318 N-Heterocycles
H 2 NNH 2 H 2 N NH 2NO 2NH 2NH 2
NO 2O 2 NH 2 NO 2 NO 2 N NO 2OO168N NNH 2 N N NH 2
173
(ANPy)
174
(ANPyO)175H 2 SO 4 , HNO 360–65 %AcOH,NH 2 OH.HCl,
KOH (aq)
39 %30 % H 2 O 2Figure 7.65The direct nitration of 2,6-diaminopyridine (168) with mixed acid yields 2,6-diamino-
3,5-dinitropyridine (ANPy) (173).^111 Oxidation of ANPy (173) with peroxyacetic acid yields
ANPyO (174) (calculated VOD∼7840 m/s,d= 1 .88 g/cm^3 ).^112 C-Amination of ANPyO
(174) with hydroxylamine hydrochloride in aqueous base yields the triamine (175), an impact
insensitive explosive of high thermal stability.^113
CKO 2 NO 2 NNNNO 2NO 2NO 2NO 2
O 2 N NO 2O 2 NO
177O
179N 3 NN 3H 3 PO 4176 NaN^3178H 2 SO 4 , NaNO 2CH 2 OHFigure 7.66The electron deficiency of the pyridine ring means that 2,4,6-trinitropyridine (178) has to
be synthesized by an indirect route. Acidification of the potassium salt of 2,2-dinitroethanol
(176) is reported to give 2,4,6-trinitropyridine-1-oxide (177), which on reaction with nitrous
acid is reduced to 2,4,6-trinitropyridine (178).^114 2,4,6-Trinitropyridine (178) is reported to
be formed directly in these reactions if the initial cyclization of (176) is performed in the
presence of dilute nitric acid^115 or 2,2-dinitroethanol^116 is used directly. TheN-oxide (177)
is susceptible to nucleophilic substitution at the 2- and 6-positions, treatment of (177) with
sodium azide yielding the energetic diazide (179).^114
7.7 6-Membered rings – 2N
Pyrazine and pyrimidine heterocycles, like pyridine, are electron deficient and need the pres-
ence of an activating/electron-releasing group to allow efficient electrophilic nitration to occur.
An example of this strategy is seen during the synthesis of 2,6-diamino-3,5-dinitropyrazine
(ANPz) (183) where one of the chloro groups of 2,6-dichloropyrazine (180) is substituted for a