Affiliation:
1. Department of Biotechnology and Industrial Pharmacy, M.V. Lomonosov Institute of Fine Chemical Technologies, MIREA-Russian Technological University, 119571 Moscow, Russian Federation
Abstract
Currently, peptide nucleic acids (PNAs) play an important role as therapeutic
agents, molecular tools for diagnosis and detection of genetic diseases as well as in biosensor
probes. This research aims to optimize the synthesis of aeg- and γ-(S)-Me PNA
monomers based on L-Ala, intended for oligomerization according to the Boc protocol.
The monomers were obtained through the condensation of the corresponding pseudopeptides
with carboxymethyl purine nucleic bases. During the work, the optimization of benzyloxycarbonyl-
N6-adenine-9-yl-acetic acid and benzyloxycarbonyl-N2-guanine-9-ylacetic
acid was carried out. The synthesis of benzyloxycarbonyl-N6-adenine-9-yl-acetic
acid was conducted in three stages based on adenine with an overall yield of 22%. At the
same time, the conditions for effective recrystallization of the mixture after alkylation of
benzyloxycarbonyl-N6-adenine with ethyl bromoacetic acid ether have been developed to isolate the desired
N9-regioisomer. Also, the optimization of a known method for producing benzyloxycarbonyl-N2-guanine-9-ylacetic
acid from 2-amino-6-chloropurine was carried out. The total yield of the five-stage scheme was 55%.
Condensation of aeg- and γ-(S)-Me pseudopeptides with benzyloxycarbonyl-N6-adenine-9-yl-acetic acid and
benzyloxycarbonyl-N2-guanine-9-yl-acetic acid was performed by the standard carbodiimide method,
DCC/HOBt in DMF followed by the removal of C-terminal methyl protective group by alkaline hydrolysis.
The structure of the new compounds obtained was confirmed by spectral analysis methods. This work provides
simple and optimized methods for obtaining protected carboxymethyl purine bases and increasing the efficiency
of the synthesis and synthesized purine PNA monomers in an acceptable yield.
Publisher
Bentham Science Publishers Ltd.
Cited by
1 articles.
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