Novel nitrated derivatives of 5,8-diazabenzo[c]phenanthrene and 9,14-diazadibenz[a,e]acephenanthrylene: new classes of potent mutagenic compounds

doi:10.1093/mutage/14.6.587

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Mutagenesis, Vol. 14, No. 6, 587-594, November 1999
© 1999 UK Environmental Mutagen Society/Oxford University Press

Novel nitrated derivatives of 5,8-diazabenzo[c]phenanthrene and 9,14-diazadibenz[a,e]acephenanthrylene: new classes of potent mutagenic compounds

Mathew Upton¹ and Christopher Upton²

Department of Pharmacy and Pharmacology, University of Bath, Claverton Down, Bath BA2 7AY, UK and ¹ Department of Microbiology, University of Otago, Dunedin, New Zealand

We report the synthesis of 4-nitro-5,8-diazabenzo[c]phenanthrene(4-NDBP) and 11-nitro-9,14-diazadibenz[a,e]acephenanthrylene(11-NDDA) and the remarkable mutagenic activity of the latter.These two compounds and their non-nitrated parents, 5,8-diazabenzo[c]phenanthrene(DBP) and 9,14-diazadibenz[a,e]acephenanthrylene (DDA), werescreened in Ames plate incorporation assays against Escherichiacoli WP2uvrA and Salmonella typhimurium TA98 both in the presenceand absence of S9 liver fraction from Aroclor 1254-induced rats.None of the four compounds were cytotoxic up to the limits oftheir solubility and none showed mutagenic activity in E.coliWP2uvrA, which suggested that any such activity they may havehad was not mediated via a base substitution mechanism. DBPand DDA also displayed a lack of activity in TA98 up to theirprecipitating doses (560 and 33.5 µg/plate, respectively).The two nitrated compounds, however, were genotoxic. 4-NDBPwas active at a dose of 500 ng/plate, in the absence of S9,producing 80.0 ± 28.0 prototrophic organisms (equivalentto 44 revertants/nmol) and at 0.5 ng/plate, in the presenceof S9, giving 147 ± 6.6 revertants (equivalent to 81000/nmol) and allowed the description of this tetracycle asa potent mutagen. Much more striking was the activity of 11-NDDA:in the absence of S9 a dose of 8.0 ng produced 2000 revertants/nmoland, remarkably, in the presence of S9 80 pg produced the equivalentof 643 000 revertants/nmol. This makes the hexacyclic 11-NDDAthe most potent mutagen to date, in the Ames procedures describedhere.

² To whom correspondence should be addressed. Tel: + 44 01225826826; Fax: +44 01225 826114; Email: c.upton{at}bath.ac.uk

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