SYNTHESIS OF THE FJORD-REGION CIS-AMINO AND TRANS-AMINO TRIOL DERIVATIVES OF THE CARCINOGENIC HYDROCARBON BENZO[G]CHRYSENE AND UTILIZATION FOR THE SYNTHESIS OF A DEOXYADENOSINE ADDUCT LINKED TO THE N6-AMINO GROUP
As. Kiselyov et al., SYNTHESIS OF THE FJORD-REGION CIS-AMINO AND TRANS-AMINO TRIOL DERIVATIVES OF THE CARCINOGENIC HYDROCARBON BENZO[G]CHRYSENE AND UTILIZATION FOR THE SYNTHESIS OF A DEOXYADENOSINE ADDUCT LINKED TO THE N6-AMINO GROUP, Journal of organic chemistry, 60(19), 1995, pp. 6129-6134
Efficient syntheses of the complete set of four diastereomeric fjord-r
egion amino triol derivatives of benzo[g]chrysene in which the amino g
roup in the 14-position and the adjacent 13-hydroxyl group are trans o
r cis to one another (trans- and cis-5 and 6) is described. This is th
e first description of the syntheses of the bay- or fjord-region cis-a
mino triol derivatives of any carcinogenic polycyclic aromatic hydroca
rbon(PAH). The amino triols are key synthetic precursors of PAH-oligon
ucleotide adducts in which the PAH moiety is covalently linked to the
exocyclic amino groups of deoxyadenosine or deoxyguanosine. Formation
of adducts of this type via reaction of a PAH diol epoxide metabolite
with DNA is believed to be a critical step in the mechanism of PAH car
cinogenesis. The synthetic amino triol isomers may be used to synthesi
ze PAH-oligonucleotides needed for site-directed mutagenesis studies t
o relate isomer structural differences to their effects on DNA replica
tion.