Organizing co mmittee
SYNTHESIS OF 2-FLUOROCORDYCEPINE
Yüklə 5,12 Mb. Pdf görüntüsü
|
|
SYNTHESIS OF 2-FLUOROCORDYCEPINE
Alexandra O. Arnautova, Alexey L. Kayushin, Konstantin V. Antonov, Irina D. Konstantinova Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, Miklukho-Maklaya 16/10, 117997 GSP-7, Moscow B-437, Russia 2-Fluorocordycepine (2-fluoro-3’-deoxyadenosine) is a potential effective antitumor and antiviral drug. We obtained 2-fluorocordycepin (2-F-Cord) ( 2 ) in two ways: by chemical synthesis and by enzymatic way using two different sources of 3-deoxyribose. Method 1. The chemical synthesis was performed in 3 stages. In the first step, the initial 2-fluoroadenosine (2-F-Ado) ( 1 ) was treated with α-acetoxyisobutyryl bromide to form two protected bromine derivatives. Resulting mixture was dehalogenated using H 2 /Pd, resulting in a mixture of protected 3'-deoxynucleosides. The protection groups were removed with aqueous methanol ammonia solution to form desired compound 2 and 2-aminocordycepine 3 in ratio 85:15 respectively. 2-F-Cord was isolated by reversed-phase chromatography with 28% yield. Method 2a. The enzymatic synthesis was performed using 3'-deoxyinosine ( 4 ) and nucleoside 1 in presence of recombinant E. coli purine nucleoside phosphorylase (PNP). Conditions: ratio of substrates ( 4 ):( 1 ) - 1.5:1.0, 2 mM potassium-phosphate buffer (pH 7.0), PNP - 2100 units, 50 ⁰С, the reaction time - 16 days. 2-F-Cord was isolated with 60% yield. Method 2b. Lithium salt of 3-deoxyribose phosphate ( 5 ) and compound 1 were used in the transglycosylation reaction as substrates. Conditions: ratio of substrates ( Yüklə 5,12 Mb. Dostları ilə paylaş:
|