisms of action. This study demonstrates that indirubin exerts antigiardial activity by targeting important metabolic enzymes in Giardia lamblia. Indirubin induced a concentration-dependent decrease in trophozoite proliferation and viability, correlating with reduced activity of native triosephosphate isomerase and aldose reductase. Using recombinant enzymes, indirubin directly inhibited triosephosphate isomerase and aldose reductase, with the parasite enzymes showing greater susceptibility than their human orthologs. Structural and computational analyses suggest preferential binding of indirubin at the dimer interface of triosephosphate isomerase and within the NADP(H)-binding pocket of aldose reductase. The dual enzymatic inhibition was concordant with methylglyoxal accumulation, extensive protein carbonylation, and the formation of advanced glycation end products. These effects culminated in apoptotic-like death and severe ultrastructural damage, including alteration of the adhesive disc and microtubule networks. By targeting vulnerabilities in the metabolic and redox pathways of G. lamblia through a multifactorial mechanism distinct from current therapies, our findings support indirubin as a promising candidate for the treatment of giardiasis. Full article

The subject of the presented work was the study of the pathways of geraniol transformation during its oxidation with molecular oxygen in the presence of a natural Japanese volcanic clay mineral—mironekuton—used as a green heterogeneous catalyst. Prior to the catalytic tests, a comprehensive characterization of mironekuton was carried out using SEM, XRD, EDX, FTIR, and UV–Vis techniques. The catalytic experiments were aimed at establishing reaction conditions enabling effective geraniol conversion and controlling the distribution of valuable transformation products under solvent-free conditions. The influence of temperature (75–100 °C), catalyst content (0.5–5.0 wt%), and reaction time (15–360 min) was systematically investigated. The obtained results demonstrated that pristine mironekuton exhibits moderate activity and limited selectivity toward low-molecular-weight oxygenated derivatives of geraniol, such as 2,3-epoxygeraniol, 2,3-epoxycitral, and citral. Instead, dehydration, isomerization, and dimerization reactions play a significant role, leading to the formation of higher-molecular-weight products, particularly thunbergol and 6,11-dimethyldodeca-2,6,10-trien-1-ol. Sulfuric acid treatment of mironekuton results in a pronounced enhancement of catalytic activity and a substantial shift in product distribution. This effect is directly related to the increased surface acidity, which promotes dehydration–dimerization pathways over epoxidation, leading to thunbergol as the dominant product with high and reproducible selectivity, while epoxidation products are no longer detected. Kinetic modeling of the geraniol transformation process revealed that epoxidation steps are kinetically disfavored and that epoxide species act only as short-lived intermediates, whereas dehydration–dimerization pathways are kinetically preferred. Overall, the results indicate that acid-activated mironekuton functions as an efficient and environmentally benign heterogeneous catalyst, favoring selective thunbergol formation under mild, solvent-free conditions, using molecular oxygen as a green oxidant. Full article

The growing problem of antibiotic resistance poses a serious threat to public health and ecosystems. New disinfection methods could help address this global issue. In this study, ultraviolet-C light-emitting diodes (UV-C LEDs) were used to inactivate Escherichia coli isolates resistant to antibiotics. These isolates were obtained from various real water sources, including seawater, surface water, and treated wastewater. Inactivation assays were performed using two wavelengths (255 nm and 265 nm), applying UV fluences ranging from 1 to 7 mJ/cm² to a phosphate-buffered saline solution inoculated with a mixture of 10 E. coli strains. Using an UV fluence of 2 mJ/cm², a log reduction of about 5 was achieved with both UV-C wavelengths tested. SEM imaging revealed no observable alterations in cell morphology after UV-C exposure. Pyrimidine dimer formation was quantified, yielding approximately 40 ng/mL of cyclobutane pyrimidine dimers after 2 mJ/cm² of exposure to both wavelengths. Additionally, water treatment was tested using ceramic silicon carbide membranes. High average rejection efficiencies (99.9%) were obtained for both total coliforms and E. coli using uncut flat sheet membranes. The combination with UV-C LEDs led to treatment of the concentrated membrane retentate (99.985% or higher), highlighting the potential of this treatment approach for effective water disinfection. Full article

Neurotensin (NTS) binds to the G protein-coupled receptors (GPCRs) NTSR1 and NTSR2. NTSR1 regulates transactivation of the EGFR, HER2, and HER3, but its effects on HER4 are unknown. By Western blot, NTSR1 and HER4 were present in six lung cancer cell lines examined. In NCI-H522 or NCI-H661 cells, adding NTS increased phosphorylation (P) of tyrosine (Y) 1284 on HER4. Because SR48692 antagonized NTS’s ability to increase P-HER4 or P-ERK, NTSR1 may play an important role in NSCLC. SR48692, HER4 siRNA, reactive oxygen species inhibitors, and the tyrosine kinase inhibitor ibrutinib inhibited NTS-induced P-HER4. Adding NTS to NCI-H661 cells increased the formation of HER4/HER4, HER4/ EGFR, and HER4/HER2 dimers. Adding NTS to NSCLC cells increased both P-ERK and P-AKT, which were inhibited by PD98059 and LY294002, respectively. The growth of NCI-H522 or NCI-H661 cells was stimulated by NTS or neuregulin 1 (NRG1), a HER4 ligand, but inhibited by SR48692 or ibrutinib. The results indicate that NTSR1 regulates HER4 transactivation, thereby increasing the proliferation of lung cancer cells. Full article

The rise in antimicrobial resistance represents a significant challenge to global health. The reason partially lies in an inappropriate use of conventional antibiotics and the subsequent rapid spread of multidrug-resistant pathogen strains. This emergency requires an urgent search for conceptually new antimicrobial agents. A viable alternative to conventional antibiotics is antimicrobial peptides (AMPs), which are ribosomally synthesized molecules with considerable potential as next-generation anti-infectious therapeutics. Previously, we have reported on the β-hairpin peptide Ap9, an analog of abarenicin from the marine polychaeta Abarenicola pacifica, with potent activity against key Gram-negative pathogens. Here, it is shown that Ap9 acts in a manner resembling polymyxin B, namely via interaction with lipopolysaccharide (LPS), and retains its activity against polymyxin-resistant isolates without observed cross-resistance, and causes insignificant damage in cytoplasmic membrane at bactericidal concentrations. NMR spectroscopy reveals that LPS binding induces a conformational rearrangement of Ap9, its dimer formation, and local structural remodeling of the peptide region (residues 8–12) into 3₁₀-helix. Bacterial resistance to Ap9 was found to be relatively low with a reduced susceptibility associated with infrequent genetic alterations, such as the mutation in lptD or the deletion in mlaA. Furthermore, Ap9 demonstrates a favorable tolerability, a wider therapeutic window than that of polymyxin B, and a sufficiently long half-life through the systemic use, as well as in vivo efficacy in murine models of Gram-negative infections, including sepsis caused by the mcr-1-harboring Escherichia coli strain. The obtained results point to Ap9 as a promising candidate for further preclinical studies aimed at development of an alternative to polymyxins. Full article

The dynamics of initial layer-by-layer growth and subsequent nucleation of quantum dots of Si and Ge on Si(001) were studied combining reflection high-energy electron diffraction, scanning electron microscopy and atomic force microscopy. It was shown that the processes occurring at the initial stage determine further growth of the heterostructure and final shape and density of nanoislands. The mechanisms of terrace formation, occurrence and dynamics of dimer rows of the 2 × N superstructure, and effects of temperature on the growth characteristics were described. The obtained experimental dependences show the critical relationship between the synthesis parameters (growth temperature), epitaxial growth processes and the characteristics of the resulting nanoislands. The fundamental studies conducted make it possible to create self-organizing quantum dots of a given size and density for advanced optoelectronics, including infrared photosensitive elements and single-photon detectors. Full article

Background/Objectives: DNA methylation is a key epigenetic modification involved in regulating many cellular processes, including gene expression and the maintenance of genome stability. Ultraviolet (UV) radiation induces DNA damage in the form of pyrimidine-pyrimidone (6-4) photoproducts [(6-4)PPs] and cyclobutane pyrimidine dimers (CPDs), which can lead to mutations if not efficiently repaired. While cytosine methylation has been implicated in influencing UV-induced DNA damage formation, the effect of DNA methylation modulators such as S-adenosyl-L-methionine (SAM) and RG108 on UV damage formation and repair remains unclear. Methods: Here, using immunoslot blot assays, we investigated the effects of SAM and RG108 on UV-induced DNA damage formation and repair in human lymphoblastoid cells. Results: We found that SAM, but not RG108, rapidly suppresses the formation of both (6-4)PP and CPD, with detectable effects within minutes of exposure. Although SAM pretreatment was associated with modestly accelerated early (6-4)PP repair, this effect was accompanied by substantially lower initial damage levels. When cells were treated with SAM or RG108 immediately after UV irradiation to ensure equivalent initial damage burden, no significant differences in repair were observed for either lesion type, demonstrating that the accelerated early (6-4)PP repair reflects reduced lesion burden rather than increased intrinsic nucleotide excision repair (NER). Global 5-methylcytosine (5mC) levels remained stable following SAM or RG108 treatment and during UV damage repair, suggesting that these effects occur independently of global alterations in DNA methylation. Conclusions: Together, our findings reveal that SAM modulates UV damage susceptibility at the level of lesion formation without altering repair, highlighting a previously unrecognized role for DNA methylation modulators in regulating genome stability. Full article

Noble metal nanostructures provide versatile platforms for light manipulation through localized surface plasmon resonances (LSPRs). Among them, triangular silver nanoplates (AgNPTs) exhibit strong field-enhancement and spectral tunability, yet assembling them reproducibly on solids is challenging. We report a two-step functionalization strategy for constructing ordered AgNPT dimers on silica substrates, combining 3-aminopropyltriethoxysilane (APTES) anchoring with 1,4-butanedithiol bridging. AFM reveals face-to-face dimers with well-defined sub-nanometer gaps. Large-area AFM statistics collected over multiple regions (N = 80 nanoplates per condition) confirm reproducible and selective vertical dimerization. Extinction spectroscopy reveals sequential dielectric and coupling effects: thiol adsorption red-shifts the main resonance from 700 to 780 nm because of increased local refractive index and near-field damping, whereas dimerization partially restores it to ≈750 nm, consistent with plasmon hybridization within rigid ∼0.7 nm molecular gaps, where nonclassical moderation may occur but classical hybridization fully explains the observed shifts. Concomitantly, the extinction intensity doubles, following an exponential growth toward saturation during assembly. Surface-enhanced Raman scattering (SERS) measurements using 4-mercaptobenzoic acid (4-MBA) confirm a fourfold increase in the SERS enhancement factor from monolayer to bilayer, consistent with near-field coupling and hotspot formation at interplate junctions. Quantitative plasmon sensitivity analysis yields comparable results between experiments and finite-difference-time-domain simulations, confirming that the observed spectral shifts arise from near-field coupling and dielectric modulation rather than ensemble effects. This reproducible methodology enables precise tuning of NPT orientation, spacing, and optical response, providing a robust platform for enhanced sensing, SERS, and nanophotonic device engineering. Full article

The central role of YB-1 in messenger ribonucleoprotein particle (mRNP) metabolism and stress-granule biology highlights the importance of defining the determinants of its self-assembly. YB-1 fibrillogenesis has been attributed primarily to the cold shock domain (CSD). Here, we show that the YB-1 fragment spanning residues 1–129 (AP–CSD) form amyloid fibrils under near-physiological ionic strength (0.12–0.15 M KCl). Fibrillization proceeds without a pronounced exponential growth phase and increases approximately linearly over 45–50 h. Far-UV circular dichroism (CD) and attenuated total reflection Fourier-transform infrared spectroscopy (ATR-FTIR) indicate no substantial change in overall secondary-structure content during aggregation. In parallel, ¹H nuclear magnetic resonance (NMR) spectroscopy reveals the depletion of soluble species, and oriented fiber X-ray diffraction displays the hallmark cross-β reflections at approximately 4.7 Å and 10 Å. The prolonged formation time implies an activation barrier that is unlikely to require global refolding. Instead, it may reflect early association events such as dimerization or other local rearrangements required for primary nucleation, followed by consolidation into stable intermolecular contacts. Aggregation that preserves a largely native-like fold while establishing cross-β order may reduce recognition by cellular quality-control systems that preferentially target globally unfolded or strongly destabilized states. This provides a plausible framework for how YB-1 derived assemblies could persist under stress and during age-associated proteostasis decline. Full article

Copper dithiocarbamate complexes have long been known and are relevant in biology, medicine and material science; however, their low solubility in water can be a limitation. Therefore, the search for modified ligands is an important task. Copper complexes with five phosphorylated dithiocarbamates were investigated in aqueous solutions by several experimental and theoretical methods. Copper(II) bis-complex formation constants were obtained from spectrophotometric titrations. Based on UV-vis and EPR spectroscopy data, the presence of monoligand complexes (in excess copper) and hydroxy-forms (under basic conditions) was revealed. The structures of the obtained forms were optimized using DFT calculations. The instability of complexes under neutral and acidic conditions was established and interpreted by the dimerization upon protonation. This assumption is supported by association constants derived from quantum chemically computed Gibbs free energies for protonated and non-protonated copper(II) bis-dithiocarbamate complexes. Crystal structures of protonated binuclear and non-protonated mononuclear complexes were established using X-ray diffraction. The redox properties of the complexes were studied by cyclic voltammetry; the electrochemical behavior of the complexes was strongly influenced by pH. The scheme of the copper(I)/(II)/(III) species transformations, including chemical and electrochemical stages, is proposed on the base of experimental data and quantum-chemical calculation results. Full article

Here, we report a comparative scanning tunneling microscopy study of two brominated dibenzo[c,g]carbazole derivatives on Ag(111): 5,9-dibromo-7H-dibenzo[c,g]carbazole (DBC) and 5,9,7-tribromo-7-(4-bromobutyl)-7H-dibenzo[c,g]carbazole (BrBu-DBC). At room temperature (RT), DBC forms ordered paired-row supramolecular assemblies, whereas annealing to 470 K induces the formation of butterfly-like dimers that further organize into periodic arrays, consistent with adatom-mediated N–Ag–N coordination. In contrast, BrBu-DBC shows disordered adsorption at RT but transforms at 490 K into dumbbell-shaped dimers coupled selectively at the terminal side chains, consistent with C–C linkage formation. We demonstrate how subtle functional modification modulates the competition between supramolecular assembly and surface-mediated transformation pathways. 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