67-51-6Relevant articles and documents
Tris(3,5-dimethylpyrazole)copper(II) nitrate: As an oxidation catalyst
Sharma, Sagar,Barooah, Nilotpal,Baruah, Jubaraj B.
, p. 171 - 176 (2005)
Tris(3,5-dimethylpyrazole)copper(II) nitrate (A) is a catalyst for mild oxidation of various organic substrates. It acts as catalyst for conversion of benzylamine to benzaldehyde in the presence of hydrogen peroxide. Various benzylic alcohols are converted to corresponding aldehydes and acids by the catalytic amount of the complex (A) with hydrogen peroxide at room temperature. The complex also catalyses dimerisation of 2,6-dimethylphenol and thiophenol. The thermal decomposition of tris(3,5-dimethylpyrazole)copper(II) nitrate at 500°C gives CuO having the monoclinic crystal system. The cyclic voltammogram of the complex tris-(3,5-dimethylpyrazole)copper(II) nitrate shows a quasi-reversible redox cycle at -101 mV (E1/2) versus the Ag/AgCl electrode (+ve scan; scan speed 100 mV/s). The ΔE between anodic and cathodic peaks is 110 mV (ipa/ipc = 1.2).
Pyrazolylamidino ligands from coupling of acetonitrile and pyrazoles: A systematic study
Gmez-Iglesias, Patricia,Arroyo, Marta,Bajo, Sonia,Strohmann, Carsten,Miguel, Daniel,Villafae, Fernando
, p. 12437 - 12448 (2014)
Mixed pyrazole-acetonitrile complexes, both neutral fac-[ReBr(CO)3(NCMe)(pzH)] (pzH = pzH, pyrazole; dmpzH, 3,5-dimethylpyrazole; or indzH, indazole) and cationic fac-[Re(CO)3(NCMe)(pzH)2]A (A = BF4, ClO4, or OTf), are described. Their role as the only starting products to obtain final pyrazolylamidino complexes fac-[ReBr(CO)3(NH=C(Me)pz-κ2N,N)] and fac-[Re(CO)3(pzH)(NH=C(Me)pz-κ2N,N)]A, respectively, is examined. Other products involved in the processes, such as fac-[ReBr(CO)3(pzH)2], fac-[Re(CO)3(NCMe)(NH=C(Me)pz-κ2N,N)]A, and fac-[Re(CO)3(pzH)2(OTf)] are also described. Warming CD3CN solutions of fac-[Re(CO)3(NCMe)(pzH)2]A at 40 °C gives cleanly the pyrazolylamidino complexes [Re(CO)3(pzH)(NH=C(Me)pz-κ2N,N)]A as the only products, pointing to an intramolecular process. This is confirmed by carrying out reactions in the presence of one equivalent of a pyrazole different from that coordinated, which affords complexes where the pyrazolylamidino ligand contains only the pyrazole previously coordinated. When the reactions lead to an equilibrium mixture of the final and starting products, the reverse reaction gives the same equilibrium mixture, which indicates that the coupling reaction of pyrazoles and nitriles to obtain pyrazolylamidino ligands is a reversible intramolecular process. A systematic study of the possible factors which may affect the reaction gives the following results: (a) the yields of the direct reactions are higher for lower temperatures; (b) the tendency of the pyrazoles to give pyrazolylamidino complexes follows the sequence indzH > pzH > dmpzH; and (c) the reaction rates do not depend on the nature of the anion even when a large excess is added. The presence of a small amount of aqueous solution of NaOH catalyzes the reaction. Thus, addition of 0.5-1% of NaOH (aq) to solutions of fac-[ReBr(CO)3(NCMe)(pzH)] (in CD3CN) or fac-[Re(CO)3(NCMe)(pzH)2]A (in CD3CN, CD3NO2 or (CD3)2CO) allowed the syntheses of the corresponding pyrazolylamidino complexes [ReBr(CO)3(NH=C(Me)pz-κ2N,N)] or [Re(CO)3(pzH)(NH=C(Me)pz-κ2N,N)]A with better yields, more rapidly, and in milder conditions.
Pd-Catalyzed Asymmetric Dearomatization of Indoles via Decarbonylative Heck-Type Reaction of Thioesters
Han, Ming-Liang,Huang, Wei,Liu, Yu-Wen,Liu, Min,Xu, Hui,Xiong, Hai,Dai, Hui-Xiong
, p. 172 - 177 (2021)
We report herein a palladium-catalyzed ligand-promoted asymmetric dearomatization of indoles via the decarbonylation of thioesters and the subsequent reductive Heck reaction. This protocol provides a facile and efficient way to construct an aza-quaternary stereocenter at the C2 position of indolines. A variety of functional groups and substitutions could be well tolerated, affording the substituted indolines with high enantioselectivities.
Synthesis and Cyclizations of N-(Thieno[2,3-b]pyridin-3-yl)cyanoacetamides
Chigorina,Bespalov,Dotsenko
, p. 2018 - 2026 (2019)
3-Aminothieno[2,3-b]pyridine-2-carboxylic acid esters readily reacted with 3,5-dimethyl-1-(cyanoacetyl)-1H-pyrazole to give previously unknown N-(thieno[2,3-b]pyridin-3-yl)cyanoacetamides. Reactions of the latter with 2-(arylmethylidene)malononitriles were nonselective, and mixtures of different heterocyclization products were generally formed. The cyclization of ethyl 4,6-dimethyl-3-[(cyanoacetyl)amino]thieno[2,3-b]-pyridine-2-carboxylate afforded 2,4-dihydroxy-7,9-dimethylthieno[2,3-b : 4,5-b′]dipyridine-3-carbonitrile whose tautomeric equilibrium was studied by DFT quantum chemical calculations. In silico analysis of biological activity of the synthesized compounds was performed.
Predicting the catalytic activity of azolium-based halogen bond donors: an experimentally-verified theoretical study
Bolotin, Dmitrii S.,Il'in, Mikhail V.,Novikov, Alexander S.,Suslonov, Vitalii V.,Sysoeva, Alexandra A.
, p. 7611 - 7620 (2021/09/22)
This report demonstrates the successful application of electrostatic surface potential distribution analysis for evaluating the relative catalytic activity of a series of azolium-based halogen bond donors. A strong correlation (R2> 0.97) was observed between the positive electrostatic potential of the σ-hole on the halogen atom and the Gibbs free energy of activation of the model reactions (i.e., halogen abstraction and carbonyl activation). The predictive ability of the applied approach was confirmed experimentally. It was also determined that the catalytic activity of azolium-based halogen bond donors was generally governed by the structure of the azolium cycle, whereas the substituents on the heterocycle had a limited impact on the activity. Ultimately, this study highlighted four of the most promising azolium halogen bond donors, which are expected to exhibit high catalytic activity.
Preparation method of dinotefuran
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Paragraph 0013; 0054-0062; 0069-0074, (2021/08/07)
The invention provides a preparation method of dinotefuran, and belongs to the field of organic synthesis. The invention provides a preparation method of dinotefuran, which is characterized by comprising the following steps: step 1, adding a compound I, a compound II and a solvent into a reaction container, heating to 50 DEG C which is the reflux temperature of the solvent, reacting for 1-24 hours, then adding tetrahydrofuran-3-methylamine, and continuously reacting for 1-24 hours to obtain a reaction solution; and 2, cooling the reaction solution to 0-20 DEG C, standing, filtering, separating the solid and filtrate, and purifying the solid to obtain dinotefuran, wherein the structural formula of the compound I is shown in the specification, the structural formula of the compound II is shown in the specification, and R1 and R2 are independently selected from any one of H, C1-C5 alkyl and C1-C5 alkyl substituted by at least one halogen atom. According to the invention, a brand new dinotefuran synthesis route is developed, the synthesis route is greatly shortened, and the production efficiency is improved.
Pyrazole-Mediated C-H Functionalization of Arene and Heteroarenes for Aryl-(Hetero)aryl Cross-Coupling Reactions
Kundu, Abhishek,Dey, Dhananjay,Pal, Subhankar,Adhikari, Debashis
, p. 15665 - 15673 (2021/11/16)
Herein we introduce a transition-metal-free protocol that involves a commercially available, inexpensive pyrazole molecule to conduct C-C cross-coupling reactions at room temperature via a radical pathway. Using this method, an aryldiazonium salt has been coupled to a wide range of arenes and heteroarenes including benzene, mesitylene, thiophene, furan, benzoxazole to result the corresponding biaryl products. The full reaction mechanism is elucidated along with the crystallographic probation of an active initiator species. A potassium-stabilized deprotonated pyrazole steers single-electron transfer to the substrate and behaves as an initiator for the reaction.