RÉSUMÉ
Diabetes mellitus is a severe endocrine disease that affects more and more people every year. Modern medical chemistry sets itself the task of finding effective and safe drugs against diabetes. This review provides an overview of potential antidiabetic drugs based on three heterocyclic compounds, namely morpholine, piperazine, and piperidine. Studies have shown that compounds containing their moieties can be quite effective in vitro and in vivo for the treatment of diabetes and its consequences.
Sujet(s)
Hypoglycémiants , Morpholines , Pipérazine , Pipéridines , Humains , Pipéridines/composition chimique , Pipéridines/pharmacologie , Pipéridines/usage thérapeutique , Hypoglycémiants/composition chimique , Hypoglycémiants/pharmacologie , Hypoglycémiants/usage thérapeutique , Morpholines/composition chimique , Morpholines/pharmacologie , Morpholines/usage thérapeutique , Pipérazine/composition chimique , Pipérazine/pharmacologie , Animaux , Pipérazines/composition chimique , Pipérazines/pharmacologie , Pipérazines/synthèse chimique , Pipérazines/usage thérapeutique , Diabète/traitement médicamenteux , Relation structure-activitéRÉSUMÉ
Monoamine oxidase inhibitors (MAOIs) have been crucial in the search for anti-neurodegenerative medications and continued to be a vital source of molecular and mechanistic diversity. Therefore, the search for selective MAOIs is one of the main areas of current drug development. To increase the effectiveness and safety of treating Parkinson's disease, new scaffolds for reversible MAO-B inhibitors are being developed. A total of 24 pyridazinobenzylpiperidine derivatives were synthesized and evaluated for MAO. Most of the compounds showed a higher inhibition of MAO-B than of MAO-A. Compound S5 most potently inhibited MAO-B with an IC50 value of 0.203 µM, followed by S16 (IC50 = 0.979 µM). In contrast, all compounds showed weak MAO-A inhibition. Among them, S15 most potently inhibited MAO-A with an IC50 value of 3.691 µM, followed by S5 (IC50 = 3.857 µM). Compound S5 had the highest selectivity index (SI) value of 19.04 for MAO-B compared with MAO-A. Compound S5 (3-Cl) showed greater MAO-B inhibition than the other derivatives with substituents of -Cl > -OCH3 > -F > -CN > -CH3 > -Br at the 3-position. However, the 2- and 4-position showed low MAO-B inhibition, except S16 (2-CN). In addition, compounds containing two or more substituents exhibited low MAO-B inhibition. In the kinetic study, the Ki values of S5 and S16 for MAO-B were 0.155 ± 0.050 and 0.721 ± 0.074 µM, respectively, with competitive reversible-type inhibition. Additionally, in the PAMPA, both lead compounds demonstrated blood-brain barrier penetration. Furthermore, stability was demonstrated by the 2V5Z-S5 complex by pi-pi stacking with Tyr398 and Tyr326. These results suggest that S5 and S16 are potent, reversible, selective MAO-B inhibitors that can be used as potential agents for the treatment of neurological disorders.
Sujet(s)
Inhibiteurs de la monoamine oxydase , Monoamine oxidase , Pipéridines , Inhibiteurs de la monoamine oxydase/pharmacologie , Inhibiteurs de la monoamine oxydase/composition chimique , Inhibiteurs de la monoamine oxydase/synthèse chimique , Monoamine oxidase/métabolisme , Pipéridines/pharmacologie , Pipéridines/composition chimique , Humains , Relation structure-activité , Pyridazines/composition chimique , Pyridazines/pharmacologie , Pyridazines/synthèse chimique , Simulation de docking moléculaire , Structure moléculaireRÉSUMÉ
Herein, we demonstrate an efficient method for multi-deuterium labelling of pirtobrutinib-a Bruton's tyrosine kinase inhibitor recently approved by the FDA-using a straightforward hydrogen isotope exchange (HIE) reaction. A remarkably high level of deuterium incorporation was achieved using an excess of a Kerr-type iridium catalyst. The key factor in the significant deuterium labelling was the decision to employ a deuterium uniformly labelled solvent, chlorobenzene-d5, at an elevated temperature. Virtually, no d0-d3 species were detected, with only traces of d4-d5 isotopomers (< 5%) observable in the mass spectrum of pirtobrutinib-d8, fulfilling requirements for stable isotope-labelled internal standard. The labelled compound-mainly consisting of isotopomers d6-d9 at 82.4% of the total abundance-was isolated in a high yield (73%) and purity (99%). Noteworthy, fluorine group acting as a directing group was observed for the first time. Significant incorporation of deuterium in ortho-positions, exceeding 87%, was observed. Interestingly, chlorinated solvent used in the HIE reactions was non-specifically deuterated yielding up to 0.42 deuterium per chlorobenzene molecule even at an exceptionally low iridium catalyst loading of 4.17 × 10-2 mol%.
Sujet(s)
Deutérium , Marquage isotopique , Deutérium/composition chimique , Pyrimidines/composition chimique , Pipéridines/composition chimiqueRÉSUMÉ
The objective of the current study is to prepare amorphous solid dispersions (ASDs) containing piperine (PIP) by utilizing organic acid glycyrrhizic acid (GA) and inorganic disordered mesoporous silica 244FP (MSN/244FP) as carriers and to investigate their dissolution mechanism. The physicochemical properties of ASDs were characterized with scanning electron microscopy (SEM), powder X-ray diffraction (PXRD), and differential scanning calorimetry (DSC). Fourier transform infrared spectroscopy (FTIR) and one-dimensional proton nuclear magnetic resonance (1H NMR) studies collectively proved that strong hydrogen-bonding interactions formed between PIP and the carriers in ASDs. Additionally, molecular dynamic (MD) simulation was conducted to simulate and predict the physical stability and dissolution mechanisms of the ASDs. Interestingly, it revealed a significant increase in the dissolution of amorphous PIP in ASDs in in vitro dissolution studies. Rapid dissolution of GA in pH 6.8 medium resulted in the immediate release of PIP drugs into a supersaturated state, acting as a dissolution-control mechanism. This exhibited a high degree of fitting with the pseudo-second-order dynamic model, with an R2 value of 0.9996. Conversely, the silanol groups on the outer surface of the MSN and its porous nanostructures enabled PIP to display a unique two-step drug release curve, indicating a diffusion-controlled mechanism. This curve conformed to the Ritger-Peppas model, with an R2 > 0.9. The results obtained provide a clear evidence of the proposed transition of dissolution mechanism within the same ASD system, induced by changes in the properties of carriers in a solution medium of varying pH levels.
Sujet(s)
Alcaloïdes , Benzodioxoles , Pipéridines , Amides gras polyinsaturés N-alkylés , Silice , Pipéridines/composition chimique , Benzodioxoles/composition chimique , Amides gras polyinsaturés N-alkylés/composition chimique , Alcaloïdes/composition chimique , Porosité , Silice/composition chimique , Acide glycyrrhizique/composition chimique , Solubilité , Simulation de dynamique moléculaire , Vecteurs de médicaments/composition chimique , Taille de particuleRÉSUMÉ
Drug solubility and dissolution remain a significant challenge in pharmaceutical formulations. This study aimed to formulate and evaluate repanglinide (RPG) nanosuspension-based buccal fast-dissolving films (BDFs) for dissolution enhancement. RPG nanosuspension was prepared by the antisolvent-precipitation method using multiple hydrophilic polymers, including soluplus®, polyvinyl alcohol, polyvinyl pyrrolidine, poloxamers, and hydroxyl propyl methyl cellulose. The nanosuspension was then directly loaded into BDFs using the solvent casting technique. Twelve formulas were prepared with a particle size range of 81.6-1389 nm and PDI 0.002-1 for the different polymers. Nanosuspensions prepared with soluplus showed a favored mean particle size of 82.6 ± 3.2 nm. The particles were spherical and non-aggregating, as demonstrated by SEM imaging. FTIR showed no interaction between soluplus and RPG. Faster dissolution occurred for the nanosuspension in comparison with pure RPG (complete release vs 60% within 30 min). The nanosuspension was successfully incorporated into BDFs. The optimum film formula showed 28 s disintegration time, and 97.3% RPG released within 10 min. Ex-vivo permeation profiles revealed improved RPG nanosuspension permeation with the cumulative amount of RPG permeated is103.4% ± 10.1 and a flux of 0.00275 mg/cm2/min compared to 39.3% ± 9.57 and a flux of 0.001058 mg/cm2/min for pure RPG. RPG was successfully formulated into nanosuspension that boosted drug dissolution and permeation. The selection of the ultimate NP formula was driven by optimal particle size, distribution, and drug content. Soluplus NPs were shown to be the successful formulations, which were further incorporated into a buccal film. The film was evaluated for ex-vivo permeation, confirming successful RPG formulation with improved performance compared to pure drugs.
Sujet(s)
Carbamates , Nanoparticules , Taille de particule , Pipéridines , Solubilité , Suspensions , Nanoparticules/composition chimique , Pipéridines/composition chimique , Pipéridines/administration et posologie , Pipéridines/pharmacocinétique , Carbamates/composition chimique , Carbamates/administration et posologie , Carbamates/pharmacocinétique , Animaux , Chimie pharmaceutique/méthodes , Libération de médicament , Polyvinyles/composition chimique , Polymères/composition chimique , Administration par voie buccale , Polyéthylène glycols/composition chimique , Préparation de médicament/méthodesRÉSUMÉ
Bedaquiline (BDQ), a first-in-class diarylquinoline anti-tuberculosis drug, and its analogue, TBAJ-587, prevent the growth and proliferation of Mycobacterium tuberculosis by inhibiting ATP synthase1,2. However, BDQ also inhibits human ATP synthase3. At present, how these compounds interact with either M. tuberculosis ATP synthase or human ATP synthase is unclear. Here we present cryogenic electron microscopy structures of M. tuberculosis ATP synthase with and without BDQ and TBAJ-587 bound, and human ATP synthase bound to BDQ. The two inhibitors interact with subunit a and the c-ring at the leading site, c-only sites and lagging site in M. tuberculosis ATP synthase, showing that BDQ and TBAJ-587 have similar modes of action. The quinolinyl and dimethylamino units of the compounds make extensive contacts with the protein. The structure of human ATP synthase in complex with BDQ reveals that the BDQ-binding site is similar to that observed for the leading site in M. tuberculosis ATP synthase, and that the quinolinyl unit also interacts extensively with the human enzyme. This study will improve researchers' understanding of the similarities and differences between human ATP synthase and M. tuberculosis ATP synthase in terms of the mode of BDQ binding, and will allow the rational design of novel diarylquinolines as anti-tuberculosis drugs.
Sujet(s)
Antituberculeux , Diarylquinoléines , Imidazoles , Mitochondrial Proton-Translocating ATPases , Mycobacterium tuberculosis , Pipéridines , Pyridines , Humains , Antituberculeux/pharmacologie , Antituberculeux/composition chimique , Sites de fixation , Cryomicroscopie électronique , Diarylquinoléines/composition chimique , Diarylquinoléines/pharmacologie , Imidazoles/composition chimique , Imidazoles/pharmacologie , Mitochondrial Proton-Translocating ATPases/antagonistes et inhibiteurs , Mitochondrial Proton-Translocating ATPases/composition chimique , Mitochondrial Proton-Translocating ATPases/métabolisme , Mitochondrial Proton-Translocating ATPases/ultrastructure , Modèles moléculaires , Mycobacterium tuberculosis/enzymologie , Mycobacterium tuberculosis/effets des médicaments et des substances chimiques , Pipéridines/composition chimique , Pipéridines/pharmacologie , Sous-unités de protéines/métabolisme , Sous-unités de protéines/composition chimique , Sous-unités de protéines/antagonistes et inhibiteurs , Pyridines/composition chimique , Pyridines/pharmacologieRÉSUMÉ
Bilastine, a new second generation antihistaminic drug, has been widely used for relieving symptoms of allergic rhinitis and urticaria without a sedative effect. A simple, cost-effective, and highly sensitive fluorimetric method was developed for the estimation of bilastine in human plasma, in addition to its pure state and tablets. The suggested method depended on binary complex formation of eosin with bilastine in a buffered medium at pH 4.2. The formed complex resulted in quantitative quenching of eosin emission at 538 nm after excitation at 335 nm. This method demonstrates a broad range of linearity, spanning from 200 to 1000 ng/mL, and exhibits exceptional sensitivity, with a limit of detection and quantitation of 30.85 and 93.48 ng/mL, respectively. In addition, this spectrofluorimetric method may be employed to determine the amount of bilastine in human plasma and tablets with satisfactory accuracy and excellent precision. Furthermore, the content uniformity of bilastine in commercially available tablets was successfully tested by this approach. Compared with the reference method, there were no significant variations in terms of precision or accuracy. In conclusion, the proposed protocol is highly recommended to quantitatively estimate bilastine in different quality control settings.
Sujet(s)
Benzimidazoles , Pipéridines , Spectrométrie de fluorescence , Comprimés , Humains , Pipéridines/sang , Pipéridines/composition chimique , Spectrométrie de fluorescence/méthodes , Benzimidazoles/sang , Benzimidazoles/composition chimique , Limite de détection , Éosine B/composition chimique , Concentration en ions d'hydrogèneRÉSUMÉ
Repaglinide (RPG) belongs to the class of drugs known as meglitinides and is used for improving and maintaining glycemic control in the treatment of patients with Type 2 diabetes. RPG is a Class II drug (BCS) because of its high permeability and low water solubility. It also undergoes hepatic first-pass metabolism. The oral bioavailability of RPG is low (about 56 %) due to these drawbacks. Our aim in this study is to prepare two different nano-sized drug carrier systems containing RPG (nanoparticle: RPG-PLGA-Zein-NPs or nanoemulsion: RPG-NE) and to carry out a pharmacokinetic study for these formulations. We prepared NPs using PLGA and Zein. In addition, a single NE formulation was developed using Tween 80 and Pluronic F68 as surfactants and Labrasol as co-surfactant. The droplet size values of the blank-NE and RPG-NE formulations were found to be less than 120 nm. The mean particle sizes of blank-Zein-PLGA-NPs and RPG-Zein-PLGA-NPs were less than 260 nm. The Cmax and tmax values of RPG-Zein-PLGA-NPs and RPG-NE (523 ± 65 ng/mL and 770 ± 91 ng/mL; 1.41 ± 0.46 h and 1.61 ± 0.37 h, respectively) were meaningfully higher than those of free RPG (280 ± 33 ng/mL; 0.72 ± 0.28 h) (p < 0.05). The AUC0-∞ values calculated for RPG-Zein-PLGA-NPs and RPG-NE were approximately 4.04 and 5.05 times higher than that calculated for free RPG. These nanosized drug delivery systems were useful in increasing the oral bioavailability of RPG. Moreover, the NE formulation was more effective than the NP formulation in improving the oral bioavailability of RPG (p < 0.05).
Sujet(s)
Carbamates , Émulsions , Hypoglycémiants , Nanoparticules , Pipéridines , Copolymère d'acide poly(lactique-co-glycolique) , Animaux , Carbamates/pharmacocinétique , Carbamates/composition chimique , Carbamates/administration et posologie , Nanoparticules/composition chimique , Nanoparticules/administration et posologie , Mâle , Pipéridines/pharmacocinétique , Pipéridines/administration et posologie , Pipéridines/composition chimique , Copolymère d'acide poly(lactique-co-glycolique)/composition chimique , Copolymère d'acide poly(lactique-co-glycolique)/pharmacocinétique , Hypoglycémiants/pharmacocinétique , Hypoglycémiants/administration et posologie , Hypoglycémiants/composition chimique , Taille de particule , Rats , Zéine/composition chimique , Zéine/pharmacocinétique , Vecteurs de médicaments/composition chimique , Vecteurs de médicaments/pharmacocinétique , Biodisponibilité , Tensioactifs/composition chimique , Tensioactifs/pharmacocinétique , Rat Sprague-Dawley , Rat Wistar , Poloxamère/composition chimique , Poloxamère/pharmacocinétique , Glycérides/composition chimique , Glycérides/pharmacocinétique , Préparation de médicament/méthodesRÉSUMÉ
Herein, we report the synthesis of new 4-amino-2-(piperidin-3-yl)isoindoline-1,3-diones and their biological evaluation in a series of in vitro experiments. The synthetic production of these materials was initiated upon the condensation of appropriate nitrophthalic acid derivatives with various 3-aminopiperidines; subsequent reduction provided the final products in moderate to good yields. Readily available chiral pool reagents facilitated entry into optically enriched samples, while the piperidine scaffold furnished a variety of amide and alkylated entries. In total, 16 candidates were produced, and their ensuing treatment in LPS-challenged RAW cells effected slight reductions in secreted TNF-α but provided more robust and dose-dependent declines in nitrite and IL-6 levels relative to basal amounts, all concurrent with maintenance of cellular viability across the concentration ranges screened. The secondary amine cohort including rac-6, (R)-7, and (S)-8 rendered the most pronounced dose-dependent reductions in nitrite and IL-6. When dosed at 30 µM, (R)-7 demonstrated the most compelling effects, with decreases of 32 % and 40 % for nitrite and IL-6, respectively. Notable reductions in the inflammatory markers were also observed for 19 which effected declines in TNF-α (14 %), nitrite (19 %), and IL-6 (11 %) when treated at 30 µM. Additionally, four representative compounds were further evaluated against numerous CNS receptors, channels, and transporters, with 6, 9, and 19 demonstrating varying degrees of nanomolar-to-low-micromolar binding to the σ-1 and σ-2 receptors and also to serotonin receptors 5HT2A, 5HT2B and 5HT3. In this regard, 6 displayed perhaps the most noteworthy affinities, with binding at σ-2 (Ki = 2.2uM), 5HT2B (Ki = 561 nM) and 5HT3 (Ki = 536 nM). Furthermore, no pronounced or dose-dependent Cereblon/DDB1 binding was observed for the screened representative compounds 6, 9, 18 and 19.
Sujet(s)
Inflammation , Lipopolysaccharides , Récepteurs sérotoninergiques , Récepteur sigma , Animaux , Lipopolysaccharides/pharmacologie , Lipopolysaccharides/antagonistes et inhibiteurs , Souris , Inflammation/traitement médicamenteux , Inflammation/métabolisme , Récepteurs sérotoninergiques/métabolisme , Récepteur sigma/métabolisme , Cellules RAW 264.7 , Pipéridines/composition chimique , Pipéridines/pharmacologie , Pipéridines/synthèse chimique , Relation dose-effet des médicaments , Structure moléculaire , Relation structure-activité , Interleukine-6/métabolisme , Survie cellulaire/effets des médicaments et des substances chimiques , Marqueurs biologiques/métabolismeRÉSUMÉ
The chemical structure of piperidine has a unique ability to combine with other molecular fragments. This fact makes it possible to actively use it as an effective basis for the creation of new drug-like substances. Thus, the aim of the current investigation was to study the acute toxicity, local anesthetic potency, and antiarrhythmic activity of the two new synthesized piperidine derivatives under laboratory codes LAS-286 and LAS-294 (local anesthetic substances). The Bulbring & Wajda animal model and method of determining the nociception threshold during electrical stimulation was used to investigate the action of the substance during infiltration anesthesia. An antiarrhythmic activity was observed by the aconitine-induced rat arrhythmia model. Additionally, these compounds were studied in relation to molecular docking to delineate the structure-activity relationships. The tested piperidine derivatives had a low toxicity in the subcutaneous and intravenous administration routes. The experimental results showed a higher prolonged and pronounced local anesthetic activity for LAS-286 at a 0.5% concentration, compared to the reference preparations. The low dosage of 0.1 mg/kg of LAS-294 demonstrated a pronounced preventive antiarrhythmic effect in 90% of cases on the development of mixed arrhythmia, caused by aconitine. The results of molecular docking confirmed a higher binding affinity of the tested piperidines with the Nav1.4 and Nav1.5 macromolecules. The results of the present study are very promising, because these piperidines have shown a high biological activity, which can suggest a potential therapeutic application in the future.
Sujet(s)
Anesthésiques locaux , Antiarythmiques , Simulation de docking moléculaire , Pipéridines , Animaux , Antiarythmiques/pharmacologie , Anesthésiques locaux/pharmacologie , Pipéridines/pharmacologie , Pipéridines/composition chimique , Rats , Mâle , Troubles du rythme cardiaque/induit chimiquement , Troubles du rythme cardiaque/traitement médicamenteux , Relation structure-activité , Rat Wistar , Modèles animaux de maladie humaineRÉSUMÉ
Piperine (PiP), a bioactive molecule, exhibits numerous health benefits and is frequently employed as a co-delivery agent with various phytomedicines (e.g., curcumin) to enhance their bioavailability. This is attributed to PiP's inhibitory activity against drug-metabolizing proteins, notably CYP3A4. Nevertheless, PiP encounters solubility challenges addressed in this study using cyclodextrins (CDs). Specifically, γ-CD and its derivatives, Hydroxypropyl-γ-CD (HP-γ-CD), and Octakis (6-O-sulfo)-γ-CD (Octakis-S-γ-CD), were employed to form supramolecular complexes with PiP. The conformational space of the complexes was assessed through 1 µs molecular dynamics simulations and umbrella sampling. Additionally, quantum mechanical calculations using wB97X-D dispersion-corrected DFT functional and 6-311 + G(d,p) basis set were conducted on the complexes to examine the thermodynamics and kinetic stability. Results indicated that Octakis-S-γ-CD exhibits superior host capabilities for PiP, with the most favorable complexation energy (-457.05 kJ/mol), followed by HP-γ-CD (-249.16 kJ/mol). Furthermore, two conformations of the Octakis-S-γ-CD/PiP complex were explored to elucidate the optimal binding orientation of PiP within the binding pocket of Octakis-S-γ-CD. Supramolecular chemistry relies significantly on non-covalent interactions. Therefore, our investigation extensively explores the critical atoms involved in these interactions, elucidating the influence of substituted groups on the stability of inclusion complexes. This comprehensive analysis contributes to emphasizing the γ-CD derivatives with improved host capacity.
Sujet(s)
Alcaloïdes , Benzodioxoles , Théorie de la fonctionnelle de la densité , Simulation de dynamique moléculaire , Pipéridines , Amides gras polyinsaturés N-alkylés , Thermodynamique , Amides gras polyinsaturés N-alkylés/composition chimique , Pipéridines/composition chimique , Alcaloïdes/composition chimique , Benzodioxoles/composition chimique , Cyclodextrines gamma/composition chimique , Cytochrome P-450 CYP3A/métabolisme , Cytochrome P-450 CYP3A/composition chimiqueRÉSUMÉ
Respiratory syncytial virus (RSV) is the major cause of bronchiolitis and pneumonia in young children and the elderly. There are currently no approved RSV-specific therapeutic small molecules available. Using high-throughput antiviral screening, we identified an oral drug, the prenylation inhibitor lonafarnib, which showed potent inhibition of the RSV fusion process. Lonafarnib exhibited antiviral activity against both the RSV A and B genotypes and showed low cytotoxicity in HEp-2 and human primary bronchial epithelial cells (HBEC). Time-of-addition and pseudovirus assays demonstrated that lonafarnib inhibits RSV entry, but has farnesyltransferase-independent antiviral efficacy. Cryo-electron microscopy revealed that lonafarnib binds to a triple-symmetric pocket within the central cavity of the RSV F metastable pre-fusion conformation. Mutants at the RSV F sites interacting with lonafarnib showed resistance to lonafarnib but remained fully sensitive to the neutralizing monoclonal antibody palivizumab. Furthermore, lonafarnib dose-dependently reduced the replication of RSV in BALB/c mice. Collectively, lonafarnib could be a potential fusion inhibitor for RSV infection.
Sujet(s)
Pyridines , Infections à virus respiratoire syncytial , Virus respiratoire syncytial humain , Protéines de fusion virale , Humains , Infections à virus respiratoire syncytial/traitement médicamenteux , Infections à virus respiratoire syncytial/génétique , Pyridines/pharmacologie , Souris , Animaux , Virus respiratoire syncytial humain/effets des médicaments et des substances chimiques , Virus respiratoire syncytial humain/génétique , Protéines de fusion virale/génétique , Protéines de fusion virale/antagonistes et inhibiteurs , Farnesyltranstransferase/antagonistes et inhibiteurs , Farnesyltranstransferase/génétique , Antiviraux/pharmacologie , Antiviraux/composition chimique , Pipéridines/pharmacologie , Pipéridines/composition chimique , Souris de lignée BALB C , Conformation des protéines , DibenzocycloheptènesRÉSUMÉ
As a subtype of the 5-hydroxytryptamine (5-HT) receptor, 5-HT1A receptors are involved in the pathological process of psychiatric disorders and is an important target for antidepressants. The research groups focus on these area have tried to design novel compounds to alleviate depression by targeting 5-HT1A receptor. The heterocyclic structures is an important scaffold to enhance the antidepressant activity of ligands, including piperazine, piperidine, benzothiazole, and pyrrolidone. The current review highlights the function and significance of nitrogen-based heterocyclics 5-HT1AR represented by piperazine, piperidine, benzothiazole, and pyrrolidone in the development of antidepressant.
Sujet(s)
Antidépresseurs , Récepteur de la sérotonine de type 5-HT1A , Agonistes des récepteurs 5-HT1 de la sérotonine , Humains , Agonistes des récepteurs 5-HT1 de la sérotonine/pharmacologie , Agonistes des récepteurs 5-HT1 de la sérotonine/usage thérapeutique , Antidépresseurs/pharmacologie , Antidépresseurs/usage thérapeutique , Récepteur de la sérotonine de type 5-HT1A/effets des médicaments et des substances chimiques , Récepteur de la sérotonine de type 5-HT1A/métabolisme , Pipérazines/pharmacologie , Pipérazines/composition chimique , Benzothiazoles/pharmacologie , Benzothiazoles/composition chimique , Composés hétérocycliques/pharmacologie , Composés hétérocycliques/composition chimique , Composés hétérocycliques/synthèse chimique , Composés hétérocycliques/usage thérapeutique , Pipéridines/pharmacologie , Pipéridines/usage thérapeutique , Pipéridines/composition chimique , Pyrrolidones/pharmacologie , Pyrrolidones/usage thérapeutique , Pyrrolidones/composition chimique , Dépression/traitement médicamenteuxRÉSUMÉ
Piperine (PIP) has been known for its pharmacological activities with low water solubility and poor dissolution, which limits its nutritional application. The purpose of this research was to enhance PIP stability, dispersibility and biological activity by preparing PIP nanoparticles using the wet-media milling approach combined with nanosuspension solidification methods of spray/freeze drying. Octenyl succinic anhydride (OSA)-modified waxy maize starch was applied as the stabilizer to suppress aggregation of PIP nanoparticles. The particle size, redispersibility, storage stability and in vitro release behavior of PIP nanoparticles were measured. The regulating effect on adipocyte differentiation was evaluated using 3T3-L1 cell model. Results showed that PIP nanoparticles had a reduced particle size of 60 ± 1 nm, increased release rate in the simulated gastric (SGF) and intestinal fluids (SIF) and enhanced inhibition effect on adipogenesis in 3T3-L1 cells compared with free PIP, indicating that PIP-loaded nanoparticles with improved stability and anti-adipogenic property were developed successfully by combining wet-media milling and drying methods.
Sujet(s)
Cellules 3T3-L1 , Adipocytes , Adipogenèse , Alcaloïdes , Benzodioxoles , Nanoparticules , Pipéridines , Amides gras polyinsaturés N-alkylés , Amidon , Animaux , Souris , Nanoparticules/composition chimique , Amides gras polyinsaturés N-alkylés/composition chimique , Amides gras polyinsaturés N-alkylés/pharmacologie , Benzodioxoles/pharmacologie , Benzodioxoles/composition chimique , Pipéridines/pharmacologie , Pipéridines/composition chimique , Adipogenèse/effets des médicaments et des substances chimiques , Alcaloïdes/composition chimique , Alcaloïdes/pharmacologie , Adipocytes/effets des médicaments et des substances chimiques , Amidon/composition chimique , Amidon/analogues et dérivés , Taille de particule , Libération de médicament , Différenciation cellulaire/effets des médicaments et des substances chimiquesRÉSUMÉ
hERG channel screening has been achieved based on electrical impedance tomography and extracellular voltage activation (EIT-EVA) to improve the non-invasive aspect of drug discovery. EIT-EVA screens hERG channels by considering the change in extracellular ion concentration which modifies the extracellular resistance in cell suspension. The rate of ion passing in cell suspension is calculated from the extracellular resistance Rex, which is obtained from the EIT measurement at a frequency of 500 kHz. In the experiment, non-invasive screening is applied by a novel integrated EIT-EVA printed circuit board (PCB) sensor to human embryonic kidney (HEK) 293 cells transfected with the human ether-a-go-go-related gene (hERG) ion channel, while the E-4031 antiarrhythmic drug is used for hERG channel inhibition. The extracellular resistance Rex of the HEK 293 cells suspension is measured by EIT as the hERG channels are activated by EVA over time. The Rex is reconstructed into extracellular conductivity distribution change Δσ to reflect the extracellular K+ ion concentration change Δc resulting from the activated hERG channel. Δc is increased rapidly during the hERG channel non-inhibition state while Δc is increased slower with increasing drug concentration cd. In order to evaluate the EIT-EVA system, the inhibitory ratio index (IR) was calculated based on the rate of Δc over time. Half-maximal inhibitory concentration (IC50) of 2.7 nM is obtained from the cd and IR dose-response relationship. The IR from EIT-EVA is compared with the results from the patch-clamp method, which gives R2 of 0.85. In conclusion, EIT-EVA is successfully applied to non-invasive hERG channel screening.
Sujet(s)
Impédance électrique , Canaux potassiques éther-à-go-go , Humains , Cellules HEK293 , Canaux potassiques éther-à-go-go/métabolisme , Canaux potassiques éther-à-go-go/antagonistes et inhibiteurs , Tomographie/instrumentation , Canal potassique ERG1/métabolisme , Canal potassique ERG1/antagonistes et inhibiteurs , Pipéridines/pharmacologie , Pipéridines/composition chimique , Pyridines/pharmacologie , Pyridines/composition chimiqueRÉSUMÉ
Inhibition of human dihydroorotate dehydrogenase (hDHODH) represents a promising strategy for suppressing the proliferation of cancer cells. To identify novel and potent hDHODH inhibitors, a total of 28 piperine derivatives were designed and synthesized. Their cytotoxicities against three human cancer cell lines (NCI-H226, HCT-116, and MDA-MB-231) and hDHODH inhibitory activities were also evaluated. Among them, compound H19, exhibited the strongest inhibitory activities (NCI-H226 IC50 = 0.95 µM, hDHODH IC50 = 0.21 µM). Further pharmacological investigations revealed that H19 exerted anticancer effects by inducing ferroptosis in NCI-H226 cells, with its cytotoxicity being reversed by ferroptosis inhibitors. This was supported by the intracellular growth or decline of ferroptosis markers, including lipid peroxidation, Fe2+, GSH, and 4-HNE. Overall, H19 emerges as a promising hDHODH inhibitor with potential anticancer properties warranting development.
Sujet(s)
Alcaloïdes , Antinéoplasiques , Benzodioxoles , Prolifération cellulaire , Dihydroorotate dehydrogenase , Tests de criblage d'agents antitumoraux , Antienzymes , Ferroptose , Pipéridines , Amides gras polyinsaturés N-alkylés , Humains , Alcaloïdes/pharmacologie , Alcaloïdes/composition chimique , Alcaloïdes/synthèse chimique , Dihydroorotate dehydrogenase/antagonistes et inhibiteurs , Pipéridines/pharmacologie , Pipéridines/composition chimique , Pipéridines/synthèse chimique , Benzodioxoles/pharmacologie , Benzodioxoles/synthèse chimique , Benzodioxoles/composition chimique , Antinéoplasiques/pharmacologie , Antinéoplasiques/composition chimique , Antinéoplasiques/synthèse chimique , Antienzymes/pharmacologie , Antienzymes/composition chimique , Antienzymes/synthèse chimique , Relation structure-activité , Ferroptose/effets des médicaments et des substances chimiques , Prolifération cellulaire/effets des médicaments et des substances chimiques , Amides gras polyinsaturés N-alkylés/pharmacologie , Amides gras polyinsaturés N-alkylés/composition chimique , Amides gras polyinsaturés N-alkylés/synthèse chimique , Structure moléculaire , Relation dose-effet des médicaments , Découverte de médicament , Lignée cellulaire tumoraleRÉSUMÉ
Piperine, derived from black pepper (Piper nigrum L.), is responsible for the pungent sensation. The diverse bioactivities of piperine underscores its promising potential as a functional food ingredient. This review presents a comprehensive overview of the research progress in extraction, synthesis, pungency transduction mechanism and bioactivities of piperine. Piperine can be extracted through various methods, such as traditional, modern, and innovative extraction techniques. Its synthesis mainly included both chemical and biosynthetic approaches. It exhibits a diverse range of bioactivities, including anticancer, anticonvulsant, antidepressant, anti-inflammatory, antioxidant, immunomodulatory, anti-obesity, neuroprotective, antidiabetic, hepatoprotective, and cardiovascular protective activities. Piperine can bind to TRPV1 receptor to elicit pungent sensation. Overall, the present review can provide a theoretical reference for advancing the potential application of piperine in the field of food science.
Sujet(s)
Alcaloïdes , Benzodioxoles , Piper nigrum , Pipéridines , Extraits de plantes , Amides gras polyinsaturés N-alkylés , Piper nigrum/composition chimique , Amides gras polyinsaturés N-alkylés/pharmacologie , Amides gras polyinsaturés N-alkylés/composition chimique , Benzodioxoles/pharmacologie , Benzodioxoles/composition chimique , Pipéridines/pharmacologie , Pipéridines/composition chimique , Alcaloïdes/pharmacologie , Alcaloïdes/composition chimique , Humains , Animaux , Extraits de plantes/composition chimique , Extraits de plantes/pharmacologieRÉSUMÉ
Poly ADP-ribose polymerase (PARP) plays an important role in the DNA repair process and has become an attractive target for cancer therapy in recent years. Given that niraparib has good clinical efficacy as a PARP inhibitor, this study aimed to develop radiolabeled niraparib derivatives for tumor imaging to detect PARP expression and improve the accuracy of stratified patient therapy. The niraparib isonitrile derivative (CNPN) was designed, synthesized, and radiolabeled to obtain the [99mTc]Tc-CNPN complex with high radiochemical purity (>95%). It was lipophilic and stable in vitro. In HeLa cell experiments, the uptake of [99mTc]Tc-CNPN was effectively inhibited by the ligand CNPN, indicating the binding affinity for PARP. According to the biodistribution studies of HeLa tumor-bearing mice, [99mTc]Tc-CNPN has moderate tumor uptake and can be effectively inhibited, demonstrating its specificity for targeting PARP. The SPECT imaging results showed that [99mTc]Tc-CNPN had tumor uptake at 2 h postinjection. All of the results of this study indicated that [99mTc]Tc-CNPN is a promising tumor imaging agent that targets PARP.
Sujet(s)
Indazoles , Pipéridines , Inhibiteurs de poly(ADP-ribose) polymérases , Animaux , Humains , Souris , Pipéridines/composition chimique , Pipéridines/pharmacocinétique , Indazoles/composition chimique , Indazoles/pharmacocinétique , Cellules HeLa , Inhibiteurs de poly(ADP-ribose) polymérases/pharmacocinétique , Inhibiteurs de poly(ADP-ribose) polymérases/pharmacologie , Inhibiteurs de poly(ADP-ribose) polymérases/composition chimique , Distribution tissulaire , Tomographie par émission monophotonique/méthodes , Radiopharmaceutiques/pharmacocinétique , Radiopharmaceutiques/composition chimique , Poly (ADP-Ribose) polymerase-1/métabolisme , Femelle , Technétium/composition chimique , Nitriles/composition chimique , Nitriles/pharmacocinétique , Souris nude , Souris de lignée BALB CRÉSUMÉ
Docetaxel (DTX) resistance poses a significant challenge in the treatment of prostate cancer (PCa), often leading to chemotherapy failure. This study investigates the ability of piperine, a compound derived from black pepper, to enhance the sensitivity of PCa cells to DTX and elucidates its underlying mechanism. We established a DTX-resistant PCa cell line, DU145/DTX, to conduct our experiments. Through a series of assays, including MTT for cell viability, flow cytometry for apoptosis, Transwell for cell migration and invasion, and western blot for protein expression analysis, we assessed the effects of piperine on these cellular functions and on the Notch signaling pathway components. Our results demonstrated that we successfully established the DTX-resistant PCa cell line DU145/DTX. Piperine effectively decreased the viability of both DU145 and its DTX-resistant counterpart, DU145/DTX, in a concentration and time-dependent manner when used alone and in combination with DTX. Notably, piperine also induced apoptosis and reduced the migration and invasion capabilities of these cells. At the molecular level, piperine down-regulated the Notch pathway by inhibiting Notch1 and Jagged1 signaling, as well as reducing the expression of downstream effectors Hey1 and hes family bHLH transcription factor 1. The study concludes that piperine's ability to modulate the Notch signaling pathway and induce apoptosis highlights its potential as a complementary treatment for DTX-resistant PCa, paving the way for the use of traditional Chinese medicinal compounds in modern oncology treatment strategies.
Sujet(s)
Alcaloïdes , Apoptose , Benzodioxoles , Mouvement cellulaire , Docetaxel , Résistance aux médicaments antinéoplasiques , Pipéridines , Amides gras polyinsaturés N-alkylés , Tumeurs de la prostate , Transduction du signal , Amides gras polyinsaturés N-alkylés/pharmacologie , Amides gras polyinsaturés N-alkylés/composition chimique , Humains , Benzodioxoles/pharmacologie , Benzodioxoles/composition chimique , Alcaloïdes/pharmacologie , Alcaloïdes/composition chimique , Pipéridines/pharmacologie , Pipéridines/composition chimique , Docetaxel/pharmacologie , Mâle , Lignée cellulaire tumorale , Transduction du signal/effets des médicaments et des substances chimiques , Résistance aux médicaments antinéoplasiques/effets des médicaments et des substances chimiques , Tumeurs de la prostate/traitement médicamenteux , Tumeurs de la prostate/métabolisme , Tumeurs de la prostate/anatomopathologie , Apoptose/effets des médicaments et des substances chimiques , Mouvement cellulaire/effets des médicaments et des substances chimiques , Récepteurs Notch/métabolisme , Antinéoplasiques/pharmacologie , Antinéoplasiques/composition chimique , Survie cellulaire/effets des médicaments et des substances chimiques , Récepteur Notch1/métabolismeRÉSUMÉ
Aim: To design and synthesize a novel series of 1-aryldonepezil analogues. Materials & methods: The 1-aryldonepezil analogues were synthesized through palladium/PCy3-catalyzed Suzuki reaction and were evaluated for cholinesterase inhibitory activities and neuroprotective effects. In silico docking of the most effective compound was conducted. Results: The 4-tert-butylphenyl analogue exhibited good inhibitory potency against acetylcholinesterase and butyrylcholinesterase and had a favorable neuroprotective effect on H2O2-induced SH-SY5Y cell injury. Conclusion: The 4-tert-butylphenyl derivative is a promising lead compound for anti-Alzheimer's disease drug development.
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