Novel analogues of spermine and spermidine with terminal H2N-CH2-group
substituted by H2N-O-group, were prepared starting the synthesis from
EtO(Me)C=NOH and subsequent extension of a polyamine backbone. To pre
pare their earlier unknown tritium labelled analoques, -ethoxyethylide
ne)amino]oxy]-poly-(iminomethylene) nitriles were reduced to amines by
NaBT2/CoCl2 complex, which did not effect the N-O or C=N bonds of eth
oxyethylidene group, whereas aminooxy group deprotection was performed
at the final step of synthesis by mild acidic hydrolysis. Novel monoa
cetylated (AcHN- or AcNHO-) analogues of spermidine were also synthesi
sed. Copyright (C) 1996 Elsevier Science Ltd