3034-50-2 Archives - Page 10 of 15 - Imidazoles-derivatives

Chen, Bo-Ru team published research on Chinese Journal of Natural Medicines (Amsterdam, Netherlands) in 2022 | 3034-50-2

Category: imidazoles-derivatives, 1H-Imidazole-4-carbaldehyde, also known as 1H-Imidazole-4-carbaldehyde, is a useful research compound. Its molecular formula is C4H4N2O and its molecular weight is 96.09 g/mol. The purity is usually 95%.
The starting material for a practical synthesis of a potent C17,20-lyase inhibitor. The lyase is a key enzyme in androgen biosynthesis as well as a target for treatment of androgen-dependent prostate cancer. Used to synthesize potent antimalarial drug.
1H-Imidazole-4-carbaldehyde is a chemical compound that has been shown to bind to the glucocorticoid receptor. It was synthesized by reacting 1,2-diaminobenzene with formaldehyde and then hydrolyzing the intermediate imidazolium salt, which is stable in acidic solutions. The complex can be prepared by mixing two solutions of imidazole and trifluoroacetic acid. The ligand has a redox potential of -0.1 V (vs NHE). This means it can be oxidized to the carbonyl group or reduced back to the imidazole ring. The compound is stable in neutral solution and forms stable complexes with metal ions such as Cu+, Fe3+, and Zn2+. It also coordinates well with oxygen atoms, nitrogen atoms, and water molecules. 1H-Imidazole-4-carbaldehyde has been shown to bind to glucocortic, 3034-50-2.

Imidazole is a heterocyclic compound with a five-membered planar ring. It is amphoteric and highly polar. 3034-50-2, formula is C4H4N2O, Name is Imidazole-4-carbaldehyde. The pharmacophore of imidazole exists in bioactive compounds including amino acids, plant growth regulators and therapeutic agents. Category: imidazoles-derivatives.

Chen, Bo-Ru;Gao, Cheng-Long;Liu, Jin;Guo, Yue-Wei;Jiang, Jian-Lan;Pang, Tao;Li, Xu-Wen research published 《 Diversity-oriented synthesis of marine sponge derived hyrtioreticulins and their anti-inflammatory activities》, the research content is summarized as follows. Diversity-oriented synthesis is aimed to increase the chem. diversity of target natural products for extensive biol. activity evaluation. Indole ring is an important functional group in a large number of drugs and other biol. active agents, and indole-containing natural products have been frequently isolated from marine sources in recent years. In this paper, a series of indole-containing marine natural hyrtioreticulin derivatives, including 19 new ones, were designed, synthesized through a key Pictet-Spengler reaction, and evaluated for their inflammation related activity. Compound 13b displayed the most promising activity by inhibiting TNF-α cytokine release with an inhibitory rate of 92% at a concentration of 20 μmol·L^-1. A preliminary structure-activity relationship anal. was also discussed. This research may throw light on the discovery of marine indole alkaloid derived anti-inflammatory drug leads.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Chen, Long team published research on Acta Pharmaceutica Sinica B in 2022 | 3034-50-2

Safety of Imidazole-4-carbaldehyde, 1H-Imidazole-4-carbaldehyde, also known as 1H-Imidazole-4-carbaldehyde, is a useful research compound. Its molecular formula is C4H4N2O and its molecular weight is 96.09 g/mol. The purity is usually 95%.
The starting material for a practical synthesis of a potent C17,20-lyase inhibitor. The lyase is a key enzyme in androgen biosynthesis as well as a target for treatment of androgen-dependent prostate cancer. Used to synthesize potent antimalarial drug.
1H-Imidazole-4-carbaldehyde is a chemical compound that has been shown to bind to the glucocorticoid receptor. It was synthesized by reacting 1,2-diaminobenzene with formaldehyde and then hydrolyzing the intermediate imidazolium salt, which is stable in acidic solutions. The complex can be prepared by mixing two solutions of imidazole and trifluoroacetic acid. The ligand has a redox potential of -0.1 V (vs NHE). This means it can be oxidized to the carbonyl group or reduced back to the imidazole ring. The compound is stable in neutral solution and forms stable complexes with metal ions such as Cu+, Fe3+, and Zn2+. It also coordinates well with oxygen atoms, nitrogen atoms, and water molecules. 1H-Imidazole-4-carbaldehyde has been shown to bind to glucocortic, 3034-50-2.

Imidazole derivatives generally have good solubility in protic solvents. Simple imidazole derivatives, such as 1H-imidazole, 2-methyl-1H-imidazole, and 1,2-dimethylimidazole, have very high solubility in water. 3034-50-2, formula is C4H4N2O, Name is Imidazole-4-carbaldehyde. Their solubility in alcohol is lower than that in water and decreases with increasing molecular weight of the alcohols . Safety of Imidazole-4-carbaldehyde.

Chen, Long;Zhang, Jing;Wang, Xinjing;Li, Yu;Zhou, Lu;Lu, Xiongxiong;Dong, Guoqiang;Sheng, Chunquan research published 《 Discovery of novel KRAS-PDEδ inhibitors with potent activity in patient-derived human pancreatic tumor xenograft models》, the research content is summarized as follows. KRAS-PDEδ interaction is revealed as a promising target for suppressing the function of mutant KRAS. The bottleneck in clin. development of PDEδ inhibitors is the poor antitumor activity of known chemotypes. Here, we identified novel spiro-cyclic PDEδ inhibitors with potent antitumor activity both in vitro and in vivo. In particular, compound 36l (KD = 127 ± 16 nmol/L) effectively bound to PDEδ and interfered with KRAS-PDEδ interaction. It influenced the distribution of KRAS in Mia PaCa-2 cells, downregulated the phosphorylation of t-ERK and t-AKT and promoted apoptosis of the cells. The novel inhibitor 36l exhibited significant in vivo antitumor potency in pancreatic cancer patient-derived xenograft (PDX) models. It represents a promising lead compound for investigating the druggability of KRAS-PDEδ interaction.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Boureghda, Chaima team published research on Tetrahedron Letters in 2021 | 3034-50-2

Recommanded Product: Imidazole-4-carbaldehyde, 1H-Imidazole-4-carbaldehyde, also known as 1H-Imidazole-4-carbaldehyde, is a useful research compound. Its molecular formula is C4H4N2O and its molecular weight is 96.09 g/mol. The purity is usually 95%.
The starting material for a practical synthesis of a potent C17,20-lyase inhibitor. The lyase is a key enzyme in androgen biosynthesis as well as a target for treatment of androgen-dependent prostate cancer. Used to synthesize potent antimalarial drug.
1H-Imidazole-4-carbaldehyde is a chemical compound that has been shown to bind to the glucocorticoid receptor. It was synthesized by reacting 1,2-diaminobenzene with formaldehyde and then hydrolyzing the intermediate imidazolium salt, which is stable in acidic solutions. The complex can be prepared by mixing two solutions of imidazole and trifluoroacetic acid. The ligand has a redox potential of -0.1 V (vs NHE). This means it can be oxidized to the carbonyl group or reduced back to the imidazole ring. The compound is stable in neutral solution and forms stable complexes with metal ions such as Cu+, Fe3+, and Zn2+. It also coordinates well with oxygen atoms, nitrogen atoms, and water molecules. 1H-Imidazole-4-carbaldehyde has been shown to bind to glucocortic, 3034-50-2.

Imidazole based anticancer drug find applications in cancer chemotherapy. 3034-50-2, formula is C4H4N2O, Name is Imidazole-4-carbaldehyde. It is used as buffer component for purification of the histidine tagged recombinant proteins in immobilized metal-affinity chromatography (IMAC). Recommanded Product: Imidazole-4-carbaldehyde.

Boureghda, Chaima;Boulcina, Raouf;Dorcet, Vincent;Berree, Fabienne;Carboni, Bertrand;Debache, Abdelmadjid research published 《 Facile synthesis of 5-arylidene rhodanine derivatives using Na₂SO₃ as an eco-friendly catalyst. Access to 2-mercapto-3-aryl-acrylic acids and a benzoxaborole derivative》, the research content is summarized as follows. A simple, efficient and environment-friendly procedure for the synthesis of 5-arylidene rhodanines derivatives via a Knoevenagel type reaction was developed using rhodanine, a variety of differently substituted aldehydes and Na₂SO₃ as benign catalyst in ethanol. Selected 5-arylidene rhodanines were subjected to basic hydrolysis to afford 2-mercapto-3-substituted-acrylic acids. The presence of a boronic acid group is well tolerated in such transformations. In the case of 2-formylphenylboronic acid, this sequence opens access to a new benzoxaborole derivative (I → II).

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Caciolla, Jessica team published research on European Journal of Medicinal Chemistry in 2021 | 3034-50-2

3034-50-2, 1H-Imidazole-4-carbaldehyde, also known as 1H-Imidazole-4-carbaldehyde, is a useful research compound. Its molecular formula is C4H4N2O and its molecular weight is 96.09 g/mol. The purity is usually 95%.
The starting material for a practical synthesis of a potent C17,20-lyase inhibitor. The lyase is a key enzyme in androgen biosynthesis as well as a target for treatment of androgen-dependent prostate cancer. Used to synthesize potent antimalarial drug.
1H-Imidazole-4-carbaldehyde is a chemical compound that has been shown to bind to the glucocorticoid receptor. It was synthesized by reacting 1,2-diaminobenzene with formaldehyde and then hydrolyzing the intermediate imidazolium salt, which is stable in acidic solutions. The complex can be prepared by mixing two solutions of imidazole and trifluoroacetic acid. The ligand has a redox potential of -0.1 V (vs NHE). This means it can be oxidized to the carbonyl group or reduced back to the imidazole ring. The compound is stable in neutral solution and forms stable complexes with metal ions such as Cu+, Fe3+, and Zn2+. It also coordinates well with oxygen atoms, nitrogen atoms, and water molecules. 1H-Imidazole-4-carbaldehyde has been shown to bind to glucocortic, Quality Control of 3034-50-2

Imidazole Biochem/physiol Actions: Imidazole derivatives have antibacterial, antifungal and anticancer functionality. It interacts with DNA and also binds to protein and stops cell division. 3034-50-2, formula is C4H4N2O, Name is Imidazole-4-carbaldehyde. It also acts as a microtubule destabilizing agents and inhibits topoisomerase and Cytochrome P450 Family 26 Subfamily A Member 1 (CYP26A1) enzymes. Quality Control of 3034-50-2.

Caciolla, Jessica;Martini, Silvia;Spinello, Angelo;Pavlin, Matic;Turrini, Eleonora;Simonelli, Federica;Belluti, Federica;Rampa, Angela;Bisi, Alessandra;Fimognari, Carmela;Zaffaroni, Nadia;Gobbi, Silvia;Magistrato, Alessandra research published 《 Balanced dual acting compounds targeting aromatase and estrogen receptor α as an emerging therapeutic opportunity to counteract estrogen responsive breast cancer》, the research content is summarized as follows. Breast Cancer (BC) is a leading cause of death in women, currently affecting 13% of female population worldwide. First-line clin. treatments against Estrogen Receptor pos. (ER+) BC rely on suppressing estrogen production, by inhibiting the aromatase (AR) enzyme, or on blocking estrogen-dependent pro-oncogenic signaling, by targeting Estrogen Receptor (ER) α with selective Modulators/Degraders (SERMs/SERDs). The development of dual acting mols. targeting AR and ERα represents a tantalizing alternative strategy to fight ER + BC, reducing the incidence of adverse effects and resistance onset that limit the effectiveness of these gold-standard therapies. Here, in silico design, synthesis, biol. evaluation and an at.-level characterization of the binding and inhibition mechanism of twelve structurally related drug-candidates enable the discovery of multiple compounds active on both AR and ERα in the sub-μM range. The best drug-candidate 3a displayed a balanced low-nanomolar IC₅₀ towards the two targets, SERM activity and moderate selectivity towards a BC cell line. Moreover, most of the studied compounds reduced ERα levels, suggesting a potential SERD activity. This study dissects the key structural traits needed to obtain optimal dual acting drug-candidates, showing that multitarget compounds may be a viable therapeutic option to counteract ER + BC.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Bargan, Alexandra team published research on Polyhedron in 2020 | 3034-50-2

HPLC of Formula: 3034-50-2, 1H-Imidazole-4-carbaldehyde, also known as 1H-Imidazole-4-carbaldehyde, is a useful research compound. Its molecular formula is C4H4N2O and its molecular weight is 96.09 g/mol. The purity is usually 95%.
The starting material for a practical synthesis of a potent C17,20-lyase inhibitor. The lyase is a key enzyme in androgen biosynthesis as well as a target for treatment of androgen-dependent prostate cancer. Used to synthesize potent antimalarial drug.
1H-Imidazole-4-carbaldehyde is a chemical compound that has been shown to bind to the glucocorticoid receptor. It was synthesized by reacting 1,2-diaminobenzene with formaldehyde and then hydrolyzing the intermediate imidazolium salt, which is stable in acidic solutions. The complex can be prepared by mixing two solutions of imidazole and trifluoroacetic acid. The ligand has a redox potential of -0.1 V (vs NHE). This means it can be oxidized to the carbonyl group or reduced back to the imidazole ring. The compound is stable in neutral solution and forms stable complexes with metal ions such as Cu+, Fe3+, and Zn2+. It also coordinates well with oxygen atoms, nitrogen atoms, and water molecules. 1H-Imidazole-4-carbaldehyde has been shown to bind to glucocortic, 3034-50-2.

Imidazole is a five-membered heterocyclic moiety that possesses three carbon, two nitrogen, four hydrogen atoms, and two double bonds. 3034-50-2, formula is C4H4N2O, Name is Imidazole-4-carbaldehyde. It is also known as 1, 3-diazole. It contains two nitrogen atoms, in which one nitrogen bear a hydrogen atom, and the other is called pyrrole type nitrogen. HPLC of Formula: 3034-50-2.

Bargan, Alexandra;Cazacu, Maria;Dascalu, Mihaela;Macsim, Ana-Maria;Soroceanu, Alina;Macsim, Ioan Florin research published 《 Synthesis, structural characterization and properties evaluation of two new zwitterionic siloxane compounds》, the research content is summarized as follows. 1,3-Bis(3-aminopropyl)tetramethyldisiloxane is a valuable tool for the introduction of siloxane segments into different organic-inorganic structures. This paper demonstrates how 1,3-bis(3-aminopropyl)tetramethyldisiloxane can easily form crystalline salts with different counterparts with which it comes into contact. Thus, in the reaction chamber 1,3-bis(3-ammoniumpropyl)tetramethyldisiloxane chloride and nitrate were formed in the detriment of one stage metal (Ni and Cu) complexes of Schiff’s base with 4-imidazole carboxaldehyde. The salt products were isolated in crystalline state and were structurally characterized by single-crystal x-ray diffraction, elemental and spectral (FTIR, ¹H NMR) anal. The thermal and moisture stability as well as the aggregation ability in solution and sorption capacity for certain mols. were evaluated by adequate techniques.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Benson, Nicole team published research on Journal of Organic Chemistry in 2019 | 3034-50-2

Benson, Nicole;Suleiman, Olabisi;Odoh, Samuel O.;Woydziak, Zachary R. research published 《 Pyrazole, Imidazole, and Isoindolone Dipyrrinone Analogues: pH-Dependent Fluorophores That Red-Shift Emission Frequencies in a Basic Solution》, the research content is summarized as follows. Dipyrrinones are nonfluorescent yellow-pigmented constituents of bilirubin that undergo Z to E isomerization when excited with UV/blue light. Mech. restriction of the E/Z isomerization process results in highly fluorescent compounds such as N,N-methylene-bridged dipyrrinones and xanthoglows. This manuscript describes the first examples of dipyrrinone analogs, which exhibit fluorescence without covalently linking the pyrrole-pyrrolidine nitrogen atoms. Instead these analogs restrict E/Z isomerization through intramol. hydrogen bonding, resulting in mild to moderately fluorescent compounds (Φ_F = 0.01-0.30). Further, in basic solutions (pH > 12), the dipyrrinone analogs readily deprotonate and absorption/emission profiles of the fluorophores red-shifts by 10-49 nm. Directly from com. materials, 10 analogs were prepared in 41-96% yields in one step. To estimate the capacity of which intramol. hydrogen bonding has upon restricting the E/Z isomerization process, conformational energies of all analogs, in both the protonated and deprotonated species, were explored by using quantum-mech. d. functional theory (DFT) and time-dependent DFT calculations The computed strengths of the intramol. hydrogen bonds are related to the barriers of rotation about the 5-6 bond and both correlate with the exptl. measured fluorescence quantum yields.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Benson, Nicole team published research on Journal of Visualized Experiments in 2021 | 3034-50-2

Reference of 3034-50-2, 1H-Imidazole-4-carbaldehyde, also known as 1H-Imidazole-4-carbaldehyde, is a useful research compound. Its molecular formula is C4H4N2O and its molecular weight is 96.09 g/mol. The purity is usually 95%.
The starting material for a practical synthesis of a potent C17,20-lyase inhibitor. The lyase is a key enzyme in androgen biosynthesis as well as a target for treatment of androgen-dependent prostate cancer. Used to synthesize potent antimalarial drug.
1H-Imidazole-4-carbaldehyde is a chemical compound that has been shown to bind to the glucocorticoid receptor. It was synthesized by reacting 1,2-diaminobenzene with formaldehyde and then hydrolyzing the intermediate imidazolium salt, which is stable in acidic solutions. The complex can be prepared by mixing two solutions of imidazole and trifluoroacetic acid. The ligand has a redox potential of -0.1 V (vs NHE). This means it can be oxidized to the carbonyl group or reduced back to the imidazole ring. The compound is stable in neutral solution and forms stable complexes with metal ions such as Cu+, Fe3+, and Zn2+. It also coordinates well with oxygen atoms, nitrogen atoms, and water molecules. 1H-Imidazole-4-carbaldehyde has been shown to bind to glucocortic, 3034-50-2.

Benson, Nicole;Davis, Adam;Woydziak, Zachary R. research published 《 Synthesis of pH dependent pyrazole, imidazole, and isoindolone dipyrrinone fluorophores using a Claisen-Schmidt condensation approach》, the research content is summarized as follows. Methine-bridged conjugated bicyclic aromatic compounds are common constituents of a range of biol. relevant mols. such as porphyrins, dipyrrinones, and pharmaceuticals. Addnl., restricted rotation of these systems often results in highly to moderately fluorescent systems as observed in 3H,5H-dipyrrolo[1,2-c:2”,1”-f]pyrimidin-3-ones, xanthoglows, pyrroloindolizinedione analogs, BODIPY analogs, and the phenolic and imidazolinone ring systems of Green Fluorescent Protein (GFP). This manuscript describes an inexpensive and operationally simple method of performing a Claisen-Schmidt condensation to generate a series of fluorescent pH dependent pyrazole/imidazole/isoindolone dipyrrinone analogs. While the methodol. illustrates the synthesis of dipyrrinone analogs, it can be translated to produce a wide range of conjugated bicyclic aromatic compounds The Claisen-Schmidt condensation reaction utilized in this method is limited in scope to nucleophiles and electrophiles that are enolizable under basic conditions (nucleophile component) and non-enolizable aldehydes (electrophile component). Addnl., both the nucleophilic and electrophilic reactants must contain functional groups that will not inadvertently react with hydroxide. Despite these limitations, this methodol. offers access to completely novel systems that can be employed as biol. or mol. probes.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Bhaskaran, Ayana team published research on Polymer in 2021 | 3034-50-2

Bhaskaran, Ayana;Aitken, Heather M.;Xiao, Zeyun;Blyth, Mitchell;Nothling, Mitchell D.;Kamdar, Shashank;O′Mara, Megan L.;Connal, Luke A. research published 《 Enzyme inspired polymer functionalized with an artificial catalytic triad》, the research content is summarized as follows. At the heart of an enzyme′s structure is the active catalytic site, which, together with the surrounding amino-acid residues, tunes the substrate properties in the electrostatic microenvironment. Taking inspiration from nature′s catalytic triad, consisting of a hydroxyl group of a serine residue, an imidazole group of a histidine residue, and a carboxyl group of an aspartic acid, a polymer scaffolded enzyme mimic is incorporated with artificial catalytic triad units. It is demonstrated that controlling the local environment of the artificial triad affects catalytic activity. Compared to a water soluble artificial catalytic triad, enhanced esterolytic activity of p-nitrophenyl benzoate was observed for the polymeric catalyst possibly due to the hydrophobic microenvironment formed by the tertiary structure of the polymer backbone. The different environments were supported by mol. dynamics simulations. It is further demonstrated that the cross-linked catalytic triad functional polystyrene could be used as a reusable solid support catalyst for esterolysis.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Abuskhuna, Suaad M. team published research on Asian Journal of Pharmaceutical Analysis and Medicinal Chemistry in 2020 | 3034-50-2

Abuskhuna, Suaad M.;Zeglam, Talal H.;Fhid, Omran N. R.;Jebril, Asma O. research published 《 Antibacterial activity of hydroxyimidazole derivatives》, the research content is summarized as follows. Different methods have been reported for the synthesis of 1-hydroxyimidazoles I (R = Me, Ph, 4-fluorophenyl; R¹ = pyridin-2-yl, 4-nitrophenyl, 2,4-dimethoxyphenyl, etc.) and a number of them reported to possess significant biol. activity, thus synthesis of some new derivatives I are introduced for better antibacterial activity.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem

Ako, Ayuk M. team published research on Inorganic Chemistry in 2020 | 3034-50-2

Ako, Ayuk M.;Kathalikkattil, Amal Cherian;Elliott, Rory;Soriano-Lopez, Joaquin;McKeogh, Ian M.;Zubair, Muhammad;Zhu, Nianyong;Garcia-Melchor, Max;Kruger, Paul E.;Schmitt, Wolfgang research published 《 Synthetic Approaches to Metallo-Supramolecular Co^II Polygons and Potential Use for H₂O Oxidation》, the research content is summarized as follows. Metal-directed self-assembly has been applied to prepare supramol. coordination polygons which adopt tetrahedral (1) or trigonal disklike topologies (2). In the solid state, 2 assembles into a stable halide-metal-organic material (Hal-MOM-2), which catalyzes H₂O oxidation under photo- and electrocatalytic conditions, operating with a maximum TON = 78 and TOF = 1.26 s^-1. DFT calculations attribute the activity to a Co^III-oxyl species. This study provides the first account of how Co^II imine based supramols. can be employed as H₂O oxidation catalysts.

Referemce:
Imidazole – Wikipedia,
Imidazole | C3H4N2 – PubChem