Mannich reaction in the synthesis of N,S-containing heterocycles. 15. Multicomponent cascade synthesis of 3,4,6a,7,8,9,10,10a-octahydro-2H,6H- pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thia(selena)-diazine derivatives

Article abstract of DOI:10.1007/s10593-013-1173-9

The reaction of (2E,4E)-2-cyano-5-phenylpenta-2,4-dienethio(seleno)amides with formaldehyde and primary aromatic amines gives 3,8,10-trisubstituted 6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-py-rimido[4',5':4,5]pyrido[2,1-b] [1,3,5]thia(selena)diazine-11-carbonitriles. The latter were also obtained by a multicomponent condensation of cinnamaldehyde, cyanothioacetamide, formaldehyde, and anilines in the presence of catalytic amounts of base. The structure of the 3,8,10-tri(4-methylphenyl)-6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H- pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thiadiazine-11-carbonitrile was studied by X-ray structural analysis.

Full text of DOI:10.1007/s10593-013-1173-9

Chemistry of Heterocyclic Compounds, Vol. 48, No. 10, January, 2013 (Russian Original Vol. 48, No. 10, October, 2012)
MANNICH REACTION IN THE SYNTHESIS OF
N,S-CONTAINING HETEROCYCLES. 15*. MULTICOMPONENT
CASCADE SYNTHESIS OF 3,4,6a,7,8,9,10,10a-OCTAHYDRO-
2H,6H-PYRIMIDO[4',5':4,5]PYRIDO[2,1-b][1,3,5]THIA(SELENA)-
DIAZINE DERIVATIVES
K. A. Frolov¹, V. V. Dotsenko¹**, and S. G. Krivokolysko¹
The reaction of (2E,4E)-2-cyano-5-phenylpenta-2,4-dienethio(seleno)amides with formaldehyde and
primary aromatic amines gives 3,8,10-trisubstituted 6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-py-
rimido[4',5':4,5]pyrido[2,1-b][1,3,5]thia(selena)diazine-11-carbonitriles. The latter were also obtained
by a multicomponent condensation of cinnamaldehyde, cyanothioacetamide, formaldehyde, and anilines
in the presence of catalytic amounts of base. The structure of the 3,8,10-tri(4-methylphenyl)-6-phenyl-
3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thiadiazine-11-
carbonitrile was studied by X-ray structural analysis.
Keywords: pyrimido[4',5',:4.5]pyrido[2,1-b][1,3,5]thia(selena)diazines, cyanoselenoacetamide, cyanothio-
acetamide, aminomethylation, multicomponent condensation, Mannich reaction, X-ray structural analysis.
It has previously been shown that treatment of 3-aryl-2-cyanoprop-2-enethio(seleno)amides 1 with
primary amines and HCHO [2-4], and also in the course of recyclization of 4H-thio(seleno)pyrans 2 under
Mannich reaction conditions [4, 5], during the aminomethylation of tetrahydropyridine-2-thiolates 3 [6], and as
a result of a multicomponent condensation of aldehydes, cyanothio(seleno)acetamides 4a,b, primary amines and
HCHO [4, 5, 7] the same products are formed, viz. the 3,4,7,8-tetrahydro-2H,6H-pyrimido[4,3-b]-
[1,3,5]thia(selena)diazine-9-carbonitriles 5.
The nitriles 5 are of both applied and theoretical interest in view of the broad spectrum of practically important
properties of 1,3,5-thiadiazine derivatives [8-10] on the one hand, and the poorly studied reactivity and methods of
preparation of compounds with a 1,3,5-thiadiazine (and especially a 1,3,5-selenadiazine) fragment [4] on the other.
In continuation of our work in this field, we have studied the reaction of the unsaturated thio(seleno)-
amides 1, viz. the (2E,4E)-2-cyano-5-phenylpenta-2,4-dienethio(seleno)amides 6a,b with formaldehyde and
primary aromatic amines. The cinnamamides 6a,b are readily formed by the Michael reaction of
_______
* For Communication 14, see [1].
**To whom correspondence should be addressed, e-mail: victor_dotsenko@bigmir.net.
¹"ChemEx" Laboratory, Vladimir Dal' East Ukrainian National University, 20-A/7 Molodyozhnyi Kv., Lugansk
91034, Ukraine
________________________________________________________________________________________
Translated from Khimiya Geterotsiklicheskikh Soedinenii, No. 10, pp. 1668-1674, October, 2012.
Original article submitted April 11, 2012.
0009-3122/13/4810-1555©2013 Springer Science+Business Media New York
1555

Ar
CN
HCHO
RNH₂
HCHO
RNH₂
NC
CN
Ar
NH₂
R
R
Ar
X
N
N
N
X
H₂N
X
2
NH₂
1
CN
O
Ar
X
CN
HCHO
RNH₂
ArCHO
RNH₂
CN
S
R
EtOH, B
NH₂
+
4a,b
5
(X = S)
HO
HCHO
N
R
H
NMMH⁺
3
X = S, Se; NMMH⁺ = N-methylmorpholinium; B = Et₃N or N-methylmorpholine
cinnamaldehyde and cyanothio(seleno)acetamides 4a,b. It was found that the cinnamamides 6a,b undergo the
Mannich reaction with an excess of formalin and ArNH₂. Surprisingly, 3,4,6a,7,8,9,10,10a-octahydro-2H,6H-
pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thia(selena)diazine derivatives 8a-c were obtained as the condensation
products of cinnamamides 6a,b, primary aromatic amines, and HCHO in the ratio of 1:3:4 instead of the
expected pyrimido[4,3-b][1,3,5]thia(selena)diazines 7 (method A). Compounds 8a,b,d were also synthesized in
comparable yields by the alternative method B through condensation of cyanothioacetamide 4a with
cinnamaldehyde in the presence of catalytic amounts of Et₃N followed by boiling with an excess of HCHO and
3.1 equivalents of aniline. It was found that the multicomponent route B generally leads to the formation of less
pure products. Several limitations determined by the structure of the amine component were also revealed.
Hence we were unable to obtain the corresponding compound 8 in the case of N-acetyl-para-phenylenediamine
and 4-aminobenzenesulfamide. In this case a tar was obtained, containing a large fraction of unidentified
impurities according to HPLC-MS data.
CHO
Ar
Ar
+
4a,b
N
N
N
EtOH, B
Ph
Ph
Ph
Ar
X
CN
CN
CN
7
Method A
ArNH₂
HCHO
EtOH
NH₂
Ar
¹⁰ N
1
X
6a,b
11
X
2
9
12–28%
⁸ N
N³
N
7
6
6a
CHO
Ar
ArNH₂
4
Method B
EtOH, Et₃N
7–23%
Ph
8a–c
8a,b,d
+
4a
Ph
HCHO
4, 6 a X = S, b X = Se; 8 a X = S, Ar = 4-MeC₆H₄; b X = S, Ar = Ph; c X = Se, Ar = 4-MeC₆H₄;
d X = S, Ar = 4-МеOC₆H₄; В = Et₃N or N-methylmorpholine
Clearly a key part of the synthesis of compounds 8 is the formation of the N(5)–C(6) bond, which is a
variation of an intramolecular aza-Michael reaction. Similar 6-endo-trig processes leading to formation of
pyridine derivatives are known [11-14], but previously unreported for cinnamothio(seleno)amides. Clarification
of mechanistic details and optimization of the cascade process conditions will be the subject of further
investigation.
1556

NHAr
X
H₂N
NC
NHAr
HN
NC
X
CN
CN
ArNH₂
HCHO
ArNH₂
HCHO
Ph
N
X
Ph HN
X
NHAr
NHAr
Ph
6a,b
Ph
Ar
Ar
Ar
N
Ar
N
CN
N
NHAr
N
X
CN
ArNH₂
HCHO
CN
HCHO
N
N
N
Ar
Ar
Ph
N
X
Ph
N
XH
NHAr
Ph
8a–d
NHAr
Compounds 8a-d are colorless or variously yellow tinged crystals, insoluble in hot EtOH but soluble in
acetone, DMSO and hot DMF. Stretching vibration absorptions corresponding to free N–H groups are absent in
the IR spectra of compounds 8a-d, but they show the presence of strong bands at 2174-2176 cm^-1 (a conjugated
1
C≡N group). The H NMR spectra of compounds 8a-d show signals for the protons of one phenyl group and
three aryl substituents from the ArNH₂ as well as a complex set of signals for the 11 protons of the tricyclic
ring.
Fig. 1. Molecular structure of compound 8a from X-ray analytical data.
The decisive answer to the question of the structure of compounds 8a-d came from an X-ray structural
investigation (Fig. 1) of the 3,8,10-tri(4-methylphenyl)-6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido-
[4',5':4,5]pyrido[2,1-b][1,3,5]thiadiazine-11-carbonitrile 8a. The tetrahydropyridine ring occurs in a "sofa"
conformation with the atom C(6) deviating by 0.70 Å from the plane of the remaining atoms. The conformation
of the 1,3,5-thiadiazine ring can be regarded as an asymmetric "half chair" and is characterized by a deviation of
N(1) and C(2) atoms from the plane of the remaining ring atoms by 0.55 and -0.23 Å, respectively. The
perhydropyrimidine ring has a "chair" conformation with absolute values of the endocyclic dihedral angles in
1557

the range of 51.75(17)-59.66(17)º and with a cis type fusion to the tetrahydropyridine ring (dihedral angle H(5)–
C(5)–C(6)–H(6) 52º). The nitrogen atoms N(1), N(3), and N(4) have a pyramidal configuration, the sums of the
valence angles centered on these atoms being 344.5(4), 335.5(4), and 345.6(4)º, respectively. The orientation of
the tolyl substituents relative to the idealized positions for the lone electron pairs (Lp) of these nitrogen atoms
points to the presence of -conjugation between them (torsion angles Lp(N1)–N(1)–C(10)–C(15) 76º, LpN(3)–
N(3)–C(24)–C(25) 54º, and LpN(4)–N(4)–C(31)–C(36) 52º).
It should be noted that, in spite of several differences in the degree of the pyramidal nature of the N(1),
N(3), and N(4) nitrogen atoms and the angles between the aromatic -system of the substituent and the lone
electron pairs of the nitrogen atoms, the lengths of the N(sp³)–C(Ar) bonds are virtually the same (N(1)–C(10)
1.431(2), N(3)–C(24) 1.434(2), and N(4)–C(31) 1.428(2) Å). Steric hindrance arises because of this type of
orientation of the benzene rings, and this is reflected in the appearance of shortened intramolecular contacts
between the hydrogen atoms at the ortho position of the aromatic ring as well as and the methylene groups
neighboring the nitrogen atom (H(11)···H(1a) 2.07 Å, H(15)···H(2b) 2.01 Å, H(29)···H(8a) 2.28 Å,
H(29)···H(8b) 2.29 Å, H(25)···H(9b) 2.25 Å, H(32)···H(9b) 2.27 Å, and H(36)···H(5) 2.25 Å, while the sum of
the van der Waals radii is 2.32 Å [15]). The N(3) tolyl group has an equatorial conformation, but the
substituents at atoms N(1), N(4), and C(7) are axial (dihedral angles C(24)–N(3)–C(9)–N(4) 172.15(13)º,
C(10)–N(1)–C(1)–S(1) 76.00(18)º, C(31)–N(4)–C(5)–C(6) 87.24(16)º, and C(2)–N(2)–C(7)–C(18) 77.34(18)º).
In summary, the reactions of (2E,4E)-2-cyano-5-phenylpenta-2,4-dienethio(seleno)amides with HCHO
and primary aromatic amines give derivatives of the novel heterocyclic system – pyrimido[4',5':4,5]pyrido[2,1-b]-
[1,3,5]thia(selena)diazine-11-carbonitrile. These same products are formed in the course of a cascade
cyclocondensation of cyanothio(seleno)acetamide, cinnamaldehyde, primary amines, and HCHO. The structure
of the compounds obtained was confirmed by the results of X-ray structural investigation of 3,8,10-tri-
(4-methylphenyl)-6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thiadi-
azine-11-carbonitrile.
EXPERIMENTAL
1
IR spectra were recorded on an IKS-29 spectrophotometer in nujol mulls. The H NMR spectra were
recorded on a Varian Unity Plus instrument (400 MHz, compounds 6b, 8c,d) or on a Bruker DRX-500
instrument (500 MHz, compounds 8a,b) using DMSO-d₆ with TMS as internal standard. Elemental analysis was
carried out on a Carlo-Erba 1106 Elemental Analyzer with a measurement accuracy of ±0.25%. Melting points
were determined on a Koffler hot stage apparatus and are not corrected. HPLC-MS analysis of compound 8d
was carried out on a Shimadzu LC-10AD liquid chromatograph using Shimadzu SP D-10A UV-Vis (254 nm)
and Sedex 75 ELSD detectors together with a PE SCIEX API 150EX mass spectrometer. Monitoring of the
purity of the compounds prepared was carried out by TLC on Silufol UV-254 plates with acetone–hexane (1:1)
as eluent and visualized with iodine vapor and UV detection. The starting cyanothioacetamide (4a) [16] and
cyanoselenoacetamide (4b) [17] were prepared by known methods.
(2E,4E)-2-Cyano-5-phenylpenta-2,4-dienethioamide (6a) was prepared by modification of method
[18] without heating the reaction mixture. Brick-red, finely crystalline powder; mp 153-155ºC (mp 149ºC
(EtOH) [18], 158-160ºC (C₆H₆) [19]). The spectroscopic parameters agreed with those given in the literature
[18].
(2E,4E)-2-Cyano-5-phenylpenta-2,4-dieneselenoamide (6b). Cinnamaldehyde (0.86 ml, 6.84 mmol)
and N-methylmorpholine (1 drop) were added to a suspension of the cyanoselenoacetamide (4b) (1.0 g,
6.8 mmol) in EtOH (4 ml). The mixture was stirred and slowly heated to about 50ºC under an argon stream until
dissolution of the selenoamide 4b. After about 5 min crystallization started. The mixture was stirred for 3 h at
20ºC under an argon stream, filtered, and washed with EtOH and ether. Yield 1.37 g (77%). Bordeaux colored
powder; mp 123-125ºC (EtOH). The product was used in further reactions without additional purification. IR
1558

1
3
spectrum, , cm^-1: 3330 (NH₂), 2224 (C≡N). H NMR spectrum, , ppm (J, Hz): 7.13 (1Н, dd, J = 11.3,
³J = 11.5, 4-CН); 7.46-7.60 (4Н, m, 3-CH, H Ph); 7.71-7.73 (2H, m, H Ph); 8.01 (1H, d, ³J = 11.3, 5-CH); 10.13
(1Н, br. s) and 10.85 (1Н, br. s, СSeNH₂). Found, %: C 55.46; H 3.96; N 10.61. C₁₂H₁₀N₂Se. Calculated, %:
C 55.18; H 3.86; N 10.73.
Preparation of Pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thia(selena)diazine-11-carbonitriles 8a-c
from Cinnamamides 6a,b (General Method A). A suspension of cinnamamide 6a,b (2.0 mmol) in EtOH
(20 ml) was treated with a primary aromatic amine (7 mmol) and excess of 37% formaldehyde free of
paraformaldehyde (2-3 ml, 26.6-40.0 mmol). The mixture was refluxed with stirring for 3-4 min, stirred for 2-3 h
at 20ºC, and left overnight. The tarry residue was filtered off, washed several times with boiling EtOH, and
recrystallized from a suitable solvent.
3,8,10-Tri(4-methylphenyl)-6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido[4',5':4,5]pyrido-
[2,1-b][1,3,5]thiadiazine-11-carbonitrile (8a). Yield 0.33 g (28%). Light-yellow crystals; mp 201-203ºC
(decomp., DMF). IR spectrum, , cm^-1: 2174 (C≡N). ¹H NMR spectrum, , ppm (J, Hz): 2.12 (3Н, s, CH₃); 2.24
2
(3Н, s, CH₃); 2.25 (3Н, s, CH₃); 2.32-2.38 (1Н, m, 6а-СН); 3.33-3.36 (1Н, m) and 3.57 (1Н, dd, J = 8.9,
2
3
³J = 3.6, 7-СН₂); 3.78 (1Н, d, J = 12.7, 9-СН_A); 3.93 (1Н, d, J = 4.9, 10а-СН); 4.64 (1Н, br. s, 6-СН);
2
2
4.87-4.90 (2Н, m, 4-СН_A, 9-СН_B); 5.02 (1Н, d, J = 13.2, 4-СН_B); 5.26 (1Н, d, J = 12.8) and 5.41 (1Н, d,
²J = 12.8, 2-СН₂); 6.68 (2Н, d, ³J = 8.3, Н Ar); 6.85 (2Н, d, ³J = 8.3, Н Ar); 6.90 (2Н, d, ³J = 8.3, Н Ar); 7.08
(2Н, d, ³J = 8.3, Н Ar); 7.13-7.17 (4H, m, Н Ar); 7.25 (2Н, d, ³J = 7.8, Н-2,6 Ph); 7.33 (1Н, t, ³J = 7.4, Н-4 Ph);
7.41 (2Н, dd, J = 7.4, J = 7.8, Н-3,5 Ph). Found, %: C 75.96; H 6.40; N 12.09. C₃₇H₃₇N₅S. Calculated, %:
C 76.12; H 6.39; N 12.00.
3
3
3,6,8,10-Tetraphenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thia-
diazine-11-carbonitrile (8b). Yield 0.13 g (12%). Yellow-orange crystals; mp 189-192ºC (decomp., DMF). IR
1
spectrum, , cm^-1: 2175 (C≡N). H NMR spectrum, , ppm (J, Hz): 2.27-2.32 (1Н, m, 6а-СН); 3.31-3.36 (1Н,
m) and 3.69 (1Н, dd, ²J = 12.0, ³J = 3.7, 7-СН₂); 3.88 (1Н, d, ²J = 12.7, 9-СН_A); 4.04 (1Н, d, ³J = 4.9, 10а-СН);
2
2
4.69 (1Н, br. s, 6-СН); 4.94 (1Н, d, J = 13.7, 4-СН_A); 5.07-5.10 (2Н, two overlapping doublets: d, J = 13.7,
4-СН_B and d, ²J = 12.7, 9-СН_B); 5.32 (1Н, d, ²J = 12.7) and 5.45 (1Н, d, ²J = 12.8, 2-СН₂); 6.71 (1Н, t, ³J = 7.3,
H Ph); 6.76 (2Н, d, ³J = 8.3, H Ph); 6.86 (1Н, t, ³J = 7.3, H Ph); 6.97-7.01 (3H, m, H Ph); 7.10 (2Н, dd, ³J = 7.3,
³J = 7.8, H Ph); 7.25-7.35 (9H, m, H Ph); 7.40-7.43 (2H, m, H Ph). Found, %: C 75.16; H 5.85; N 13.05.
C₃₄H₃₁N₅S. Calculated, %: C 75.39; H 5.77; N 12.93.
3,8,10-Tri(4-methylphenyl)-6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido[4',5':4,5]pyrido-
[2,1-b][1,3,5]selenadiazine-11-carbonitrile (8c). Yield 0.32 g (25%). Light-brown, finely crystalline powder;
1
decomp. temp. > 160ºC (DMF). IR spectrum, , cm^-1: 2176 (C≡N). H NMR spectrum, , ppm (J, Hz): 2.15
(3Н, s, CH₃); 2.22-2.32 (1Н, m, 6а-СН); 2.26 (3Н, s, CH₃); 2.27 (3Н, s, CH₃); 3.03-3.06 (1Н, m) and 3.35 (1Н,
br. d, ²J = 8.8, 7-СН₂); 3.85 (1Н, d, ²J = 12.7) and 4.75 (1Н, d, ²J = 12.7, 9-СН₂); 3.90 (1Н, d, ³J = 2.4, Н-10а);
4.53 (1Н, br. s, Н-6); 4.82 (1Н, d, ²J = 13.7) and 4.97 (1Н, d, ²J = 13.7, 4-СН₂); 5.21 (1Н, d, ²J = 10.8) and 5.46
(1Н, d, ²J = 10.8, 2-СН₂); 6.67 (2Н, d, ³J = 8.0, Н Ar); 6.71 (2Н, d, ³J = 8.0, Н Ar); 6.85 (2Н, d, ³J = 8.0, Н Ar);
7.00 (2Н, d, ³J = 8.0, Н Ar); 7.08-7.13 (4H, m, Н Ar); 7.20 (2Н, d, ³J = 7.5, Н-2,6 Ph); 7.28 (1Н, t, ³J = 7.3, Н-4
Ph); 7.36 (2Н, dd, ³J = 7.3, ³J = 7.5, Н-3,5 Ph). Found, %: C 70.23; H 6.00; N 11.21. C₃₇H₃₇N₅Se. Calculated, %:
C 70.46; H 5.91; N 11.10.
Preparation of Pyrimido[4',5':4,5]pyrido[2,1-b][1,3,5]thiadiazine-11-carbonitriles 8a,b,d by
Multicomponent Condensation (General Method B). Et₃N (5 drops) was added to a solution of the
cyanothioacetamide (4a) (0.5 g, 5 mmol) and cinnamaldehyde (0.63 ml, 5 mmol) in EtOH (10 ml) and stirred
for 15 min. Then additional EtOH (10 ml), a primary aromatic amine (3.1 equiv., 15.5 mmol), and 37%
formaldehyde free of paraformaldehyde (4.5 ml, 60 mmol) were added in succession. The solution obtained was
refluxed for 2-3 min with vigorous stirring, stirred at 20ºC for 3-4 h, and left overnight. The tarry precipitate
was separated, treated with EtOH, filtered, washed twice with boiling EtOH, and recrystallized.
Compound 8a. Yield 0.53 g (18%); mp 201-203ºC (decomp., DMF–EtOH). The spectral parameters
were identical to those of a sample obtained using method A.
1559

Compound 8b. Yield 0.19 g (7%); mp 188-190ºC (decomp., DMF). The spectral parameters were
identical to those of a sample obtained using method A.
3,8,10-Tri(4-methoxyphenyl)-6-phenyl-3,4,6a,7,8,9,10,10a-octahydro-2H,6H-pyrimido-[4',5':4,5]-
pyrido[2,1-b][1,3,5]thiadiazine-11-carbonitrile (8d). Yield 0.73 g (23%). Colorless, finely crystalline powder;
mp 191-193ºC (decomp., EtOH–acetone 1:1). IR spectrum, , cm^-1: 2175 (C≡N). ¹H NMR spectrum, , ppm (J,
2
Hz): 2.23-2.31 (1Н, m, 6а-СН); 3.30-3.33 (1Н, m) and 3.39 (1Н, br. d, J = 8.1, 7-СН₂); 3.61 (3Н, s, OСН₃);
3
2
3.71-3.74 (7H, m, 2OСН₃, 9-СН_A); 3.79 (1Н, d, J = 2.7, 10а-СН); 4.54 (1Н, br. s, 6-СН); 4.68 (1Н, d, J =
12.6, 9-СН_B); 4.84 (1Н, d, ²J = 13.2) and 4.99 (1Н, d, ²J = 13.2, 4-СН₂); 5.20 (1Н, d, ²J = 12.4) and 5.39 (1Н, d,
²J = 12.4, 2-СН₂); 6.70 (2Н, d, ³J = 8.9, Н Ar); 6.80 (2Н, d, ³J = 8.9, Н Ar); 6.83-6.86 (4H, m, Н Ar); 6.90 (2Н,
3
d, J = 8.6, Н Ar); 7.19-7.23 (4Н, m, Н Ar); 7.29-7.32 (1Н, m, Н-4 Ph); 7.38 (2Н, dd, ³J = 7.0, ³J = 7.5, Н-3,5
Ph). Mass spectrum, m/z (I_rel, %): 632.3 [М+H]⁺, 497.3 [М+Н-ArN=CH₂]⁺, 362.1 [М+Н-2ArN=CH₂]⁺, 228.4
[М+Н-3ArN=CH₂]⁺. Found, %: C 70.20; H 5.99; N 11.17. C₃₇H₃₇N₅O₃S. Calculated, %: C 70.34; H 5.90; N
11.08.
X-ray Structural Investigation of Compound 8a. Crystals of compound 8a are monoclinic,
C₃₇H₃₇N₅S, at 298 K: a 10.5638(7), b 9.2115(7), c 32.074(2) Å; β 92.996(6)º, V 3116.8(4) ų, M=583.78; Z 4;
space group P2₁/c; d_calc 1.244 g/cm³; (MoK) 0.138 mm^-1; F(000) 1240. The unit cell parameters and
intensities of 23684 reflections (9913 independent, R_int 0.025) were measured on an Xcalibur 3 automatic, four
circle diffractometer (MoK radiation, graphite monochromator, CCD detector, -scanning to 2_max 63.6º). The
structure was solved by the direct method using the SHELX-97 software package [20]. The position of the
hydrogen atoms was calculated geometrically and refined using the "riding" model with U_iso = nU_eq for the
attached atom (n = 1.5 for methyl groups and n = 1.2 for remaining hydrogen atoms). The structure was refined
in F² full-matrix least-squares analysis in the anisotropic approximation for non-hydrogen atoms to wR₂ 0.151
for 9913 reflections (R₁ 0.060 for 5024 reflections with F > 4(F), S 1.02). The full crystallographic data has
been placed at the Cambridge Crystallographic Data Center as deposit CCDC 874747.
The authors thank Dr. O. V. Shishkin of the Scientific-Technological Complex "Institute of
Monocrystals", National Academy of Sciences of Ukraine, Kharkov for carrying out the X-ray structural
investigation.
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