Synthesis 2024; 56(02): 329-345
DOI: 10.1055/s-0042-1751521
paper

Synthesis of New Structural Analogues of Natural Integrastatins with a Basic Epoxybenzo[7,8]oxocine Skeleton: Combined Experimental and Computational Study

Alena L. Stalinskaya
a   Institute of Chemistry, Tyumen State University, 15a Perekopskaya St., Tyumen 625003, Russian Federation
,
Semyon Y. Chikunov
a   Institute of Chemistry, Tyumen State University, 15a Perekopskaya St., Tyumen 625003, Russian Federation
,
Irina A. Pustolaikina
b   Karagandy University of the Name of Academician E. A. Buketov, Karaganda, 100024 Kazakhstan, Kazakhstan
,
Yuri V. Gatilov
с   N. N. Vorozhtsov Novosibirsk Institute of Organic Chemistry, Siberian Branch of the Russian Academy of Science, 9 Akademika Lavrientieva Ave., Novosibirsk 630090, Russian Federation
,
a   Institute of Chemistry, Tyumen State University, 15a Perekopskaya St., Tyumen 625003, Russian Federation
› Author Affiliations
The study was supported by a grant from the Russian Science Foundation (No. 22-23-01015, https://rscf.ru/project/22-23-01015/).


Abstract

In this work, the cyclization reactivity of various 3-acetyl-2-methylpyridines (including 3-acetyl-2-methylquinoline) containing both electron donor and acceptor substituents with salicylaldehyde into epoxybenzooxocino[4,3-b]pyridine derivatives was studied. The reactions were carried out in mild (under room temperature or reflux in 2-propanol) and harsh (in a sealed glass ampoule) conditions. It was shown that 3-acetyl-2-methylpyridines with an aryl substituent in the 4-position do not react with salicylaldehyde either under normal convection heating conditions or under more severe conditions. This effect was explained by the steric hindrance of the substituents using quantum chemical calculations. It was found that electron donor substituents in 3-acetyl-2-methylpyridines significantly facilitate cyclization in epoxybenzooxocino[4,3-b]pyridines. The presence of electron acceptor substituents (NO2 group for example) in the 5-position of pyridine prevents cyclization under normal conditions, but gives a rather high conversion to oxocinopyridines under more specific conditions. This effect is quantum-chemically explained by the decrease in the basicity of pyridine. Pyridines with two pairs of methyl groups in ortho-positions to the acetyl group are capable to form mixtures of regioisomeric epoxybenzooxocinopyridines. Further, epoxybenzooxocinopyridines with methyl and acetyl groups can form a mixture of diastereomeric bisoxocins under more specific conditions. All 17 initial pyridines were studied quantum-chemically in order to understand what features of their structure and properties affect the success of the cyclization reaction and the yield of the target product. The pyridine molecules were calculated by the DFT RB3LYP/6-311++G(d,p) method taking into account the alcohol solvent within the CPCM model using Gaussian-2016 program. It was shown that the absence of steric hindrances in the form of bulky substituents in 4-position of pyridines is the main factor affecting the success of the cyclization reaction. Also, the yield of the target product is affected by the CH-acidity of the methyl group in 2-position, which, in turn, is affected by electron-donating and electron-withdrawing substituents in the 5- and 6-positions.

Supporting Information



Publication History

Received: 20 September 2023

Accepted after revision: 19 October 2023

Article published online:
21 November 2023

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