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

Journal logoCRYSTALLOGRAPHIC
COMMUNICATIONS
ISSN: 2056-9890
Volume 82| Part 6| June 2026| Pages 751-754
https://doi.org/10.1107/S2056989026004895

Crystal structure of (3R,5aS,6R,9R,12R,12aR)-3,6,9-tri­methyl­deca­hydro-12H-3,12-ep­­oxy[1,2]dioxepino[4,3-i]isochromen-10-yl 5-((3aS,4S,6aR)-2-oxohexa­hydro-1H-thieno[3,4-d]imidazol-4-yl)penta­noate

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Xiaomei Yang,a Siyu Chen,b Wenxin Liu,a Mengjie Cuia and Qingjie Zhaoa*

aInnovation Research Institute of Traditional Chinese Medicine, Shanghai University of Traditional Chinese Medicine, Shanghai 201203, People's Republic of China, and bCollege of Life Sciences, Shanghai Normal University, Shanghai 201418, People's Republic of China
*Correspondence e-mail: [email protected]

Edited by W. T. A. Harrison, University of Aberdeen, United Kingdom (Received 22 April 2026; accepted 11 May 2026; online 29 May 2026)

In the title biotin-conjugated di­hydro­artemisinin (DHA) derivative, C25H38N2O7S, the mol­ecule retains the essential endoperoxide bridge and links the C-10 position of DHA to the penta­noate chain of biotin via an ester bond. In the solid state, the tetra­hydro­pyran ring of DHA adopts a chair conformation, the fused peroxide seven-membered ring exhibits a twist conformation, the imidazolidone ring of biotin shows an envelope conformation and the tetra­hydro­thio­phene ring adopts a twisted conformation. Supra­molecularly, adjacent mol­ecules are linked through a classical N—H⋯O double hydrogen-bonding motif between the urea groups of biotin, forming anti­parallel cyclic dimers. These strong dimers are further supported by weaker C—H⋯O inter­actions. The SQUEEZE [Spek (2015View full citation). Acta Cryst. C71, 9-18] routine in PLATON was used to remove electron density corresponding to disordered solvent mol­ecules. This structure determination provides a valuable blueprint for the rational design of hybrid anti­malarial and anti­cancer therapies based on DHA–biotin conjugates.

CCDC reference: 2553196

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1. Chemical context

Artemisinin (C15H22O5; ART), isolated from Artemisia annua, and its active metabolite di­hydro­artemisinin (C15H24O5; DHA) are cornerstone anti­malarial agents, particularly effective against drug-resistant Plasmodium falciparum strains. Their pharmacological significance extends to oncology, where DHA exhibits potent anti­tumor activity across various cancers, including breast, lung, and melanoma, by inhibiting angiogenesis, inducing apoptosis, and promoting ferroptosis through iron-dependent reactive oxygen species (ROS) generation. The endoperoxide bridge in ART and DHA is crucial for cytotoxicity. In the presence of ferrous iron, this moiety undergoes homolytic cleavage, yielding carbon-centered radicals that alkyl­ate biomacromolecules and trigger oxidative stress, leading to parasite and cancer cell death. Derivatives lacking this bridge, such as de­oxy­artemisinin, show markedly reduced potency, underscoring its essential role.

Conjugating DHA with biotin – a vitamin overexpressed on tumor cells via specific transporters – offers significant biological advantages. Biotinylation enhances tumor targeting, improves cellular uptake, and enables avidin-mediated delivery systems, boosting efficacy while minimizing off-target effects, as demonstrated in biotin-ART micelle formulations that reduced tumor volumes in breast cancer models.

[Scheme 1]

As part of our studies in this area, we now report the synthesis and single-crystal structure of the title biotin-conjugated DHA derivative, C26H40N2O6S (I). This polycyclic scaffold preserves the peroxide bridge while linking DHA's C-10 atom to biotin's penta­noate chain, potentially optimizing pharmacokinetics and selectivity.

2. Structural commentary

The crystal of (I) belongs to the monoclinic system, space group P21, with Z = 2, containing one complete mol­ecule in the asymmetric unit (Fig. 1[link]). Mol­ecule (I) consists of a di­hydro­artemisinin (DHA) core linked to a biotin side chain through an ester bond. The DHA moiety retains its natural absolute configuration of (3R, 5aS, 6R, 9R, 12R, 12aR), while the biotin moiety adopts a (3aS, 4S, 6aR) configuration. Key bond lengths are as follows: the per­oxy bridge O1—O2 separation is 1.462 (4) Å, the ester C10—O5 bond is 1.416 (4) Å, and the carbonyl C16=O6 bond is 1.206 (5) Å, all within normal ranges. The crucial O5—C10—O4 bond angle measures 104.3 (3)°. Four representative torsion angles are C1—O1—O2—C12 = 46.5 (4), C8—C9—C10—O5 = 178.5 (3), C11—O4—C10—O5 = 1778.0 (3) and C15—C9—C10—O5 = −56.8 (5)°. The tetra­hydro­pyran (C4–C8/C12) ring in the DHA core adopts a stable chair conformation, while the fused peroxide and seven-membered ring (C1–C4/C12/C11/O3) exhibits a twist conformation. The imidazolidone ring in the biotin unit (N1/C24/C23/N2/C25) displays an envelope conformation, and the tetra­hydro­thio­phene ring (S1/C21/C24/C23/C22) shows a twisted conformation. The overall stereochemistry of the mol­ecule agrees with the expected configuration, and formation of the ester linkage does not introduce any significant conformational distortion.

[Figure 1]
Figure 1
The mol­ecular structure of (I) showing 50% probability ellipsoids.

3. Supra­molecular features

The extended structure of (I) (Fig. 2[link]) exhibits a well-defined hydrogen-bonded network dominated by strong N—H⋯O inter­actions between the urea groups of the biotin moieties. These classical amide–urea dimers adopt the characteristic DADA double hydrogen-bond motif (Table 1[link]), a supra­molecular feature commonly observed in biotin and its derivatives: the N1—H1⋯O7 and N2—H2⋯O7 bonds together link adjacent mol­ecules through a pair of nearly linear N—H⋯O hydrogen bonds to generate cyclic dimeric units. Each dimer is stabilized by the anti­parallel orientation of the biotin urea fragments, resulting in a robust ring-like supra­molecular motif.

Table 1
Hydrogen-bond geometry (Å, °)

D—H⋯A D—H H⋯A DA D—H⋯A
N1—H1⋯O7i 0.88 2.16 3.004 (4) 162
N2—H2⋯O7ii 0.88 2.07 2.886 (5) 154
C13—H13A⋯O7iii 0.98 2.63 3.438 (6) 140
C17—H17A⋯O2iv 0.99 2.44 3.431 (5) 178
C24—H24⋯O3v 1.00 2.44 3.204 (5) 133
Symmetry codes: (i) Mathematical equation; (ii) Mathematical equation; (iii) Mathematical equation; (iv) Mathematical equation; (v) Mathematical equation.
[Figure 2]
Figure 2
The packing of (I) viewed along the b-axis direction. Dashed lines indicate C—H⋯O and N—H⋯O hydrogen bonds between adjacent mol­ecules, illustrating the hydrogen-bonded three-dimensional supra­molecular assembly network and the unit-cell arrangement.

In addition to these dominant inter­actions, several weaker C—H⋯O hydrogen bonds further consolidate the crystal packing and help maintain the conformation of the di­hydro­artemisinin (DHA) unit and its ester side chain. Notably, a C13—H13A⋯O7 contact connects a methyl group of the DHA moiety with the carbonyl oxygen atom of the biotin fragment. A nearly linear (178°) C17—H17A⋯O2 inter­action links the methyl­ene group of the linker region to a peroxide oxygen atom within the DHA core, while C24—H24⋯O3 connects the tetra­hydro­thio­phene ring of biotin to an ether oxygen atom of the DHA framework.

These N—H⋯O and C—H⋯O inter­actions inter­link the mol­ecules along the crystallographic b-axis through the 21 screw axis, giving rise to a three-dimensional supra­molecular network. Overall, the supra­molecular architecture is primarily governed by the strong dimeric hydrogen bonds between urea groups, complemented by auxiliary C—H⋯O contacts that anchor the flexible DHA skeleton within the lattice while preserving the classical self-recognition mode characteristic of biotin-based systems.

4. Database survey

A search of the Cambridge Structural Database (CSD) via the WebCSD inter­face (CSD version 2025.1, May 2025 release; Groom et al., 2016View full citation) for artemisinin-related structures returned 23 hits, predominantly consisting of artemisinin, di­hydro­artemisinin (DHA), artemether, artesunate and their derivatives. Key entries include the parent artemisinin structure with CSD refcode QINGHA (Liu et al., 1979View full citation; Qinghaosu Research Group, 1980View full citation), which confirmed the absolute configuration and endoperoxide bridge essential for anti­malarial activity. The α/β-di­hydro­artemisinin ether dimer YIGGEC (Yue et al., 2006View full citation) and the 7β-hy­droxy­artemisinin derivative GEMBET (Carvalho et al., 2008View full citation) represent metabolically modified analogs generated via microbial transformation. Other notable entries comprise a multicomponent crystal of artesunate with urea aceto­nitrile solvate (CCDC 1590278; Jiang et al., 2020View full citation), illustrating the use of cinchona alkaloids to form multicomponent crystals with artesunate. A trioxane azido derivative LALBON (Xie et al., 2010View full citation) retains the endoperoxide and exhibits weak C—H⋯N/O inter­actions in the solid state. The ferrous bromide rearrangement product of a 5β-hy­droxy-D-secoartemisinin analog (LALBOT; Jahan et al., 2021View full citation) and the corresponding Mosher ester derivative (CCDC 2006194; Jahan et al., 2021View full citation) provide insight into iron-mediated degradation pathways relevant to the mechanism of action. A search for biotin-related small mol­ecules gave 19 hits, including d-biotin (BIOTIN; DeTitta et al., 1976View full citation), de­thio­biotin (DETHIO10; DeTitta & Edmonds, 1980View full citation) and various biotin ester derivatives (e.g., BIWYEA; Blauż et al., 2016View full citation). A substructure search for a covalent conjugate featuring both an artemisinin-derived endoperoxide moiety and a biotin-derived ureido­tetra­hydro­thieno[3,4-d]imidazole scaffold linked via an ester bond, however, returned zero hits. This finding establishes the structural novelty of the present DHA–biotin ester conjugate, whose single-crystal X-ray analysis confirms the retention of the endoperoxide bridge [O1—O2 = 1.462 (4) Å] and the classical N—H⋯O dimeric hydrogen-bonding motif between biotin urea groups, as previously observed in avidin–biotin recognition (Livnah et al., 1993View full citation) and in ferrocene–biotin conjugates (Blauż et al., 2016View full citation).

5. Synthesis and crystallization

To a solution of biotin (1.0 equiv) and di­hydro­artemisinin (1.1 equiv) in anhydrous di­methyl­formamide (DMF; 2 ml) were added 1-ethyl-3-(3-di­methyl­amino­prop­yl)carbodi­imide (EDC) (3.0 equiv) and 4-di­methyl­amino­pyridine (DMAP) (1.0 equiv) (Fig. 3[link]) at room temperature under nitro­gen atmosphere. The reaction proceeded smoothly for 2 h to afford the title compound in a yield of 78% (Fig. 3[link]).

[Figure 3]
Figure 3
Reaction scheme for obtaining the title compound.

The compound with a purity of over 98% was dissolved in petroleum ether, then left to stand while the solvent was allowed to evaporate gradually under controlled conditions to form colorless needles of (I).

6. Refinement

Crystal data, data collection and structure refinement details are summarized in Table 2[link]. There were severely disordered solvent mol­ecules (likely petroleum ether or DMF) in the structure that could not be modeled effectively. Therefore, the SQUEEZE routine (Spek, 2015View full citation) in PLATON was used to remove the corresponding electron density. The calculated mol­ecular weight and density do not include the contribution of these squeezed solvents.

Table 2
Experimental details

Crystal data
Chemical formula C25H38N2O7S
Mr 510.63
Crystal system, space group Monoclinic, P21
Temperature (K) 150
a, b, c (Å) 12.8909 (8), 7.5857 (4), 14.9027 (9)
β (°) 103.924 (4)
V3) 1414.46 (15)
Z 2
Radiation type Cu Kα
μ (mm−1) 1.37
Crystal size (mm) 0.08 × 0.03 × 0.01
 
Data collection
Diffractometer Bruker D8 VENTURE DUO PHOTON III
Absorption correction Multi-scan (SADABS; Krause et al., 2015View full citation)
Tmin, Tmax 0.90, 0.99
No. of measured, independent and observed [I > 2σ(I)] reflections 16792, 4678, 3874
Rint 0.059
(sin θ/λ)max−1) 0.597
 
Refinement
R[F2 > 2σ(F2)], wR(F2), S 0.044, 0.123, 1.02
No. of reflections 4678
No. of parameters 320
No. of restraints 1
H-atom treatment H-atom parameters constrained
Δρmax, Δρmin (e Å−3) 0.25, −0.23
Absolute structure Flack x determined using 1374 quotients [(I+)−(I)]/[(I+)+(I)] (Parsons et al., 2013View full citation)
Absolute structure parameter 0.034 (14)
Computer programs: APEX4 and SAINT (Bruker, 2021View full citation), SHELXT2018/2 (Sheldrick, 2015aView full citation), SHELXL2018/3 (Sheldrick, 2015bView full citation) and OLEX2 (Dolomanov et al., 2009View full citation).

Supporting information

CCDC reference: 2553196

Crystal structure: contains datablocks global, I. DOI: https://doi.org/10.1107/S2056989026004895/hb8220sup1.cif

Structure factors: contains datablock I. DOI: https://doi.org/10.1107/S2056989026004895/hb8220Isup2.hkl

checkCIF report


Computing details top

(3R,5aS,6R,9R,12R,12aR)-3,6,9-Trimethyldecahydro-12H-3,12-epoxy[1,2]dioxepino[4,3-i]isochromen-10-yl 5-((3aS,4S,6aR)-2-oxohexahydro-1H-thieno[3,4-d]imidazol-4-yl)pentanoate top
Crystal data top
C25H38N2O7SF(000) = 548
Mr = 510.63Dx = 1.199 Mg m3
Monoclinic, P21Cu Kα radiation, λ = 1.54178 Å
a = 12.8909 (8) ÅCell parameters from 4632 reflections
b = 7.5857 (4) Åθ = 3.1–66.7°
c = 14.9027 (9) ŵ = 1.37 mm1
β = 103.924 (4)°T = 150 K
V = 1414.46 (15) Å3Needle, colorless
Z = 20.08 × 0.03 × 0.01 mm
Data collection top
Bruker D8 VENTURE DUO PHOTON III
diffractometer		3874 reflections with I > 2σ(I)
ω scansRint = 0.059
Absorption correction: multi-scan
(SADABS; Krause et al., 2015)		θmax = 66.9°, θmin = 3.1°
Tmin = 0.90, Tmax = 0.99h = 1515
16792 measured reflectionsk = 79
4678 independent reflectionsl = 1717
Refinement top
Refinement on F2H-atom parameters constrained
Least-squares matrix: full w = 1/[σ2(Fo2) + (0.0757P)2]
where P = (Fo2 + 2Fc2)/3
R[F2 > 2σ(F2)] = 0.044(Δ/σ)max = 0.005
wR(F2) = 0.123Δρmax = 0.25 e Å3
S = 1.02Δρmin = 0.23 e Å3
4678 reflectionsExtinction correction: SHELXL-2018/3 (Sheldrick 2015b), Fc*=kFc[1+0.001xFc2λ3/sin(2θ)]-1/4
320 parametersExtinction coefficient: 0.0052 (9)
1 restraintAbsolute structure: Flack x determined using 1374 quotients [(I+)-(I-)]/[(I+)+(I-)] (Parsons et al., 2013)
Hydrogen site location: inferred from neighbouring sitesAbsolute structure parameter: 0.034 (14)
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
S10.20915 (8)0.91961 (15)0.81646 (8)0.0505 (3)
O10.3657 (2)0.0313 (4)0.2718 (2)0.0458 (7)
O20.44866 (19)0.0792 (4)0.24888 (19)0.0404 (6)
O30.2270 (2)0.1621 (4)0.2161 (2)0.0456 (7)
O40.3154 (2)0.2950 (4)0.34723 (19)0.0462 (7)
O50.3909 (2)0.4090 (4)0.48693 (18)0.0468 (7)
O60.2471 (3)0.5877 (5)0.4587 (2)0.0628 (9)
O70.0070 (2)0.9020 (4)1.02806 (17)0.0454 (6)
N10.0146 (3)0.7662 (4)0.8946 (2)0.0361 (7)
H10.0276710.6587620.9166970.043*
N20.0131 (3)1.0527 (5)0.8929 (2)0.0489 (9)
H20.0291461.1568960.9117580.059*
C10.2702 (3)0.0056 (6)0.2019 (3)0.0472 (10)
C20.2875 (4)0.0182 (6)0.1046 (3)0.0568 (12)
H2A0.2247010.0764230.0641250.068*
H2B0.3506400.0936090.1061400.068*
C30.3047 (4)0.1613 (7)0.0624 (3)0.0530 (11)
H3A0.3169220.1407430.0000950.064*
H3B0.2381350.2308650.0543500.064*
C40.3979 (3)0.2722 (6)0.1184 (3)0.0440 (10)
H40.4646040.2205330.1062010.053*
C50.3932 (3)0.4658 (6)0.0846 (3)0.0487 (11)
H50.3280700.5218260.0973740.058*
C60.4891 (4)0.5656 (7)0.1371 (3)0.0568 (12)
H6A0.4844680.6891240.1150310.068*
H6B0.5544090.5127100.1246600.068*
C70.4980 (4)0.5642 (6)0.2411 (3)0.0520 (11)
H7A0.4359230.6270830.2541810.062*
H7B0.5635450.6278810.2729310.062*
C80.5017 (3)0.3759 (5)0.2794 (3)0.0416 (9)
H80.5701050.3222680.2723090.050*
C90.5033 (3)0.3668 (5)0.3833 (3)0.0428 (9)
H90.5156950.2414110.4037530.051*
C100.3938 (3)0.4198 (6)0.3927 (2)0.0425 (8)
H100.3753360.5413690.3680370.051*
C110.3043 (3)0.2912 (6)0.2501 (3)0.0386 (8)
H110.2755350.4077660.2241630.046*
C120.4096 (3)0.2584 (5)0.2232 (3)0.0375 (9)
C130.1948 (4)0.1446 (7)0.2248 (4)0.0644 (14)
H13A0.1208700.1136830.1945820.097*
H13B0.2032150.1492630.2918710.097*
H13C0.2120730.2600220.2026220.097*
C140.3851 (4)0.4786 (8)0.0199 (3)0.0702 (15)
H14A0.3868120.6027620.0376770.105*
H14B0.3178800.4250940.0539130.105*
H14C0.4453600.4160900.0347980.105*
C150.5923 (4)0.4794 (7)0.4432 (3)0.0559 (11)
H15A0.5976800.4538810.5086210.084*
H15B0.5756890.6045240.4311670.084*
H15C0.6603790.4517580.4280800.084*
C160.3104 (3)0.4963 (6)0.5113 (3)0.0464 (10)
C170.3106 (3)0.4587 (6)0.6095 (3)0.0458 (10)
H17A0.3804000.4954700.6490240.055*
H17B0.3041320.3297800.6167970.055*
C180.2231 (3)0.5482 (6)0.6440 (3)0.0451 (10)
H18A0.1528210.5010300.6105200.054*
H18B0.2239510.6762730.6314810.054*
C190.2379 (3)0.5181 (6)0.7478 (3)0.0429 (9)
H19A0.3003970.5869480.7816850.052*
H19B0.2533490.3918700.7616970.052*
C200.1395 (3)0.5716 (5)0.7824 (3)0.0401 (9)
H20A0.0788930.4949970.7524090.048*
H20B0.1546770.5501050.8497980.048*
C210.1064 (3)0.7618 (5)0.7639 (3)0.0390 (9)
H210.0893650.7805230.6954820.047*
C220.1103 (4)1.0931 (6)0.7889 (4)0.0540 (12)
H22A0.1327341.1953110.8303390.065*
H22B0.1022921.1326180.7242640.065*
C230.0041 (4)1.0191 (6)0.8017 (3)0.0444 (10)
H230.0569771.0654230.7527000.053*
C240.0082 (3)0.8141 (5)0.7977 (3)0.0369 (9)
H240.0583460.7658820.7559390.044*
C250.0017 (3)0.9048 (5)0.9458 (3)0.0370 (8)
Atomic displacement parameters (Å2) top
U11U22U33U12U13U23
S10.0525 (5)0.0362 (6)0.0686 (7)0.0132 (5)0.0258 (5)0.0079 (5)
O10.0413 (13)0.0288 (16)0.0662 (17)0.0034 (11)0.0108 (12)0.0005 (13)
O20.0362 (13)0.0272 (14)0.0578 (16)0.0016 (11)0.0111 (11)0.0007 (12)
O30.0378 (14)0.0413 (17)0.0604 (18)0.0028 (12)0.0173 (12)0.0038 (14)
O40.0519 (15)0.0422 (17)0.0504 (16)0.0006 (13)0.0237 (12)0.0025 (13)
O50.0582 (15)0.0404 (16)0.0465 (14)0.0076 (14)0.0217 (12)0.0016 (14)
O60.082 (2)0.060 (2)0.0547 (18)0.0288 (19)0.0323 (16)0.0079 (17)
O70.0724 (17)0.0240 (14)0.0471 (15)0.0008 (13)0.0285 (12)0.0000 (13)
N10.0512 (18)0.0223 (17)0.0400 (18)0.0007 (13)0.0209 (14)0.0019 (13)
N20.084 (3)0.0252 (19)0.046 (2)0.0104 (17)0.0325 (18)0.0021 (15)
C10.041 (2)0.034 (2)0.065 (3)0.0002 (17)0.0097 (18)0.004 (2)
C20.061 (3)0.047 (3)0.060 (3)0.003 (2)0.010 (2)0.019 (2)
C30.055 (3)0.056 (3)0.048 (3)0.006 (2)0.011 (2)0.008 (2)
C40.048 (2)0.046 (3)0.041 (2)0.0097 (18)0.0172 (17)0.0022 (19)
C50.053 (2)0.049 (3)0.049 (2)0.010 (2)0.0221 (18)0.009 (2)
C60.059 (3)0.046 (3)0.073 (3)0.005 (2)0.030 (2)0.019 (2)
C70.061 (3)0.037 (3)0.060 (3)0.007 (2)0.019 (2)0.001 (2)
C80.043 (2)0.034 (2)0.049 (2)0.0002 (16)0.0148 (16)0.0025 (18)
C90.049 (2)0.030 (2)0.050 (2)0.0015 (16)0.0136 (17)0.0067 (17)
C100.057 (2)0.034 (2)0.0408 (19)0.002 (2)0.0212 (16)0.0039 (19)
C110.0414 (19)0.033 (2)0.044 (2)0.0050 (16)0.0163 (16)0.0003 (17)
C120.043 (2)0.028 (2)0.044 (2)0.0053 (15)0.0142 (16)0.0028 (16)
C130.053 (3)0.045 (3)0.091 (4)0.010 (2)0.010 (2)0.001 (3)
C140.085 (3)0.076 (4)0.056 (3)0.014 (3)0.030 (2)0.024 (3)
C150.060 (2)0.053 (3)0.056 (2)0.008 (2)0.016 (2)0.013 (2)
C160.056 (2)0.038 (2)0.051 (2)0.012 (2)0.0242 (19)0.004 (2)
C170.054 (2)0.041 (3)0.045 (2)0.0073 (19)0.0180 (17)0.0006 (19)
C180.055 (2)0.041 (2)0.044 (2)0.0058 (19)0.0212 (18)0.0022 (19)
C190.053 (2)0.034 (2)0.047 (2)0.0064 (17)0.0240 (17)0.0061 (18)
C200.051 (2)0.028 (2)0.048 (2)0.0020 (17)0.0229 (17)0.0004 (17)
C210.047 (2)0.027 (2)0.048 (2)0.0009 (16)0.0225 (17)0.0023 (17)
C220.083 (3)0.025 (2)0.066 (3)0.001 (2)0.040 (2)0.000 (2)
C230.065 (3)0.035 (2)0.040 (2)0.0116 (19)0.0246 (19)0.0032 (18)
C240.043 (2)0.032 (2)0.040 (2)0.0000 (16)0.0181 (17)0.0012 (17)
C250.0449 (18)0.024 (2)0.046 (2)0.0011 (16)0.0177 (15)0.0004 (18)
Geometric parameters (Å, º) top
S1—C211.817 (4)C8—H81.0000
S1—C221.809 (5)C8—C91.545 (6)
O1—O21.462 (4)C8—C121.558 (5)
O1—C11.422 (5)C9—H91.0000
O2—C121.468 (5)C9—C101.506 (5)
O3—C11.425 (5)C9—C151.533 (6)
O3—C111.402 (5)C10—H101.0000
O4—C101.431 (5)C11—H111.0000
O4—C111.420 (5)C11—C121.525 (5)
O5—C101.416 (4)C13—H13A0.9800
O5—C161.351 (5)C13—H13B0.9800
O6—C161.206 (5)C13—H13C0.9800
O7—C251.245 (4)C14—H14A0.9800
N1—H10.8800C14—H14B0.9800
N1—C241.473 (5)C14—H14C0.9800
N1—C251.344 (5)C15—H15A0.9800
N2—H20.8800C15—H15B0.9800
N2—C231.452 (5)C15—H15C0.9800
N2—C251.358 (5)C16—C171.490 (6)
C1—C21.522 (6)C17—H17A0.9900
C1—C131.527 (6)C17—H17B0.9900
C2—H2A0.9900C17—C181.509 (5)
C2—H2B0.9900C18—H18A0.9900
C2—C31.538 (7)C18—H18B0.9900
C3—H3A0.9900C18—C191.529 (5)
C3—H3B0.9900C19—H19A0.9900
C3—C41.538 (6)C19—H19B0.9900
C4—H41.0000C19—C201.534 (5)
C4—C51.549 (7)C20—H20A0.9900
C4—C121.537 (5)C20—H20B0.9900
C5—H51.0000C20—C211.511 (6)
C5—C61.499 (7)C21—H211.0000
C5—C141.539 (6)C21—C241.522 (5)
C6—H6A0.9900C22—H22A0.9900
C6—H6B0.9900C22—H22B0.9900
C6—C71.526 (6)C22—C231.533 (7)
C7—H7A0.9900C23—H231.0000
C7—H7B0.9900C23—C241.558 (5)
C7—C81.535 (6)C24—H241.0000
C22—S1—C2188.9 (2)O2—C12—C4105.7 (3)
C1—O1—O2107.6 (3)O2—C12—C8102.7 (3)
O1—O2—C12111.5 (2)O2—C12—C11110.7 (3)
C11—O3—C1114.1 (3)C4—C12—C8112.5 (3)
C11—O4—C10112.5 (3)C11—C12—C4112.4 (3)
C16—O5—C10116.3 (3)C11—C12—C8112.1 (3)
C24—N1—H1123.7C1—C13—H13A109.5
C25—N1—H1123.7C1—C13—H13B109.5
C25—N1—C24112.6 (3)C1—C13—H13C109.5
C23—N2—H2123.9H13A—C13—H13B109.5
C25—N2—H2123.9H13A—C13—H13C109.5
C25—N2—C23112.2 (3)H13B—C13—H13C109.5
O1—C1—O3108.3 (3)C5—C14—H14A109.5
O1—C1—C2113.0 (3)C5—C14—H14B109.5
O1—C1—C13103.1 (4)C5—C14—H14C109.5
O3—C1—C2110.5 (4)H14A—C14—H14B109.5
O3—C1—C13106.9 (4)H14A—C14—H14C109.5
C2—C1—C13114.6 (4)H14B—C14—H14C109.5
C1—C2—H2A108.8C9—C15—H15A109.5
C1—C2—H2B108.8C9—C15—H15B109.5
C1—C2—C3113.8 (4)C9—C15—H15C109.5
H2A—C2—H2B107.7H15A—C15—H15B109.5
C3—C2—H2A108.8H15A—C15—H15C109.5
C3—C2—H2B108.8H15B—C15—H15C109.5
C2—C3—H3A108.4O5—C16—C17110.5 (3)
C2—C3—H3B108.4O6—C16—O5123.4 (4)
H3A—C3—H3B107.4O6—C16—C17126.1 (4)
C4—C3—C2115.6 (4)C16—C17—H17A108.5
C4—C3—H3A108.4C16—C17—H17B108.5
C4—C3—H3B108.4C16—C17—C18115.1 (3)
C3—C4—H4106.3H17A—C17—H17B107.5
C3—C4—C5112.2 (3)C18—C17—H17A108.5
C5—C4—H4106.3C18—C17—H17B108.5
C12—C4—C3112.8 (4)C17—C18—H18A109.5
C12—C4—H4106.3C17—C18—H18B109.5
C12—C4—C5112.5 (3)C17—C18—C19110.9 (3)
C4—C5—H5108.1H18A—C18—H18B108.1
C6—C5—C4110.3 (3)C19—C18—H18A109.5
C6—C5—H5108.1C19—C18—H18B109.5
C6—C5—C14110.1 (4)C18—C19—H19A109.0
C14—C5—C4112.1 (4)C18—C19—H19B109.0
C14—C5—H5108.1C18—C19—C20112.8 (3)
C5—C6—H6A109.2H19A—C19—H19B107.8
C5—C6—H6B109.2C20—C19—H19A109.0
C5—C6—C7112.2 (3)C20—C19—H19B109.0
H6A—C6—H6B107.9C19—C20—H20A108.7
C7—C6—H6A109.2C19—C20—H20B108.7
C7—C6—H6B109.2H20A—C20—H20B107.6
C6—C7—H7A109.2C21—C20—C19114.3 (3)
C6—C7—H7B109.2C21—C20—H20A108.7
C6—C7—C8111.9 (4)C21—C20—H20B108.7
H7A—C7—H7B107.9S1—C21—H21107.7
C8—C7—H7A109.2C20—C21—S1113.9 (3)
C8—C7—H7B109.2C20—C21—H21107.7
C7—C8—H8106.8C20—C21—C24114.2 (3)
C7—C8—C9113.9 (3)C24—C21—S1105.3 (3)
C7—C8—C12112.4 (3)C24—C21—H21107.7
C9—C8—H8106.8S1—C22—H22A110.1
C9—C8—C12109.8 (3)S1—C22—H22B110.1
C12—C8—H8106.8H22A—C22—H22B108.5
C8—C9—H9108.1C23—C22—S1107.8 (3)
C10—C9—C8107.1 (3)C23—C22—H22A110.1
C10—C9—H9108.1C23—C22—H22B110.1
C10—C9—C15112.6 (3)N2—C23—C22113.2 (4)
C15—C9—C8112.7 (3)N2—C23—H23110.5
C15—C9—H9108.1N2—C23—C24103.0 (3)
O4—C10—C9110.5 (3)C22—C23—H23110.5
O4—C10—H10110.9C22—C23—C24108.7 (4)
O5—C10—O4104.3 (3)C24—C23—H23110.5
O5—C10—C9109.0 (3)N1—C24—C21113.9 (3)
O5—C10—H10110.9N1—C24—C23101.7 (3)
C9—C10—H10110.9N1—C24—H24110.9
O3—C11—O4105.7 (3)C21—C24—C23108.1 (3)
O3—C11—H11108.3C21—C24—H24110.9
O3—C11—C12113.0 (3)C23—C24—H24110.9
O4—C11—H11108.3O7—C25—N1126.7 (4)
O4—C11—C12113.1 (3)O7—C25—N2124.2 (4)
C12—C11—H11108.3N1—C25—N2109.1 (3)
S1—C21—C24—N174.8 (4)C8—C9—C10—O464.4 (4)
S1—C21—C24—C2337.4 (4)C8—C9—C10—O5178.5 (3)
S1—C22—C23—N293.4 (4)C9—C8—C12—O271.1 (4)
S1—C22—C23—C2420.5 (5)C9—C8—C12—C4175.7 (3)
O1—O2—C12—C4108.2 (3)C9—C8—C12—C1147.9 (4)
O1—O2—C12—C8133.7 (3)C10—O4—C11—O3179.0 (3)
O1—O2—C12—C1113.8 (4)C10—O4—C11—C1254.8 (4)
O1—C1—C2—C395.4 (4)C10—O5—C16—O64.2 (7)
O2—O1—C1—O374.8 (3)C10—O5—C16—C17174.2 (3)
O2—O1—C1—C247.9 (4)C11—O3—C1—O134.9 (4)
O2—O1—C1—C13172.2 (3)C11—O3—C1—C289.4 (4)
O3—C1—C2—C326.0 (5)C11—O3—C1—C13145.3 (4)
O3—C11—C12—O252.7 (4)C11—O4—C10—O5178.0 (3)
O3—C11—C12—C465.3 (4)C11—O4—C10—C964.9 (4)
O3—C11—C12—C8166.8 (3)C12—C4—C5—C655.2 (4)
O4—C11—C12—O267.4 (4)C12—C4—C5—C14178.2 (3)
O4—C11—C12—C4174.6 (3)C12—C8—C9—C1055.7 (4)
O4—C11—C12—C846.7 (4)C12—C8—C9—C15179.9 (3)
O5—C16—C17—C18179.4 (4)C13—C1—C2—C3146.9 (4)
O6—C16—C17—C181.0 (7)C14—C5—C6—C7177.3 (4)
N2—C23—C24—N111.1 (4)C15—C9—C10—O4171.1 (3)
N2—C23—C24—C21131.4 (3)C15—C9—C10—O557.0 (5)
C1—O1—O2—C1246.5 (4)C16—O5—C10—O479.5 (4)
C1—O3—C11—O497.3 (4)C16—O5—C10—C9162.5 (4)
C1—O3—C11—C1226.9 (5)C16—C17—C18—C19173.5 (4)
C1—C2—C3—C456.9 (5)C17—C18—C19—C20167.7 (4)
C2—C3—C4—C5166.2 (3)C18—C19—C20—C2157.8 (5)
C2—C3—C4—C1238.0 (5)C19—C20—C21—S159.4 (4)
C3—C4—C5—C6176.5 (3)C19—C20—C21—C24179.6 (3)
C3—C4—C5—C1453.4 (5)C20—C21—C24—N150.8 (5)
C3—C4—C12—O270.6 (4)C20—C21—C24—C23163.1 (4)
C3—C4—C12—C8178.1 (3)C21—S1—C22—C2336.8 (3)
C3—C4—C12—C1150.4 (5)C22—S1—C21—C20168.9 (3)
C4—C5—C6—C758.4 (5)C22—S1—C21—C2443.0 (3)
C5—C4—C12—O2161.4 (3)C22—C23—C24—N1109.3 (4)
C5—C4—C12—C850.0 (4)C22—C23—C24—C2110.9 (5)
C5—C4—C12—C1177.7 (4)C23—N2—C25—O7176.0 (4)
C5—C6—C7—C856.9 (5)C23—N2—C25—N14.6 (5)
C6—C7—C8—C9176.3 (3)C24—N1—C25—O7175.6 (3)
C6—C7—C8—C1250.6 (5)C24—N1—C25—N23.7 (4)
C7—C8—C9—C1071.4 (4)C25—N1—C24—C21125.6 (4)
C7—C8—C9—C1553.0 (5)C25—N1—C24—C239.5 (4)
C7—C8—C12—O2161.0 (3)C25—N2—C23—C22107.1 (4)
C7—C8—C12—C447.8 (4)C25—N2—C23—C2410.2 (5)
C7—C8—C12—C1180.0 (4)
Hydrogen-bond geometry (Å, º) top
D—H···AD—HH···AD···AD—H···A
N1—H1···O7i0.882.163.004 (4)162
N2—H2···O7ii0.882.072.886 (5)154
C13—H13A···O7iii0.982.633.438 (6)140
C17—H17A···O2iv0.992.443.431 (5)178
C24—H24···O3v1.002.443.204 (5)133
Symmetry codes: (i) x, y1/2, z+2; (ii) x, y+1/2, z+2; (iii) x, y1, z1; (iv) x+1, y+1/2, z+1; (v) x, y+1/2, z+1.
 

Acknowledgements

The authors are grateful to the Single Crystal Diffraction Facility of Shanghai University for providing the X-ray data. We also acknowledge the Cambridge Crystallographic Data Centre (CCDC) for access to the Cambridge Structural Database and related resources.

References

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Volume 82| Part 6| June 2026| Pages 751-754
https://doi.org/10.1107/S2056989026004895
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