Crystal structure of a nucleoside analogue, 2′,3′-dideoxy-3′-fluoro-5-chlorocytidine

The title compound, 1-(2,3-dideoxy-3-fluoro--d-erythro pentofuranos-1-yl)-5-chlorocytosine, crystallises in the orthorhombic space groupP2₁2₁2₁ witha=5.142(1),b=14.177(2),c=15.721(2) Å,Z=4. The crystal structure was solved by the heavy atom method and refined by full-matrix least-squares method to a finalR value of 0.031 for 1629 unique observed reflections. The N-glycosidic torsion angle is –156.1(2)° and the sugar moiety is anti to the cytosine base. The sugar pucker is ₂ ³ T withP=178.2(1)° and=31(1)°. The atom 05 is in a +sc conformation with respect to the furanose ring. The molecular packing in the crystal is stabilized by N-HN, N-HO, O-HO hydrogen bonds and C-HO close contacts.     

Crystal and molecular structure ofp-aminobenzene sulfonacetamide sodium [sulfacetamide sodium] monohydrate

The crystal and molecular structure ofp-aminobenzene sulfonacetamide sodium, C₈H₉N₂NaO₃S·H₂O, an important substituted sulfa drug, has been determined from diffractometric data using MoK radiation. The crystals are monoclinic, witha=6.614(2),b=23.788(6),c=7.012(2) Å,=103.13(2)°, and space groupP2₁/c. The structure was solved by the heavyatom method, and refined by full-matrix least squares to a finalR value of 0.040 with 1435 unique reflections. In packing, the molecules form dimers through pairs of N-HN and N-HO hydrogen bonds. The molecules are further stabilized by O-HO and O-HN hydrogen bonds.     

Crystal structure of a nucleoside analog, 2′,3′-dideoxy-3′-azido-5-chlorocytidine

The title compound, l-(2,3-dideoxy-3-azido--D-erythro pentofuranos-1-yl)-5-chlorocytosine, crystallizes in the orthorhombic space groupP2₁2₁2₁ witha=5.840(1),b=13.780(1),c=15.396(2)Å,Z=4. The structure was solved by direct methods and refined by full-matrix least-squares calculations to a finalR value of 0.033 for 1688 unique observed reflections. The N-glycosidic torsion angle has a value of –160.8(1)°, in the and range. The sugar pucker is ₂ ³ T withP=180(1)° and=34(1)°. The C4–C5 conformation is +sc with =50.8(2)°. The azido group is nonlinear and oriented trans to the C3–C4 bond. The molecular packing in the crystalline space is stabilized by N-HN, N-HO, O-HO hydrogen bonds and C-HO close contacts.     

Crystal and molecular structure of (±)-1-phenyl-2-amino-1-propanol,C9H13NO

The crystal structure of (±)-phenylpropanolamine has been determined by single-crystal X-ray diffraction methods. The structure was solved by direct methods and refined by least-squares toR=0.055 andR _w=0.045 for 2000 reflections (I2 (I)). The molecule was found to adoptgauche geometry. Inter- and intramolecular N-HO and O-HN hydrogen bonds were observed in the crystal structure.     

Structure of fruticuline B: A new natural anthracene quinodimethide of abietanoid origin

The title compound is C₁₉H₁₈O₄·1/2 CH₃OH, triclinic,P¯1,a=9.891(2),b=13.273(4),c=13.860(4) Å,a=66.47(2),=86.91(2), and =85.59(2)°. The structure was solved by direct methods and refined by least-squares techniques to anR factor of 0.082 for 2282 observed reflections. The X-ray structure uniquely resolves the one remaining ambiguity, namely the assignment of the correct structure4. There are two crystallographically independent molecules (A and B) and one disordered methanol molecule. Both molecular skeletons show small distortions from planarity with inclinations of 1.7 and 4.0° between the outermost rings A/C in molecules A and B, respectively. Intramolecular hydrogen bonds of the form O(3A)-HO(2A) and O(3B)-HO(2B) are observed in molecules A and B, respectively. The molecules are linked by pairs of O(3A)-HO(2B) and O(3B)-HO(2A) hydrogen bonds. The dimerlike structures are stabilized by intermolecular C-HO interactions and van der Waals forces.     

Structure of 6-aminobenzofuran-2-sulfonamide: A tropically active carbonic anhydrase inhibitor

Crystals of the title compound are triclinic. Space groupP1,a=8.652(2),b=5.184(2),c=5.050(2)Å,=100.26(3)°,=100.33(4)°, =72.82(3)°. The structure was solved by direct methods and refined by a full-matrix, least-squares procedure toR=0.033 for 1168 observed [I >2(I)] reflections. The sulfonamide group is at a right angle to the benzofuran ring and the dihedral angle between the benzene and furan ring is 2.0(1)°. In the crystal packing the molecules are linked together by N-HO and N-HN type hydrogen bonds arranging themselves in such a way that there are alternate hydrophobic and hydrophilic regions extended along the a-axis.     

C-H⋯π(Ar)⋯Cl-C,C-Cl⋯π(Ar), Cl⋯Cl and other interactions in the crystal structure of 6-benzoyl-2,4-bis(trichloromethyl)-1,3-benzdioxin

The title compound is monoclinic,P2₁/n,Z=4,a=9.934(1),b=18.399(2),c=11.098(2)Å, =111.08(1)°. The molecule can conveniently be visualized as a benzophenone molecule with one of the aromatic rings fused to a 1,3-dioxin ring which adopts a distorted envelope conformation withcis-trichloromethyl groups substituted at positions 2 and 4. An interaction, observed for the first time, involves a hydrogen atom and a chlorine atom from opposite sides of the same aromatic ring to give C-H-(Ar)Cl-C. The parameters are Hring-centroid 2.63 A, Clring centroid 3.41 Å, Hring-centroidCl 167°, C-Hring centroid 159°, C-Clring centroid 150.2°. The (Ar) system is that of the unfused aromatic ring. A second (Ar) Cl-C interaction occurs but this time with the (Ar) system of the fused aromatic ring. The ClCl and ClO(=C) interactions form the familiar zig-zag pattern which has been noted for many chloroaromatic compounds.     

Crystal structure of a nucleoside analog: 2′,3′-dideoxy-3′-fluoro-5-bromocytidine

The title compound crystallizes in the orthorhombic space groupP2₁2₁2₁ witha=5.084(1),b=14.322(3),c=16.065(2)Å,Z=4. The structure was solved by the heavy atom method and refined by full-matrix least-squares calculations to a finalR value of 0.033 for 1106 unique observed reflections. The N-glycosidic torsion anglex has a value of –153.7(4)°, in the anti-range. The sugar pucker is²T₃ withP=175(1)° and=30(1)°. The C4-C5 conformation is + sc with =46.7(7)°. The structure is stabilized by N-HN, N-HO and O-HO hydrogen bonds and C-HO close contacts.     

Crystal structure of 1,3-(N,N′-benzamide)-2-methyl-1-pentene

Crystals of the title compound are monoclinic (C20H22N2O2): space groupP2₁/n,a=11.800(3),b=13.820(2),c=11.004(3) Å,=92.74(3)°. The structure was solved by direct methods and refined by block-matrix least-squares procedure to giveR=0.078 andRw=0.076 for 1960 reflections above 3(I). The two amide groups are not coplanar with respect to their benzene rings. An intramolecular N-HO hydrogen bond was found in the molecules which are joined in chains by other strong N-HO hydrogen bonds.     

Two acetylamino derivatives of 2,4-bis(trichloromethyl)-1,3-benzdioxin showing different types of hydrogen bonding: (a) (C13C)CH⋯O=C and (b) N-H⋯O=C

8-Acetylamino-6-methyl-2,4-bis(trichloromethyl)-1,3-benzdioxin, (I), is monoclinic,P2₁/c,a=15.174(4),b=11.977(7),c=9.911(3)Å,=99.72(2)°. 6-Acetylamino-2,4-bis(trichloromethyl)-1,3-benzdioxin, (II), is monoclinic,P2₁/_n,a=5.927(4),b=40.623(1),c =7.120(3)Å,=91.39(4)°. In compound (I) the imino hydrogen atom is locked in an intramolecular hydrogen bond to the proximate oxygen atom of the heterocyclic ring and is not available for intermolecular hydrogen bonding. Instead the weakly acidic hydrogen atom [Cl₃C-C(2)]H takes part in a hydrogen bond to the carbonyl oxygen atom in another molecule. In compound (II) a normal intermolecular hydrogen bond of the type N-HO=C occurs. The 6-acetylam-ino group is twisted about the (C_Ar-N) bond such that the angles NHO=C, C_ArH_ArO=C, NHOH_ArC_Ar, at the carbonyl oxygen group total 360° (where NH is in the related molecule). The packing in both compounds takes the form of infinite chains and in compound (II) partial overlap of the aromatic ring and the acetylamino group, with very little offset, also occurs.     

Polymorphs of nitrofurantoin. I. Preparation and X-ray crystal structures of two monohydrated forms of nitrofurantoin

The preparation and X-ray crystal structures of two monohydrates of the antibacterial drug nitro furantoin are reported. MonohydrateI crystallizes in the monoclinic space groupP2₁ n and monohydrateII in the orthorhombic space group Pbca. The nitrofurantoin molecule maintains the same, planar conformation in both crystals. The molecular packing arrangements inI andII are distinctly different,I possessing a layer structure while inII the packing is based on a herring bone motif. Hydrogen bonds of the type O-HO, N-HO, O-HN and C-HO stabilize the crystal structures.     

Cl⋯π(Ar), Cl⋯Cl,and other intermolecular interactions in the crystal structure of 8-nitro-6-methyl-2-trichloromethyl-4-dichloromethylene-1,3-benzodioxin

Crystals of the title compound are monoclinic,P2₁,a=9.791(4),b=7.129(3),c=10.428(3)Å,=91.84(3)°,V=727.50ų,Z=2. The structure was solved by direct methods, from data collected at room temperature on an Enraf-Nonius CAD4 diffractometer, and refined by full matrix least squares to a finalR value of 0.045 using 2466 reflections. The molecules form stacks along theb axis of the formA, B, A, B(A=dichloromethylene group; B=aromatic ring in the molecule at –x, 1/2+y, –z to the molecule atx, y, z containing A). Cl(Ar),, ClCl, ClO(N), (Cl₃C)HO intermolecular interactions are also present. An inverse correlation between the (C)ClCl(C) distance and the difference in the corresponding pairs of C-ClCl angles is observed and is interpreted in terms of incipient nucleophile: electrophile attack.     

Crystal structure of 4,6-dinitro-1-(5-tetrazolyl)-1H-indazole trihydrate

The title compound, C₈H₄N₈O₄·3H₂O, crystallizes in space groupP¯1 with cell constantsa=7.022(1),b=9.507(2),c=10.906(2) Å,=84.99(1),=71.89(1),=72.56(1)°,Z=2, andV _c =660.2 ų. The structure was solved by direct methods using diffractometer data and was refined by full-matrix least-squares methods to anR value of 0.060 for 2112 observed reflections. The molecule, consisting of a phenyl ring fused to a pyrazole ring with a tetrazole ring connected to it equatorially, is planar except for the N(7) nitro-group oxygen atoms. The structure is stabilized by a three-dimensional network of O-HO, O-HN, and N-HO hydrogen bonds through the water molecules.     

Crystal and molecular structure of 4-p-hydroxyphenyl-2,2,4-trimethylthiachroman-1,1-dioxide

The title compound1 crystallizes as colorless polyhedra in the monoclinic polar space groupCc, witha=8.107(2),b=21.577(3),c=9.542(2)Å,=103.58(2)°, by contrast with its thioether precursor3, crystals of which have the trigonal space groupR¯3. The structure comprises infinite chains of molecules linked head-to-tail by S=OHO hydrogen bonds of length 2.723(2)Å, with HO contact 1.97(4)Å and O-HO 177(3)°; HÔ=S 146(1)°.     

Crystal structure of 5-fluoro-1-(2,3,6-trideoxy-α-l-glycero-hex-2-enopyranos-4-ulosyl)uracil

The present compound crystallizes in the space groupP2₁2₁2₁ withZ=4 and cell parametersa=21.687(2),b=8.155(3),c=5.883(2)Å. The structure was solved by direct methods and refined by full-matrix least-squares to a finalR value of 0.045 for 1153 observed reflections. The N-glycosidic torsion angle _CN is in the anti-range and the pyranosyl ring adopts a distorted half-chair conformation with ₂=142.7(4)°, ₂=124.4(3)° andQ=0.456(2)Å. In the crystal packing the molecules are linked together by N-HO hydrogen bonds and C-HO contacts.     

Crystal structure and conformation of N-(t-butoxycarbonyl)-L-isoleucyl-L-alanine benzylester

C₂₂N₂O₅H₃₂,M _r =404.5, monoclinic,C2,a=21.781(5),b=5.065(1),c=22.333(4)Å,=112.81(2)°,V=2271.1(9)ų,D _calc=1.148 g cm³, (CuK )=1.5418 Å,=5.89 cm^–1,F(000)=848, room temperature,R=0.058 for 2178 unique reflections [I2.5(I)]. The peptide linkage is in thetrans conformation. The molecule adopts the-sheet structure. The crystal structure is stabilized by a three-dimensional network of N-HO and C-HO hydrogen bonds.DCB Contribution No. 813.     

Crystal structures of two therapeutically active 2-imidazolines: naphazoline nitrate and tymazoline hydrochloride monohydrate

Naphazoline·HNO₃ (1): C₁₄H₁₅N₃O₃,M _r =273.3, crystallizes in the orthorhombic space group Pbca(Z=8) witha=12.028(1),b=14.408(2) andc=15.894(2) Å,V=2754.4 ų,D _x =1.318 g cm^–3,=0.70 mm^–1, (CuK)=1.54178 Å,F(000)=1152. FinalR=0.092 andwR=0.088 for 1348 observed reflections collected on a diffractometer. The structure was solved with direct methods, it shows two distinct positions of the naphthyl group with populations about 0.5, which differ by a 180 rotation. As in other arylmethyl-2-imidazolines, the imidazoline ring is approximately perpendicular to the aromatic ring. The molecules are linked by two hydrogen bonds N(3)-HO (nitrate anion)H-N(1) into infinite chains running along the 2₁ axis in the [100] direction. Tymazoline·HC1·H₂O (2): C₁₄H₂₃ClN₂O₂,M _r =286.8, crystallizes in the monoclinic space groupP2₁/n (Z=4) witha=8.136(1),b=10.015(1),c=18.601(1) Å and,=97.20(1)°,V=1503.7 ų D _x =1.266 g cm^–3,=2.27 mm^–1, (CuK)=1.54178 Å,F(000)=636. FinalR=0.115 andwR=0.119 for 3073 observed reflections collected on a diffractometer. The structure was solved with direct methods. Unlike other aryloxymethyl-2-imidazolines, the molecule is almost planar with an angle of 12.8(2)° between the two rings. Hydrogen bonding networks consist of N(1)-HO (water)Cl^–H-N(3) chains joined by an additional link O(water)-HCl^– between chains running in opposite directions.     

Preparation and X-ray structure of [(methyl quinaldate)2H]+ [AuBr4]−

The crystal structure of the title complex (R _F =0.051 for 2384 observed MoK data) consists of a packing of tetrabromoaurate(III) anions and [(methyl quinaldate)₂H]⁺ cations in which the two planar heterocyclic ring moieties are interlinked by a proton to form a NHN hydrogen bond of length 2.88(1) Å; the dihedral angle of the planes is 79.5°. The infrared spectrum of the compound is also discussed.     

Polymorphs of nitrofurantoin. 2. Preparation and X-ray crystal structures of two anhydrous forms of nitrofurantoin

The preparation and X-ray crystal structures of two polymorphs of the antibacterial drug nitrofurantoin are reported. The -polymorph is triclinic, space groupP¯1 witha=6.774(1),b=7.795(1),c=9.803(2)Å, =106.68(1),=104.09(2), =92.29(1)°,Z=2. The-polymorph is monoclinic, space groupP2₁/n witha=7.840(5),b=6.486(1),c=18.911(6)Å,=93.17(3)°,Z=4. The nitrofurantoin molecules adopt the same, planar conformation in both polymorphs. Both crystal structures are built up from layers held together by van der Waals forces. In each polymorph, intralayer cohesion is effected by N-HO and C-HO hydrogen bonds, but their arrangements differ in the two crystals. The significance of the C-HO hydrogen bond, now known to occur in four modifications of nitrofurantoin, is discussed.     

Crystal structure of μ-adeninatobis (methylmercury (II)) perchlorate monohydrate

The title compound belongs to the triclinic space groupP¯1,a= 8.189 Å,b = 9.863 Å,c = 10.726 Å, = 69.93 °, = 68.62 °, = 73.66 °, andZ = 2. The structure was refined on 1337 observed reflections to anR factor of 0.042. The crystals contain [adeninato(CH₃Hg)₂]⁺ complex cations in which mercury is linearly bonded to N(7) and N(9) of a deprotonated adenine ring. Centrosymmetrically related complex cations are paired via two N(6)-H(6) N(l) hydrogen bonds. Those planar units are stacked in the crystal with a distance of 3.4 Å between rings. The water molecule and the ClO₄ ^-ion are involved in hydrogen bonding and HgO contacts. This structure identifies N(7) as the best residual coordination site after H(9) has been substituted by CH₃Hg.