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The method of anti-micheal addition reaction of arurone skeleton compound as acceptor
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An addition reaction and compound technology, applied in the field of anti-Micheal addition reaction, to achieve the effects of wide substrate applicability, efficient and convenient reaction, and high atom economy
Active Publication Date: 2021-01-12
QINGDAO AGRI UNIV
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However, the α-functionalization of heterodienes via the Michael pathway remains a challenge
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Embodiment 1
[0041]
[0042] Orange ketone compound 1a (0.1mmol) was subjected to trans-Michael addition in solvent (1.0mL) under the action of catalyst (20mol%, 0.02mmol) to obtain addition product 2a, and the conditions such as its catalyst, solvent and temperature were as follows: Table 1 shows:
[0043] Table 1
[0044] serial number catalyst solvent temperature(°C) time (h) Yield(%) 1 Cu(OTf) 2
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Abstract
The invention provides a method for carrying out a trans-Micheal addition reaction by taking a compound with an aurone skeleton as a receptor, and belongs to the technical field of chemical synthesis.According to the method, a reaction can be carried out under the conditions that Sc(OTf) 3 is used as a catalyst, the temperature is 80 DEG C and dichloromethane is used as a solvent. According to the method provided by the invention, the alpha-functionalized trans-Michael addition product of oxadiene is obtained through a negative hydrogen migration / aromatization / dearomatization / cyclization reaction by taking a carbonyl group conjugated with an aurone skeleton compound and a double bond as a receptor for Michael addition under the catalysis of Lewis acid. The method is simple and practical to operate, efficient and convenient in reaction, wide in substrate applicability and extremely high in atom economy.
Description
technical field [0001] The invention belongs to the technical field of chemical synthesis, and in particular relates to a compound with an aurone skeleton as an acceptor for trans-Micheal addition reaction. Background technique [0002] The helical loop structure widely exists in biologically active natural products and drugs, and is usually an ideal structure for new drug development due to its inherent three-dimensionality and structural novelty. Among the various spirocyclic structures, the [6,5]-piperidine spirofuran structure shown in the following structure is a very important class, present in nicotinic acetylcholine receptor (nAChR) modulators, CCR1 antagonists, acetyl Coenzyme a carboxylase (ACC) inhibitors. Therefore, the synthesis of related spirocyclic backbones has attracted considerable interest in recent years. [0003] [0004] Orange ketone is a secondary metabolite in plants. It belongs to flavonoids and can be regarded as a substituted benzofuranone d...
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