research communications\(\def\hfill{\hskip 5em}\def\hfil{\hskip 3em}\def\eqno#1{\hfil {#1}}\)

Journal logoCRYSTALLOGRAPHIC
COMMUNICATIONS
ISSN: 2056-9890
Volume 82| Part 4| April 2026| Pages 375-378
https://doi.org/10.1107/S2056989026002720

Crystal structure and Hirshfeld surface analysis of luteolin di­methyl sulfoxide monosolvate

crossmark logo
Jia Xua*

aSchool of Pharmacy, Jiangsu Medical College, Yancheng 224005, People's Republic of China
*Correspondence e-mail: [email protected]

Edited by G. Ferrence, Illinois State University, USA (Received 28 May 2025; accepted 12 March 2026; online 19 March 2026)

The title compound, 3′,4′,5,7-tetrahydroxyflavone dimethyl sulfoxide monosolvate (LUT-DMSO), C2H6OS·C15H10O6, crystallizes in the monoclinic space group P21. The LUT mol­ecule adopts a planar conformation, and the crystal structure is consolidated by extensive hydrogen-bonding inter­actions. Hirshfeld surface analysis indicates that the predominant inter­molecular inter­actions are O⋯H/H⋯O, C⋯H/H⋯C, and H⋯H, with these contacts contributing significantly to the overall cohesion of the crystal.

CCDC reference: 2537224

Similar articles

1. Chemical context

Luteolin (3′,4′,5-tetra­hydroxy­flavone) is a naturally occurring flavonoid found in multiple flora such as honeysuckle, scutellaria (Lamiaceae), dandelion (Asteraceae), as well as peanut shells and corn whiskers (Mahwish et al., 2025View full citation). This compound has received worldwide research inter­est due to its wide variety of biological activities, particularly anti­oxidant, anti-inflammatory, anti­cancer, and neuroprotective properties (Zhang & Ma, 2024View full citation). Luteolin is a potent anti­oxidant which promotes the expression of anti­oxidant enzymes (e.g. SOD, heme oxygenase-1, HO-1) and scavenges reactive oxygen species (ROS) therefore reducing oxidative stress. Luteolin's anti-inflammatory activity results from the inhibition of numerous pro-inflammatory cytokines and enzymes (TNF-α, IL-6, COX-2, iNOS) and the modulation of cellular signalling pathways (NF-κB, MAPK/AP-1) (Pandey et al., 2025View full citation). With regards to cancer, luteolin has been shown to induce apoptosis, inhibit cell proliferation, and reduce angiogenesis in various cancer models from breast, colon, and pancreatic cancer (Prasher et al., 2022View full citation). Research has shown that luteolin exerts neuroprotection in models of Alzheimer's and Parkinson's disease by decreasing neuro-inflammation, oxidative damage, and neuronal apoptosis (Zhu et al., 2024View full citation).

[Scheme 1]

In this study, we report the crystal structure and Hirshfeld surface analysis of luteolin dimethyl sulfoxide solvate, which has not previously been reported in the literature.

2. Structural commentary

LUT-DMSO crystallizes in the monoclinic space group P21. The asymmetric unit consists of one LUT mol­ecule and one DMSO mol­ecule, as depicted in Fig. 1[link]. The luteolin mol­ecules adopt a planar configuration due to conjugation in the flavonoid backbone. The dihedral angle between the fused rings is 2.2 (5)° and that between the phenyl ring and the fused ring system is 3.1 (4)°. The torsion angles for O3—C4—C5—C6, O3—C4—C5—C10, C3—C4—C5—C6, and C3—C4—C5–C10 are 177.7 (9), −1.9 (14), −1.8 (16), and 178.6 (10)°, respectively. Several intra­molecular hydrogen bonds are also observed within the LUT mol­ecules (O4—H4⋯O5, O6—H6⋯O7, and C10—H10⋯O3; Table 1[link]).

Table 1
Hydrogen-bond geometry (Å, °)

D—H⋯A D—H H⋯A DA D—H⋯A
O1—H1⋯O5i 0.84 1.83 2.649 (11) 163
O2—H2⋯O1ii 0.84 2.14 2.846 (11) 142
O2—H2⋯O2ii 0.84 2.35 2.989 (11) 133
O4—H4⋯O5 0.84 1.79 2.626 (10) 170
O6—H6⋯O7iii 0.84 1.79 2.626 (10) 170
C3—H3⋯O1iv 0.95 2.54 3.220 (13) 129
C10—H10⋯O3 0.95 2.35 2.682 (11) 100
C16—H16C⋯O4iii 0.98 2.44 3.293 (15) 145
C17—H17A⋯O7v 0.98 2.39 3.308 (18) 156
Symmetry codes: (i) Mathematical equation; (ii) Mathematical equation; (iii) Mathematical equation; (iv) Mathematical equation; (v) Mathematical equation.
[Figure 1]
Figure 1
The mol­ecular structure of LUT-DMSO, with atomic displacement ellipsoids drawn at the 30% probability level, showing the atom labeling. Hydrogen atoms are represented as small spheres with arbitrary radii.

3. Supra­molecular features

In the crystal, each LUT and DMSO mol­ecule is involved in extensive hydrogen-bonding inter­actions, contributing to crystal cohesion (Fig. 2[link], Table 1[link]). DMSO mol­ecules are connected to neighboring DMSO mol­ecules through C17—H17A⋯O7 inter­actions, forming a chain-like structure. The DMSO mol­ecules also inter­act with LUT mol­ecules through C16—H16C⋯O4 and O6—H6⋯O7 hydrogen bonds. The LUT mol­ecules are connected to each other through O1—H1⋯O5, C3—H3⋯O1, O2—H2⋯O1, and O2—H2⋯O2 hydrogen bonds. Collectively, these interactions give rise to a two-dimensional network that lies parallel to the (100) plane, as illustrated in Fig. 2[link].

[Figure 2]
Figure 2
Hydrogen-bond networks in LUT-DMSO, showing the two-dimensional network parallel to the (100) plane (hydrogen bonding is indicated by orange dashed lines).

To validate the hydrogen-bonding inter­actions observed in LUT-DMSO, we have compared the observed donor–acceptor distances with those found in other luteolin-containing crystal structures, such as ZIKPUG01 and ZIKPUG02 (cocrystals with isonicotinamide; Sowa et al., 2013View full citation) and VOHKIO (a dapsone-luteolin-ethanol solvate; Jiang et al., 2014View full citation). In our structure, the intra­molecular O⋯O distances are 2.626 (10) Å (O4—H4⋯O5) and the C⋯O distance is 2.682 (11) Å (C10—H10⋯O3). The inter­molecular O⋯O distances range from 2.649 (11) to 2.989 (11) Å, and the inter­molecular C⋯O distances range from 3.220 (13) to 3.308 (18) Å. When compared with other luteolin-containing crystal structures, all DA distances in the title structure fall within typical ranges for O—H⋯O and C—H⋯O hydrogen bonds, except for the intra­molecular C⋯O contact (C10—H10⋯O3), which appears slightly shorter. However, this short distance is likely due to the rigidity of the luteolin backbone, which forces the O3 and C10 atoms into close proximity, rather than an artefact of the riding model. The H⋯A distance of 2.35 Å for this inter­action is well within the range of normal C—H⋯O hydrogen bonds. No similar intra­molecular C—H⋯O hydrogen bond has been reported in other LUT structures, possibly because of differences in mol­ecular conformation or crystal packing. Therefore, we conclude that the hydrogen-bonding geometry in the title structure is reasonable and consistent with known LUT-containing crystals.

4. Hirshfeld surface analysis

The Hirshfeld surface analysis of LUT-DMSO was conducted to evaluate the inter­molecular inter­actions within the crystal structure. Hirshfeld surfaces and fingerprint plots (Spackman & McKinnon, 2002View full citation; Spackman & Jayatilaka, 2009View full citation) were generated using CrystalExplorer software (Spackman et al., 2021View full citation). Fig. 3[link] shows the Hirshfeld surfaces and the corresponding two-dimensional fingerprint plots for the LUT mol­ecule, while Fig. 4[link] illustrates the same for the DMSO mol­ecule.

[Figure 3]
Figure 3
Hirshfeld surfaces and the corresponding two-dimensional fingerprint plots of various hydrogen-bonding and van der Waals inter­actions for the LUT mol­ecule of LUT-DMSO. The di and de values represent the closest inter­nal and external distances (in Å), respectively, from given points on the Hirshfeld surface.
[Figure 4]
Figure 4
Hirshfeld surfaces and the corresponding two-dimensional fingerprint plots of various hydrogen-bonding and van der Waals inter­actions for the DMSO mol­ecule of LUT-DMSO. The di and de values represent the closest inter­nal and external distances (in Å), respectively, from given points on the Hirshfeld surface.

For the LUT mol­ecule, the predominant inter­molecular inter­actions are O⋯H/H⋯O, C⋯H/H⋯C, H⋯H, and S⋯H/H⋯S, which account for 84.3% of the total inter­actions, indicating their significant role in consolidating the structure. Among these, O⋯H/H⋯O inter­actions are the most prevalent, contributing 30.8% of the Hirshfeld surface, followed by C⋯H/H⋯C (26.9%) and H⋯H (25.0%) inter­actions. The S⋯H/H⋯S inter­action is relatively weak, contributing only 1.6% of the Hirshfeld surface.

For the DMSO mol­ecule (Fig. 4[link]), the most significant contacts are H⋯H, O⋯H/H⋯O, S⋯H/H⋯S and C⋯H/H⋯C. The H⋯H inter­action is the dominant contributor, accounting for 46.4%, followed by O⋯H/H⋯O (35.9%), S⋯H/H⋯S (9.3%) and C⋯H/H⋯C (7.0%) inter­actions. The total contribution of these inter­actions is 98.6%, emphasizing their dominant role in the structural cohesion.

In both mol­ecules, the Hirshfeld surface offers a clear depiction of mol­ecular inter­actions, with the majority of red spots on the surface corresponding to O⋯H inter­actions, which are also reflected in the 2D fingerprint plots as prominent spikes. These findings emphasize the crucial role of hydrogen bonding and van der Waals inter­actions in determining the packing and cohesion of the LUT-DMSO crystal.

5. Database survey

A survey of the Cambridge Structural Database WebCSD, May 2025; Groom et al., 2016View full citation) did not reveal any structures of LUT-DMSO. The survey revealed seven crystal structures that related to LUT compounds, viz. OJEQUP, EJEPUG, EJEQIV, VOHKIO, ZIKPUG, ZIKPUG01 and ZIKPUG02. OJEQUP (Cox et al., 2003View full citation) is a hemihydrate of luteolin, although the water mol­ecules were disordered and not located, which crystallize in the monoclinic C2 space group. EJEPUG and EJEQIV (He et al., 2016View full citation) are cocrystals of LUT with proline. Luteolin is a poorly soluble compound and the cocrystallization of LUT with L-proline and D-proline is useful for solubility enhancement. Additionally, the structures VOHKIO (a dapsone-luteolin ethanol solvate; Jiang et al., 2014View full citation) and ZIKPUG, ZIKPUG01, ZIKPUG02 (cocrystals of luteolin with isonicotinamide, with ZIKPUG and ZIKPUG01 representing one polymorph and ZIKPUG02 a second polymorph; Sowa et al., 2013View full citation) have also been reported, further illustrating the versatility of luteolin in forming multicomponent crystals and its polymorphic behavior.

6. Synthesis and crystallization

The commercially available form of luteolin (98%) was purchased from Aladdin. LUT (50 mg, 0.18 mmol) was dissolved in 15 mL of DMSO by heating. Colorless plate-like single crystals were obtained by slowly evaporating the filtrated solution at room temperature for 30 days.

7. Refinement

Crystal data, data collection and structure refinement details are summarized in Table 2[link]. Due to the limited data quality, the hydrogen atoms attached to oxygen atoms could not be located in the difference-Fourier map. Therefore, all H atoms were placed in geometrically calculated positions and refined using a riding model.

Table 2
Experimental details

Crystal data
Chemical formula C2H6OS·C15H10O6
Mr 364.36
Crystal system, space group Monoclinic, P21
Temperature (K) 170
a, b, c (Å) 6.676 (2), 5.6991 (17), 20.724 (6)
β (°) 90.749 (11)
V3) 788.4 (4)
Z 2
Radiation type Mo Kα
μ (mm−1) 0.25
Crystal size (mm) 0.12 × 0.06 × 0.04
 
Data collection
Diffractometer Bruker APEXII CCD
Absorption correction Multi-scan (SADABS; Krause et al., 2015View full citation)
Tmin, Tmax 0.479, 0.745
No. of measured, independent and observed [I > 2σ(I)] reflections 5797, 3000, 1894
Rint 0.083
(sin θ/λ)max−1) 0.628
 
Refinement
R[F2 > 2σ(F2)], wR(F2), S 0.095, 0.284, 1.04
No. of reflections 3000
No. of parameters 232
No. of restraints 1
H-atom treatment H-atom parameters constrained
Δρmax, Δρmin (e Å−3) 1.08, −0.56
Absolute structure Flack x determined using 528 quotients [(I+)−(I)]/[(I+)+(I)] (Parsons et al., 2013View full citation)
Absolute structure parameter 0.3 (2)
Computer programs: APEX5 (Bruker, 2019View full citation) and SAINT (Bruker, 2019View full citation), SHELXT2014/5 (Sheldrick, 2015aView full citation), SHELXL2025/1 (Sheldrick, 2015bView full citation), OLEX2 (Dolomanov et al., 2009View full citation), DIAMOND (Pennington, 1999View full citation) and PLATON (Spek, 2020View full citation).

Supporting information

CCDC reference: 2537224

Crystal structure: contains datablock I. DOI: https://doi.org/10.1107/S2056989026002720/ej2014sup1.cif

Supporting information file. DOI: https://doi.org/10.1107/S2056989026002720/ej2014Isup3.cml

Structure factors: contains datablock I. DOI: https://doi.org/10.1107/S2056989026002720/ej2014Isup5.hkl

checkCIF report


Computing details top

3',4',5,7-Tetrahydroxyflavone dimethyl sulfoxide monosolvate top
Crystal data top
C2H6OS·C15H10O6F(000) = 380
Mr = 364.36Dx = 1.535 Mg m3
Monoclinic, P21Mo Kα radiation, λ = 0.71073 Å
a = 6.676 (2) ÅCell parameters from 1758 reflections
b = 5.6991 (17) Åθ = 3.0–25.4°
c = 20.724 (6) ŵ = 0.25 mm1
β = 90.749 (11)°T = 170 K
V = 788.4 (4) Å3Plate, colourless
Z = 20.12 × 0.06 × 0.04 mm
Data collection top
Bruker APEXII CCD
diffractometer		1894 reflections with I > 2σ(I)
φ and ω scansRint = 0.083
Absorption correction: multi-scan
(SADABS; Krause et al., 2015)		θmax = 26.5°, θmin = 2.0°
Tmin = 0.479, Tmax = 0.745h = 78
5797 measured reflectionsk = 77
3000 independent reflectionsl = 2525
Refinement top
Refinement on F2Hydrogen site location: inferred from neighbouring sites
Least-squares matrix: fullH-atom parameters constrained
R[F2 > 2σ(F2)] = 0.095 w = 1/[σ2(Fo2) + (0.1706P)2]
where P = (Fo2 + 2Fc2)/3
wR(F2) = 0.284(Δ/σ)max < 0.001
S = 1.04Δρmax = 1.08 e Å3
3000 reflectionsΔρmin = 0.56 e Å3
232 parametersAbsolute structure: Flack x determined using 528 quotients [(I+)-(I-)]/[(I+)+(I-)] (Parsons et al., 2013)
1 restraintAbsolute structure parameter: 0.3 (2)
Primary atom site location: dual
Special details top

Geometry. All esds (except the esd in the dihedral angle between two l.s. planes) are estimated using the full covariance matrix. The cell esds are taken into account individually in the estimation of esds in distances, angles and torsion angles; correlations between esds in cell parameters are only used when they are defined by crystal symmetry. An approximate (isotropic) treatment of cell esds is used for estimating esds involving l.s. planes.

Fractional atomic coordinates and isotropic or equivalent isotropic displacement parameters (Å2) top
xyzUiso*/Ueq
S10.1500 (4)0.6686 (6)0.42114 (13)0.0341 (7)
O30.7284 (9)0.6422 (15)0.7946 (3)0.0290 (17)
O50.2840 (9)1.1285 (14)0.8075 (3)0.0307 (18)
O21.4443 (10)0.7383 (14)0.9875 (4)0.0338 (19)
H21.4558770.8423731.0159660.051*
O11.3744 (10)0.4339 (13)0.8997 (4)0.0344 (18)
H11.3287770.3261510.8760100.052*
O60.3923 (11)0.2151 (16)0.6316 (4)0.040 (2)
H60.2818190.2088260.6118330.060*
O70.0686 (9)0.6616 (19)0.4402 (3)0.044 (2)
O40.0868 (11)0.9060 (15)0.7183 (4)0.039 (2)
H40.1101421.0069890.7469330.059*
C81.2725 (15)0.7742 (18)0.9529 (5)0.026 (2)
C20.4218 (15)0.9746 (19)0.8028 (5)0.029 (2)
C30.5968 (16)0.9797 (19)0.8422 (5)0.028 (2)
H30.6132721.1030810.8726060.034*
C150.5642 (14)0.6218 (19)0.7539 (5)0.028 (2)
C10.4081 (15)0.7865 (19)0.7581 (5)0.027 (2)
C50.9248 (14)0.8020 (18)0.8774 (5)0.026 (2)
C60.9677 (15)0.9718 (19)0.9236 (5)0.031 (2)
H6A0.8777551.0989730.9294890.038*
C91.2322 (14)0.6052 (18)0.9063 (5)0.028 (2)
C71.1419 (15)0.957 (2)0.9614 (5)0.028 (2)
H71.1700551.0740200.9929510.033*
C40.7407 (16)0.8147 (17)0.8377 (5)0.027 (2)
C101.0600 (14)0.618 (2)0.8688 (5)0.032 (3)
H101.0334880.5018470.8369680.039*
C140.5649 (15)0.436 (2)0.7119 (5)0.030 (2)
H140.6761900.3327210.7093580.036*
C110.2402 (15)0.750 (2)0.7166 (6)0.033 (3)
C130.3934 (16)0.406 (2)0.6728 (5)0.032 (2)
C170.2812 (16)0.694 (3)0.4955 (6)0.043 (3)
H17A0.2587200.8502100.5137070.065*
H17B0.4247910.6711070.4884080.065*
H17C0.2329270.5744150.5255070.065*
C120.2344 (17)0.565 (2)0.6751 (6)0.040 (3)
H120.1212740.5439770.6473970.048*
C160.2299 (19)0.368 (2)0.4044 (6)0.042 (3)
H16A0.1948640.2662270.4407780.063*
H16B0.3752770.3642260.3984100.063*
H16C0.1624380.3109790.3651270.063*
Atomic displacement parameters (Å2) top
U11U22U33U12U13U23
S10.0286 (13)0.0364 (15)0.0373 (14)0.0047 (13)0.0010 (9)0.0028 (14)
O30.020 (3)0.037 (4)0.030 (3)0.004 (4)0.005 (2)0.005 (4)
O50.022 (3)0.037 (5)0.033 (4)0.010 (3)0.008 (3)0.003 (4)
O20.026 (4)0.040 (5)0.035 (4)0.001 (3)0.012 (3)0.007 (3)
O10.029 (4)0.018 (4)0.055 (5)0.009 (3)0.010 (3)0.008 (4)
O60.030 (4)0.051 (6)0.039 (4)0.006 (4)0.008 (3)0.009 (4)
O70.022 (4)0.069 (6)0.040 (4)0.015 (5)0.002 (3)0.006 (5)
O40.032 (4)0.036 (5)0.051 (5)0.013 (4)0.009 (3)0.011 (4)
C80.029 (5)0.023 (5)0.025 (5)0.002 (4)0.006 (4)0.002 (5)
C20.024 (5)0.024 (6)0.037 (6)0.001 (4)0.005 (4)0.004 (5)
C30.033 (6)0.019 (5)0.034 (6)0.004 (4)0.001 (4)0.000 (5)
C150.027 (5)0.032 (6)0.023 (5)0.004 (5)0.007 (3)0.002 (5)
C10.021 (5)0.029 (6)0.033 (6)0.002 (4)0.002 (4)0.001 (5)
C50.017 (5)0.026 (6)0.036 (6)0.005 (4)0.007 (4)0.001 (5)
C60.021 (5)0.024 (6)0.049 (7)0.003 (4)0.005 (4)0.006 (5)
C90.021 (5)0.028 (6)0.036 (6)0.003 (4)0.000 (4)0.000 (5)
C70.035 (6)0.027 (6)0.022 (5)0.007 (5)0.001 (4)0.003 (5)
C40.042 (6)0.013 (5)0.025 (6)0.004 (4)0.004 (4)0.005 (4)
C100.024 (5)0.047 (7)0.026 (5)0.012 (5)0.004 (4)0.001 (5)
C140.024 (5)0.027 (6)0.040 (6)0.007 (4)0.006 (4)0.009 (5)
C110.025 (6)0.034 (6)0.038 (6)0.001 (4)0.003 (4)0.003 (5)
C130.030 (6)0.031 (6)0.034 (6)0.004 (5)0.003 (4)0.006 (5)
C170.038 (6)0.049 (8)0.043 (6)0.009 (6)0.002 (5)0.006 (7)
C120.027 (6)0.049 (7)0.043 (7)0.010 (5)0.007 (5)0.002 (6)
C160.047 (7)0.035 (7)0.045 (7)0.001 (6)0.009 (5)0.011 (6)
Geometric parameters (Å, º) top
S1—O71.518 (7)C15—C141.370 (15)
S1—C171.768 (12)C1—C111.419 (15)
S1—C161.831 (13)C5—C61.388 (15)
O3—C151.380 (11)C5—C41.472 (14)
O3—C41.330 (12)C5—C101.395 (14)
O5—C21.276 (12)C6—H6A0.9500
O2—H20.8400C6—C71.397 (14)
O2—C81.359 (12)C9—C101.382 (14)
O1—H10.8400C7—H70.9500
O1—C91.370 (12)C10—H100.9500
O6—H60.8400C14—H140.9500
O6—C131.382 (14)C14—C131.405 (14)
O4—H40.8400C11—C121.362 (17)
O4—C111.356 (13)C13—C121.398 (15)
C8—C91.389 (15)C17—H17A0.9800
C8—C71.372 (14)C17—H17B0.9800
C2—C31.416 (14)C17—H17C0.9800
C2—C11.420 (15)C12—H120.9500
C3—H30.9500C16—H16A0.9800
C3—C41.348 (14)C16—H16B0.9800
C15—C11.406 (14)C16—H16C0.9800
O7—S1—C17104.0 (5)C8—C7—H7120.0
O7—S1—C16107.9 (6)C6—C7—H7120.0
C17—S1—C1695.7 (6)O3—C4—C3121.6 (9)
C4—O3—C15121.0 (8)O3—C4—C5112.5 (9)
C8—O2—H2109.5C3—C4—C5125.9 (9)
C9—O1—H1109.5C5—C10—H10119.9
C13—O6—H6109.5C9—C10—C5120.2 (10)
C11—O4—H4109.5C9—C10—H10119.9
O2—C8—C9114.6 (9)C15—C14—H14121.6
O2—C8—C7125.5 (9)C15—C14—C13116.8 (9)
C7—C8—C9119.9 (9)C13—C14—H14121.6
O5—C2—C3122.2 (9)O4—C11—C1118.7 (10)
O5—C2—C1121.9 (9)O4—C11—C12120.6 (10)
C3—C2—C1115.9 (9)C12—C11—C1120.7 (10)
C2—C3—H3119.0O6—C13—C14116.8 (9)
C4—C3—C2122.0 (10)O6—C13—C12122.2 (10)
C4—C3—H3119.0C12—C13—C14121.0 (11)
O3—C15—C1119.3 (9)S1—C17—H17A109.5
C14—C15—O3116.4 (9)S1—C17—H17B109.5
C14—C15—C1124.3 (9)S1—C17—H17C109.5
C15—C1—C2120.2 (9)H17A—C17—H17B109.5
C15—C1—C11116.5 (10)H17A—C17—H17C109.5
C11—C1—C2123.3 (9)H17B—C17—H17C109.5
C6—C5—C4120.9 (9)C11—C12—C13120.6 (11)
C6—C5—C10119.0 (9)C11—C12—H12119.7
C10—C5—C4120.1 (9)C13—C12—H12119.7
C5—C6—H6A119.7S1—C16—H16A109.5
C5—C6—C7120.5 (9)S1—C16—H16B109.5
C7—C6—H6A119.7S1—C16—H16C109.5
O1—C9—C8115.9 (9)H16A—C16—H16B109.5
O1—C9—C10123.7 (10)H16A—C16—H16C109.5
C10—C9—C8120.4 (10)H16B—C16—H16C109.5
C8—C7—C6120.0 (10)
O3—C15—C1—C21.4 (15)C15—C14—C13—O6178.5 (9)
O3—C15—C1—C11177.7 (9)C15—C14—C13—C122.8 (17)
O3—C15—C14—C13176.4 (10)C1—C2—C3—C40.6 (15)
O5—C2—C3—C4179.0 (9)C1—C15—C14—C132.8 (16)
O5—C2—C1—C15179.3 (10)C1—C11—C12—C130.4 (17)
O5—C2—C1—C111.8 (16)C5—C6—C7—C80.1 (15)
O2—C8—C9—O12.9 (13)C6—C5—C4—O3177.7 (9)
O2—C8—C9—C10178.6 (10)C6—C5—C4—C31.8 (16)
O2—C8—C7—C6178.6 (10)C6—C5—C10—C90.8 (15)
O1—C9—C10—C5178.3 (9)C9—C8—C7—C60.7 (15)
O6—C13—C12—C11179.6 (10)C7—C8—C9—O1177.7 (9)
O4—C11—C12—C13179.4 (11)C7—C8—C9—C100.8 (15)
C8—C9—C10—C50.0 (15)C4—O3—C15—C10.1 (14)
C2—C3—C4—O32.1 (16)C4—O3—C15—C14179.1 (9)
C2—C3—C4—C5178.4 (10)C4—C5—C6—C7179.5 (10)
C2—C1—C11—O41.7 (16)C4—C5—C10—C9179.6 (10)
C2—C1—C11—C12179.2 (10)C10—C5—C6—C70.9 (15)
C3—C2—C1—C151.1 (14)C10—C5—C4—O31.9 (14)
C3—C2—C1—C11177.8 (10)C10—C5—C4—C3178.6 (10)
C15—O3—C4—C31.9 (14)C14—C15—C1—C2179.5 (10)
C15—O3—C4—C5178.6 (8)C14—C15—C1—C111.5 (16)
C15—C1—C11—O4179.3 (9)C14—C13—C12—C111.7 (18)
C15—C1—C11—C120.2 (16)
Hydrogen-bond geometry (Å, º) top
D—H···AD—HH···AD···AD—H···A
O1—H1···O5i0.841.832.649 (11)163
O2—H2···O1ii0.842.142.846 (11)142
O2—H2···O2ii0.842.352.989 (11)133
O4—H4···O50.841.792.626 (10)170
O6—H6···O7iii0.841.792.626 (10)170
C3—H3···O1iv0.952.543.220 (13)129
C10—H10···O30.952.352.682 (11)100
C16—H16C···O4iii0.982.443.293 (15)145
C17—H17A···O7v0.982.393.308 (18)156
Symmetry codes: (i) x+1, y1, z; (ii) x+3, y+1/2, z+2; (iii) x, y1/2, z+1; (iv) x1, y+1, z; (v) x, y+1/2, z+1.
 

Funding information

The author is grateful for the financial support of this work by the National Natural Science Foundation of China (No. 82404543), the Universities Natural Science Foundation of Jiangsu Province (No. 24KJB350002), and the Basic Research Foundation of Yancheng City (No. YCBK202220).

References

Return to citationBruker (2019). APEX5 and SAINT. Bruker AXS Inc. Madison, Wisconsin, USA.  Google Scholar
 Return to citationCox, P. J., Kumarasamy, Y., Nahar, L., Sarker, S. D. & Shoeb, M. (2003). Acta Cryst. E59, o975–o977.  Web of Science CSD CrossRef IUCr Journals Google Scholar
 Return to citationDolomanov, O. V., Bourhis, L. J., Gildea, R. J., Howard, J. A. K. & Puschmann, H. (2009). J. Appl. Cryst. 42, 339–341.  Web of Science CrossRef CAS IUCr Journals Google Scholar
 Return to citationGroom, C. R., Bruno, I. J., Lightfoot, M. P. & Ward, S. C. (2016). Acta Cryst. B72, 171–179.  Web of Science CrossRef IUCr Journals Google Scholar
 Return to citationHe, H., Huang, Y., Zhang, Q., Wang, J.-R. & Mei, X. (2016). Cryst. Growth Des. 16, 2348–2356.  Web of Science CSD CrossRef CAS Google Scholar
 Return to citationJiang, L., Huang, Y., Zhang, Q., He, H., Xu, Y. & Mei, X. (2014). Cryst. Growth Des. 14, 4562–4573.  Web of Science CSD CrossRef CAS Google Scholar
 Return to citationKrause, L., Herbst-Irmer, R., Sheldrick, G. M. & Stalke, D. (2015). J. Appl. Cryst. 48, 3–10.  Web of Science CSD CrossRef ICSD CAS IUCr Journals Google Scholar
 Return to citationMahwish, Imran, M., Naeem, H., Hussain, M., Alsagaby, S. A., Al Abdulmonem, W., Mujtaba, A., Abdelgawad, M. A., Ghoneim, M. M., El–Ghorab, A. H., Selim, S., Al Jaouni, S. K., Mostafa, E. M. & Yehuala, T. F. (2025). Food. Sci. & Nutr. 13, e4682.  Google Scholar
 Return to citationPandey, P., Lakhanpal, S., Mahmood, D., Kang, H. N., Kim, B., Kang, S., Choi, J., Choi, M., Pandey, S., Bhat, M., Sharma, S., Khan, F., Park, M. N. & Kim, B. (2025). Front. Pharmacol. 15, 1513422.  CrossRef PubMed Google Scholar
 Return to citationParsons, S., Flack, H. D. & Wagner, T. (2013). Acta Cryst. B69, 249–259.  Web of Science CSD CrossRef CAS IUCr Journals Google Scholar
 Return to citationPennington, W. T. (1999). J. Appl. Cryst. 32, 1028–1029.  Web of Science CrossRef CAS IUCr Journals Google Scholar
 Return to citationPrasher, P., Sharma, M., Singh, S. K., Gulati, M., Chellappan, D. K., Zacconi, F., De Rubis, G., Gupta, G., Sharifi-Rad, J., Cho, W. C. & Dua, K. (2022). Cancer Cell Int. 22, 386.  CrossRef PubMed Google Scholar
 Return to citationSheldrick, G. M. (2015a). Acta Cryst. A71, 3–8.  Web of Science CrossRef IUCr Journals Google Scholar
 Return to citationSheldrick, G. M. (2015b). Acta Cryst. C71, 3–8.  Web of Science CrossRef IUCr Journals Google Scholar
 Return to citationSowa, M., Ślepokura, K. & Matczak-Jon, E. (2013). CrystEngComm 15, 7696–7708.  CSD CrossRef CAS Google Scholar
 Return to citationSpackman, M. A. & Jayatilaka, D. (2009). CrystEngComm 11, 19–32.  Web of Science CrossRef CAS Google Scholar
 Return to citationSpackman, M. A. & McKinnon, J. J. (2002). CrystEngComm 4, 378–392.  Web of Science CrossRef CAS Google Scholar
 Return to citationSpackman, P. R., Turner, M. J., McKinnon, J. J., Wolff, S. K., Grimwood, D. J., Jayatilaka, D. & Spackman, M. A. (2021). J. Appl. Cryst. 54, 1006–1011.  Web of Science CrossRef CAS IUCr Journals Google Scholar
 Return to citationSpek, A. L. (2020). Acta Cryst. E76, 1–11.  Web of Science CrossRef IUCr Journals Google Scholar
 Return to citationZhang, J. & Ma, Y. (2024). Biomed. Pharmacother. 176, 116909.  CrossRef PubMed Google Scholar
 Return to citationZhu, M., Sun, Y., Su, Y., Guan, W., Wang, Y., Han, J., Wang, S., Yang, B., Wang, Q. & Kuang, H. (2024). Phytother. Res. 38, 3417–3443.  CrossRef PubMed Google Scholar

This is an open-access article distributed under the terms of the Creative Commons Attribution (CC-BY) Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original authors and source are cited.

Journal logoCRYSTALLOGRAPHIC
COMMUNICATIONS
ISSN: 2056-9890
Volume 82| Part 4| April 2026| Pages 375-378
https://doi.org/10.1107/S2056989026002720
Follow Acta Cryst. E
Sign up for e-alerts
E-alerts
Follow Acta Cryst. on Twitter
Twitter
Follow us on facebook
Facebook
Sign up for RSS feeds
RSS