Research Article pubs.acs.org/journal/ascecg
Synthesis of Quinone Methide Substituted Neonicotinoid Derivatives via 1,6-Conjugate Addition of N‑Benzyl Nitro Ketene Aminals with para-Quinone Methides Accompanying Oxidation Bao-Qu Wang, Qin Luo, Qiang Xiao, Jun Lin,* and Sheng-Jiao Yan* Key Laboratory of Medicinal Chemistry for Natural Resource (Yunnan University), Ministry of Education, School of Chemical Science and Technology, Yunnan University, Kunming 650091, P. R. China S Supporting Information *
ABSTRACT: A concise and efficient route for the synthesis of quinone methide substituted neonicotinoid derivatives (4−5) via the one-pot Cs2CO3-catalyzed 1,6-conjugate addition of N-benzyl nitro ketene amines (2) or 1,1-enediamines (3) with paraquinone methides (1) in acetone and an oxidation reaction using atmospheric oxygen has been developed. This protocol represents a route to obtain a novel class of quinone methide substituted neonicotinoid derivatives in a concise, rapid, and practical manner. This reaction is particularly attractive because of the following features: low-cost and biocompatible solvent, mild temperature, atomic economy, high yields, and potential biological activity of the product. KEYWORDS: 1,6-Conjugate addition, Environmentally friendly, Oxidation, Neonicotinoids, para-Quinone methides
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methides (p-QMs) are important intermediates in the field of chemistry, medicine, and biological research.11,12 For example, ferrocenyl quinone methides A and B (Figure 1) possess remarkable intrinsic antiproliferative properties, which have key anticancer roles.13−15 According to the splicing principle of the drug’s molecular structure, we tried to combine the two active core structures pictured above in the hope of producing a new class of pharmaceutical molecules which may possess potential bioactivities. As part of our ongoing research effort, we tried to use N-benzyl nitro ketene aminals (NBNKAs, 2) and 1,1enediamines (EDAMs, 3) as synthons to accomplish this goal. NBNKAs belong to heterocyclic ketene aminals (HKAs)16−23 which are widely used to construct molecular diverse heterocyclic compounds24−32 such as spirooxindoles,33,34 quinolones, pyridines,35 pyrroles, and others. However, the structural features of p-QMs result from the assembly of carbonyl and olefin moieties, and they have been widely used in
INTRODUCTION All over the world, over 50% of major chemical production is related to the use of the oxidation reaction, including the oxidation of hydrocarbons and oxygenated chemicals. Among organic reactions, oxidation reactions are the most difficult to control, with accompanying byproducts, which lead to low yields with poor selectivity of desired products. At this time, inorganic oxygen donors, such as sodium hypochlorite, sodium hypobromite, nitric acid, potassium peroxymonosulfate, chromium trioxide, potassium permanganate, and potassium dichromate, etc., are still used to produce oxidation reactions. The use of inorganic electron donors as oxidants generates large amounts of salt as a waste product, which can cause environmental pollution and places a strain on waste resource management. Oxygen, however, is the most environmentally friendly industrial oxidant. The overall structure of neonicotinoid derivatives exhibits special molecular characteristics1 including an electron-withdrawing nitro, a flexible side chain, and guanidine/amidine groups. Neonicotinoid derivatives exhibit a potent insecticidal activity (Figure 1; 6-Cl-PMNI, IPPA08, and Palchongding)2−9 and have strong antimicrobial properties.10 para-Quinone © 2017 American Chemical Society
Received: June 30, 2017 Revised: August 1, 2017 Published: August 4, 2017 8382
DOI: 10.1021/acssuschemeng.7b02166 ACS Sustainable Chem. Eng. 2017, 5, 8382−8389
Research Article
ACS Sustainable Chemistry & Engineering
Figure 1. Biologically active neonicotinoids and para-quinone methide compounds.
Therefore, the discovery of a practical and efficient method for 1,6-conjugate addition and the oxidation reaction by atmospheric O2 in one step is still a highly desirable and yet formidable challenge (Figure 2). The oxidative ability of atmospheric oxygen is usually very poor and often requires a catalyst to increase its oxidative ability. As a result, applicable literature seldom mentions the utilization of oxygen without a catalyst. Herein, we describe 1,6conjugate addition and oxidation by using an oxygen oxidizer for the synthesis of quinone methide substituted neonicotinoid derivatives (also named para-quinone methide derivatives) (4) in a single-step reaction. To the best of our knowledge, the synthesis of these derivatives has not been reported using 1,6conjugate addition followed by the oxidation of para-quinone methide (1) and NBNKAs (2) or EDAMs (3).
a variety of addition reactions as universal Michael receptors, and are also chemically defined as neutral and zwitterionic resonance entities.36,37 These structural features also allow for natural product synthesis as well as for the production of bioactive molecules.38−41 There have been comprehensive reports produced about para-quinone methide reactions such as [3 + 2] addition,42−46 [4 + 2] cycloaddition,47 [1 + 4] addition,48 and others.49−52 Since Fan and Jørgensen reported on the 1,6-addition reaction of methylene quinone compounds,53−60 many catalytic systems such as transition-metal catalysts (Figure 2),61−67 BF3·Et2O (Figure 2),68,69 N-
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EXPERIMENTAL SECTION
General Methods. All compounds were fully characterized by spectroscopic data. The NMR spectra were recorded on a Bruker DRX500 and DRX600 device. Chemical shift (δ) values are expressed in ppm, J values are given in Hz, and deuterated DMSO-d6 and CDCl3 were used as the solvent. IR spectra were recorded on an FT-IR Thermo Nicolet Avatar 360 device using a KBr pellet. The reactions were monitored by thin layer chromatography (TLC) using silica gel GF254. The melting points were determined on an XT-4A melting point apparatus and are uncorrected. HRMS was performed on an Agilent LC/Msd TOF instrument. Materials used were purchased from Adamas-beta Corp., Ltd. All chemicals and solvents were used as received without further purification unless otherwise noted. Column chromatography was performed on silica gel (200−300 mesh). 4-Benzylidene-2,6-di-tertbutylcyclohexa-2,5-dienone 1 was prepared according to the literature,80,81 and NBNKAs 2 were also prepared in this way;82,83 EDAMs 3 were prepared according to the literature.84 General Procedure for the Synthesis of Compounds 4−5. A 25 mL sealed tube was charged with p-QMs 1 (1.1 mmol), acetone (15 mL), and NBNKAs 2 (1.0 mmol) or EDAMs 3 (1.0 mmol). A small amount of Cs2CO3 (10 mg) was then added to this mixture. The solution was stirred for 8 h at 70 °C. The mixture was cooled to room temperature and added to 40 mL of water, then neutralized with saturated NH4Cl solution to alkalinity, after which time it was extracted with an appropriate amount of ethyl acetate. Its organic phase was combined and dried over anhydrous Na2SO4 and then concentrated under reduced pressure and purified by fast column chromatography (petroleum ether/EtOAc = 1/1). This produced a yield of 4−5 of 70−92%.
Figure 2. Strategies for 1,6-conjugate addition and oxidation of pQMs.
heterocyclic carbene catalysts (Figure 2),70,71 K2CO3 (Figure 2),72,73 phosphoric acids (Figure 2),74,75 and other catalysts were reportedly used in the 1,6-addition reaction.76,77 Recently, the Li Xin group realized the organocatalyzed asymmetric 1,6conjugate addition of para-quinone methides with dicyanoolefins.78,79 To our knowledge, all of the above reactions produced the phenolic compounds via the 1,6-addition reactions of pQMs with different nucleophilic reagents. However, the method of p-QM derivative synthesis with a large conjugated ketene which is based on the 1,6-addition and the oxidation of p-QMs with nucleophilic reagents has not been realized. 8383
DOI: 10.1021/acssuschemeng.7b02166 ACS Sustainable Chem. Eng. 2017, 5, 8382−8389
Research Article
ACS Sustainable Chemistry & Engineering Table 1. Optimization of the Reaction Conditionsa
entry
solvent
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21
1,4-dioxane 1,4-dioxane 1,4-dioxane 1,4-dioxane 1,4-dioxane 1,4-dioxane 1,4-dioxane 1,4-dioxane THF CH2Cl2 EtOH toluene DMF DMSO ethyl acetate CH3CN CH3COCH3 CH3COCH3 CH3COCH3 CH3COCH3 CH3COCH3
catalyst
T (°C)
t (h)
yieldb (%)
Et3Nd K2CO3d NaHCO3d Cs2CO3d piperidined t-BuOKd Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3d Cs2CO3e
room temp reflux reflux reflux reflux reflux reflux reflux reflux reflux reflux reflux reflux reflux reflux reflux 70 °C 70 °C 70 °C 70 °C 70 °C
8 8 4 4 4 4 4 4 4 4 4 4 4 4 4 4 4 8 10 8 8
nrc nr nr nr nr 40 nr nr nr nr nr nr 20 30 40 75 80 90 90 92 90
a Reactions (entries 1−21) were carried out using 1c (1.1 mmol), 2c (1.0 mmol), and solvent (15 mL). bIsolated yield based on NBNKA 2c. cnr = not recorded. dCatalyst (0.05 mmol). eCatalyst (0.1 mmol).
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RESULTS AND DISCUSSION In this paper, we attempted to establish a one-pot protocol to synthesize a series of quinone methide substituted neonicotinoid derivatives. To obtain optimal reaction conditions for the synthesis of our target molecule, we chose the reaction of pQMs (1c) with NBNKAs (2c) as a model. First, the reaction of 1c with 2c was carried out with a different catalyst, consisting of Et3N, K2CO3, NaHCO3, Cs2CO3, piperidine, and t-BuOK at different temperatures (Table 1, entries 1−8). The results showed a product yield of 45% (Table 1, entry 6) with the Cs2CO3 catalyst for 4 h in 1,4-dioxane. Next, we investigated the effects of several solvents, including THF, CH2Cl2, EtOH, CH3COCH3, toluene, DMF, DMSO, ethyl acetate, and CH3CN at reflux temperatures (Table 1, entries 9−17). With most solvents, the target compound was not produced at all (Table 1, entries 9−12); however, with DMF and DMSO the products were obtained, but only at a low yield (Table 1, entries 13 and 14). However, when the solvents ethyl acetate, CH3CN, and CH3COCH3 were used, an excellent yield of the desired compound 4cc was obtained, with the solvent CH3COCH3 producing an optimal yield (Table 1, entries 15−17); additionally, with the reaction time extended to 8 h, the yield of a desirable product 4cc was improved to 92%. However, when the reaction time was increased to 10 h, the yield of a desirable product was not improved (Table 1, entries 18 and 19). On this basis, we further examined the effects of the
amount of catalyst upon percent yield. When we adjusted the amount of catalyst Cs2CO3 to 5% (0.05 mmol) of the amount of raw material 2c, the target compound 4cc was obtained at a 92% yield. The yield was 90% when the amount of Cs2CO3 was adjusted to 10% (0.1 mmol) of the amount of raw material 2c (Table 1, entries 20 versus 21). Thus, the use of catalyst at 5% by weight sufficiently produces high yield percentages. Preparation of 4cc required a mixture of 1c and 2c in acetone for about 20 min, along with the addition of Cs2CO3 at 70 °C. Under optimal conditions, we explored the scope and limitations of these addition reactions involving various p-QMs (1a−1e) with NBNKAs (2a−2h) or EDAMs (3a−3f) (Table 2, entries 1−41). The results showed that although the reaction proceeded within 8 h in all cases (Table 2, entries 1−30), the different substituent groups (R = F, Cl, H, Me, or MeO) at the C8 position of the p-QMs 1 usually had a slight influence on the yields. An electron-withdrawing group on p-QMs 1 (F or Cl) usually can obtain higher yields than an electron-donating group on p-QMs 1 (Me or MeO) (Table 2, entries 1−11 versus 20−30). In general, an electron-withdrawing group (F or Cl) on NBNKAs 2 had higher yields than an electron-donating group (Me or MeO) on NBNKAs 2 (Table 2, entries 1 versus 2, 7 versus 8−9, and 20 versus 21 and 22). For the acquisition of molecular diversity of the products, 1,1-enediamines (3), which have a different structure, were used as a substrate reacted with p-QMs 1 to synthesize the products 5 with good yields (78−88%). In cases where the 8384
DOI: 10.1021/acssuschemeng.7b02166 ACS Sustainable Chem. Eng. 2017, 5, 8382−8389
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ACS Sustainable Chemistry & Engineering Table 2. One-Pot Protocol for the Regioselective Synthesis of Compounds 4−5a
entry
1 (R)
2 (Ar) or 3 (R′)
4 or 5
yieldb (%)
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30 31 32 33 34 35 36 37 38 39 40 41
1a (F) 1a (F) 1a (F) 1a (F) 1a (F) 1b (Cl) 1b (Cl) 1b (Cl) 1b (Cl) 1b (Cl) 1b (Cl) 1c (H) 1c (H) 1c (H) 1c (H) 1c (H) 1c (H) 1c (H) 1c (H) 1d (Me) 1d (Me) 1d (Me) 1d (Me) 1e (MeO) 1e (MeO) 1e (MeO) 1e (MeO) 1e (MeO) 1e (MeO) 1e (MeO) 1b (Cl) 1b (Cl) 1b (Cl) 1b (Cl) 1c (H) 1c (H) 1c (H) 1c (H) 1c (H) 1d (Me) 1d (Me)
2b (4-FC6H4) 2d (4-CH3C6H4) 2e (4-CH3OC6H4) 2f (2,4-difluorophenyl) 2g (3,4-dichlorophenyl) 2a (3-FC6H5) 2b (4-FC6H4) 2d (4-CH3C6H4) 2e (4-CH3OC6H4) 2f (2,4-difluorophenyl) 2g (3,4-dichlorophenyl) 2a (3-FC6H5) 2b (4-FC6H4) 2c (C6H5) 2d (4-CH3C6H4) 2e (4-CH3OC6H4) 2f (2,4-difluorophenyl) 2h (3,5-difluorophenyl) 2g (3,4-dichlorophenyl) 2b (4-FC6H4) 2d (4-CH3C6H4) 2e (4-CH3OC6H4) 2g (3,4-dichlorophenyl) 2a (3-FC6H4) 2b (4-FC6H4) 2d (4-CH3C6H4) 2e (4-CH3OC6H4) 2f (2,4-difluorophenyl) 2h (3,5-difluorophenyl) 2g (3,4-dichlorophenyl) 3a (4-FC6H4CH2) 3b (4-ClC6H4CH2) 3c (C6H5CH2CH2) 3d (4-CH3OC6H4CH2CH2) 2e (4-FC6H4) 3a (4-FC6H4CH2) 3b (4-ClC6H4CH2) 3c (C6H5CH2CH2) 3d (4-CH3OC6H4CH2CH2) 3a (4-FC6H4CH2) 3f (4-CH3C6H4CH2)
4ab 4ad 4ae 4af 4ag 4ba 4bb 4bd 4be 4bf 4bg 4ca 4cb 4cc 4cd 4ce 4cf 4ch 4cg 4db 4dd 4de 4dg 4ea 4eb 4ed 4ee 4ef 4eh 4eg 5ba 5bb 5bc 5bd 5ce 5ca 5cb 5cc 5cd 5da 5df
90 80 91 85 85 80 89 75 80 88 80 80 85 92 85 80 90 89 85 75 70 71 75 80 85 87 86 80 82 90 80 83 79 84 86 81 83 78 88 82 85
a
All reactions were run under the following conditions: 1 (1.1 mmol) and 2 (1.0 mmol) were refluxed in the solvent acetone (15 mL) for 20 min, and then Cs2CO3 was added to reflux 8 h at 70 °C. bIsolated yield based on NBNKAs 2 or EDAMs 3.
unequivocally confirmed by X-ray diffraction analysis as shown in Figures 3 (CCDC1558265) and 4 (CCDC1565720). It should be pointed out that the target compound 4af is Econfiguration based on the intramolecular H-bond of 4af. Compound 4af only has one H proton (Figure 3). However, compound 5ce is Z-configuration due to the fact that there is one intramolecular H-bond between the nitro group and 4FC6H4NH of 5ce (Figure 4).
reaction proceeded for 8 h, there were no large discrepancies in product yields for the different substituent groups on 1,1enediamines (3) (Table 2, entries 31−41). The chemical structures of all target derivatives 4−5 were fully characterized by IR, 1H NMR, 13C NMR, and HRMS. For further verification of the structure of the targeted products, one of the representative compounds (4af and 5ce) was selected as a representative compound, whose presence was 8385
DOI: 10.1021/acssuschemeng.7b02166 ACS Sustainable Chem. Eng. 2017, 5, 8382−8389
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for 70 °C, promoted by Cs2CO3 only for 3 h, and then with the reaction mixture injected in the HPLC−HRMS system. The molecular ion peak appeared in high-resolution mass spectrometry [HRMS (TOF ES + ): m/z calcd for C33H40Cl2N3O4 [M + H]+, 612.2390; found, 612.2329] (see the Supporting Information, which contains the HRMS spectra of compound Int 2). However, the pure compound of Int 2 could not be isolated by silica gel column chromatography under a nitrogen atmosphere. Therefore, we speculated that Int 2 had been oxidized by oxygen when we concentrated the reaction mixture.
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CONCLUSIONS In summary, we looked at the use of the Cs2CO3 catalyst for the efficient synthesis of neonicotinoid quinone methide derivatives by a 1,6-coupling reaction along with the oxidation of para-quinone methides 1 with NBNKAs 2 or EDAMs 3 in acetone. Novel classes of neonicotinoid quinone methide derivatives produce adequate to excellent yields. The reaction itself may be performed easily under mild conditions with very good atomic economy and operational simplicity. Moreover, this series of neonicotinoid quinone methide derivatives may possess potential biological and pharmaceutical activities. Our further investigations will aim at assessing the in vitro biological activities of compounds 4−5.
Figure 3. X-ray crystal structures containing the intramolecular Hbonds of 4af; ellipsoids are drawn at the 30% probability level.
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Figure 4. X-ray crystal structures containing the intramolecular Hbonds of 5ce; ellipsoids are drawn at the 30% probability level.
ASSOCIATED CONTENT
S Supporting Information *
The Supporting Information is available free of charge on the ACS Publications website at DOI: 10.1021/acssuschemeng.7b02166. Spectroscopic and analytical data as well as the original copy of 1H and 13C NMR spectra of all new compounds (PDF) X-ray crystallographic data of compounds 4af (CCDC 1558265) and 5ce (CCDC 1565720) (CIF)
A proposed mechanism for the synthesis of the quinone methide substituted neonicotinoid derivatives 4 by the 1,6conjugate addition of p-QMs 1 with NBNKAs 2 and oxidation using oxygen is illustrated in Scheme 1. NBNKAs 2, with a strong electron-withdrawing nitro group at the α-position and two electron-donating diamino groups on the diaza-heterocycle of NBNKAs,85,86 might serve as the nucleophilic component and may also produce 1,6-conjugate addition to the olefin bond group of p-QMs 1 to form intermediate Int 1. The Int 1 was followed by imine-enamine tautomerization to produce Int 2. Finally, the oxidation of Int 2 by oxygen is used to form the target compound 4. To prove this mechanism, we tried to perform the reaction under a nitrogen atmosphere in acetone
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AUTHOR INFORMATION
Corresponding Authors
*E-mail:
[email protected].
Scheme 1. Mechanism Hypotheses for the Synthesis of Target Compounds 4
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DOI: 10.1021/acssuschemeng.7b02166 ACS Sustainable Chem. Eng. 2017, 5, 8382−8389
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[email protected]. Phone/Fax: +86 87165031633.
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ORCID
Jun Lin: 0000-0002-2087-6013 Sheng-Jiao Yan: 0000-0002-7430-4096 Notes
The authors declare no competing financial interest.
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ACKNOWLEDGMENTS This work was supported by the National Natural Science Foundation of China (21662042, 21362042, U1202221, and 21262042), the Program for Changjiang Scholars and Innovative Research Team in University (IRT17R94), the Natural Science Foundation of Yunnan Province (2017FA003), the Reserve Talent Foundation of Yunnan Province for Middleaged and Young Academic and Technical Leaders (2012HB001), Donglu Schloars of Yunnan University, Excellent Young Talents, Yunnan University, and High-Level Talents Introduction Plan of Yunnan Province.
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ACS Sustainable Chemistry & Engineering
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DOI: 10.1021/acssuschemeng.7b02166 ACS Sustainable Chem. Eng. 2017, 5, 8382−8389