Tyrosinase Inhibitors from the Stems of Streblus Ilicifolius.

Two new stilbene derivatives, named strebluses C and D, were isolated from the EtOAc-soluble fraction of the stems of Streblus ilicifolius (Moraceae). Its absolute configuration was elucidated based on NMR spectroscopic data interpretation and optical rotation calculation. Streblus C possesses strong tyrosinase inhibitory activity with an IC50 value of 0.01 μM. Docking studies of 1 and 2 with oxy-tyrosinase were carried out to analyze their interactions. The analysis of the docked poses confirmed that 1 showed better binding affinity for oxy-tyrosinase than that of 2.

1. Introduction

Tyrosinase (EC 1.14.18.1), which is a binuclear copper-containing monooxygenase, is a key enzyme in the oxidation of phenol to the corresponding o-quinone [1, 2]. It plays a main factor causing freckles, brown age spots, and melasma. Some commercial compounds, such as hydroquinone, arbutin, kojic acid, azelaic acid, l-ascorbic acid, ellagic acid, and tranexamic acid, were reported as the well-known tyrosinase inhibitors. These compounds have been used as skin whitening agents in cosmetic products, but they have certain drawbacks [3]. Thus, the finding of the new efficient and safe tyrosinase inhibitors is necessary for antihyperpigmentation product development.

Streblus ilicifolius (Vidal) Corner, which belongs to Moraceae family, was found and cultivated in Vietnam. Its barks have been traditionally used as an antipimple medicine. In a few published studies, some phenolic compounds have been reported in this plant [4-7]. In our continued studies on the screening of medicinal plants for tyrosinase inhibitory activity [8-12], it was found that a MeOH-soluble extract of the stems of Streblus ilicifolius showed a strong inhibitory effect, with an IC50 value of 0.63 μg·mL−1. Thus, our study on chemical constituents of the stems of S. ilicifolius was carried out, leading to the isolation of two undescribed stilbene derivatives, strebluses C (1) and D (2). Compound 1 showed a strong tyrosinase inhibitory activity with an IC50 value of 0.01 μM, which makes it 4400 times more potent than that of kojic acid (IC50, 44.6 μM). In addition, molecular docking studies of 1 and 2 with the oxy-form of the copper-bound Streptomyces castaneoglobisporus tyrosinase were performed.

2. Materials and Methods

2.1. General Experimental Procedures

Optical values were measured on a Shimadzu UV-1800 spectrophotometer (Shimadzu Pte., Ltd., Singapore). IR spectra were measured with a Shimadzu IR-408 infrared spectrometer (Shimadzu Pte., Ltd., Singapore). NMR spectra were acquired on a Bruker Avance III 500 spectrometer (Bruker BioSpin AG, Bangkok, Thailand). Chemical shifts are expressed as δ values. HRESIMS data were acquired on Bruker micrOTOF-QII mass spectrometer (Bruker Singapore Pte., Ltd., Singapore). Column chromatography was carried out using silica gel 60, 0.06–0.2 mm (Scharlau, Barcelona, Spain), and LiChroprep RP-18, 40−63 μm (Merck KGaA, Darmstadt, Germany). Kieselgel 60 F254 or RP-18 F254 plates for TLC were purchased from Merck (Merck KGaA, Darmstadt, Germany). Tyrosinase (EC 1.14.18.1) from mushroom (3933 U·mL−1) and l-dihydroxyphenylalanine (l-DOPA) were obtained from Sigma-Aldrich (Sigma-Aldrich Pte Ltd, Singapore). Other chemicals were of the highest grade available.

2.2. Plant Material

The stems of Streblus ilicifolius were collected at Hoai Nhon District, Binh Dinh Province, Vietnam, in October 2017. The plant was identified by Dr. rer. nat. Anh Tuan Dang-Le, Faculty of Biology and Biotechnology, University of Science, Ho Chi Minh City, Vietnam. A voucher sample (MCE0052) has been deposited at the Department of Medicinal Chemistry, Faculty of Chemistry, University of Science, Ho Chi Minh City, Vietnam.

2.2.1. Extraction and Isolation

The dried powdered stems of S. ilicifolius (7.0 kg) were exhaustively extracted in a Soxhlet extractor with n-hexane, EtOAc, and MeOH to yield n-hexane-(64.8 g), EtOAc-(117.2 g), and MeOH-(378.0 g) soluble fractions, respectively. The EtOAc-soluble fraction was chromatographed by silica gel column chromatography (15 × 150 cm) and eluted with MeOH–CHCl3 (v/v, 0 : 100 ⟶ 100 : 0) mixtures to afford 18 fractions (Fr.1−Fr.18). Fraction Fr.8 (0.8 g) was separated by silica gel column chromatography with MeOH–CHCl3 (v/v, 0 : 100 ⟶ 30 : 70) mixtures to obtain six subfractions (Fr.8.1−Fr.8.6). Subfraction Fr.8.1 (34.8 mg) was loaded onto a silica gel column and eluted with EtOAc−CHCl3 mixtures (v/v, 0 : 100 ⟶ 100 : 0) and then purified by preparative TLC with an EtOAc−CHCl3 mixture (v/v, 15 : 85) to afford compound 2 (2.0 mg). Fraction Fr.14 (19.6 g) was subjected to further silica gel column chromatography and was eluted with CHCl3–n-hexane (v/v, 0 : 100 ⟶ 100 : 0) mixtures to yield 11 subfractions (Fr.14.1−Fr.14.11). Subfraction Fr.14.2 (69.0 mg) was chromatographed over a silica gel column with CHCl3–n-hexane (v/v, 0 : 100 ⟶ 100 : 0) mixtures to obtain two subfractions (Fr.14.2.1 and Fr.14.2.2). Subfraction Fr.14.2.2 (28.1 mg) was again chromatographed with CHCl3–n-hexane (v/v, 0 : 100 ⟶ 100 : 0) mixtures to give four subfractions (Fr.14.2.2.1−Fr.14.2.2.4). Subfraction Fr.14.2.2.3 (8.5 mg) was purified by preparative TLC with EtOAc−n-hexane (v/v, 20 : 80) mixture to afford 1 (3.9 mg).

2.2.2. Streblus C (1)

Yellow, amorphous powder; 1H and 13C NMR (500 MHz, acetone-d6, see Table 1 and Figures S2–S7); HRESIMS m/z 393.1704 [M + Na]+ (Figure S8) (calcd for C22H26O5Na, 393.1678).

Table 1

1H (500 MHz) and 13C (125 MHz) NMR data (acetone-d6) for compounds 1 and 2.

Position	1		2
	δ C, type C	δ H (J, Hz)	δ C, type C	δ H (J, Hz)
1	116.3, C		122.0, C
2	158.3, C		158.0, C
3	103.6, CH	6.46, d (2.4)	98.3, CH	7.00, d (2.1)
4	160.8, C		158.9, C
5	108.9, CH	6.42, dd (8.5, 2.4)	114.3, CH	6.87, dd (8.5, 2.1)
6	129.6, CH	7.48, d (8.5)	123.4, CH	7.52, d (8.5)
1′	153.9, C		143.6, C
2′	125.0, CH	5.97, d (2.0)	118.7, CH	6.48, d (2.1)
3′	199.2, C=O		200.6, C=O
4′	82.8, C		79.6, C
5′	77.3, CH	4.48, dd (4.3, 1.6)	73.0, CH	4.27, dd (5.9, 2.7)
6′	27.4, CH2	3.19, dd (18.8, 1.6)2.82, ddd (18.8, 4.3, 2.0)	32.0, CH2	3.15, ddd (18.5, 5.9, 2.1)3.08, dd (18.5, 2.7)
α	132.3, CH	7.40, d (16.4)	110.7, CH	7.31, s
β	126.4, CH	7.01, d (16.4)	153.2, C
1″	33.0, CH2	2.54, dd (14.4, 8.0)2.39, dd (14.4, 7.2)	35.3, CH2	2.47, dd (14.9, 7.7)2.40, dd (14.9, 7.0)
2″	118.1, CH	5.18, brs	118.8, CH	5.22, brt (7.3)
3″	136.0, C		135.0, C
4″	26.0, CH3	1.68, s	26.1, CH3	1.67, s
5″	18.1, CH3	1.63, s	18.1, CH3	1.58, s
1‴	108.0, C
2‴	27.8, CH3	1.32, s
3‴	26.8, CH3	1.18, s
4-OH				8.88, s
4′-OH				4.18, s
5′-OH				3.83, s

2.2.3. Streblus D (2) (Figures S9–S15)

Yellow, amorphous powder; 1H and 13C NMR (500 MHz, acetone-d6, see Table 1 and Figures S8–S14); HRESIMS m/z 351.1224 [M + Na]+ (Figure S15) (calcd for C19H20O5Na, 351.1208).

2.3. Tyrosinase Inhibitory Assay

All pure compounds were dissolved in DMSO and tested at concentrations ranging from 0.01 to 100 μM. Assay mixtures in 0.1 M phosphate buffer pH 6.8 were prepared immediately before use, consisting of 100 μL of tyrosinase solution (15 U/mL) and 1900 μL of test solution. These mixtures were preincubated at 32°C for 30 min, followed by addition of 1000 μL of l-DOPA 1.5 mM in pH 6.8 phosphate buffer, and incubated at 32°C for 7 min. The absorbance (A) at 475 nm was acquired on Shimadzu UV-1800 spectrophotometer. The inhibitory percentage (I%) was calculated according to the formula: I% = [(Acontrol − Asample)/Acontrol] × 100%. Data were represented as means ± standard error (n = 3). The IC50 values were determined by using GraphPad Prism software with multivariate nonlinear regression and R2 > 0.9. Kojic acid was used as positive control.

2.4. HPLC Data of the EtOAc-Soluble Fraction from S. ilicifolius

The concentrations of the EtOAc-soluble fraction and streblus C (1) were approximately 12,000 ppm and 200 ppm, respectively. The detection wavelength was set at 385 nm. An Agilent Zorbax SB-C18 column (150 × 4.6 × 5 mm) was used with a flow rate of 1 mL/min. The injection volume was 10 Μl, and the column temperature was maintained at 30°C. The mixtures of water and ACN were used as the mobile phase with gradient elution (20 ⟶ 40% ACN for 30 min).

2.5. Optical Rotation Calculation

The conformational searches were performed on Spartan'18 (Wave function, Inc., Irvine, USA) by using Merck molecular force field (MMFF). All conformers with Boltzmann weight ˃10% were optimized using DFT method at the B3LYP/6-31G∗ level in the gas phase, to give the preferred conformers with the Boltzmann weight >90%. The optical rotation calculations at sodium D line frequency were carried out using the B3LYP functional and the 6-311++G(2d, 2p) basis set in IEFPCM solvation model for methanol. These calculations were performed on Gaussian 09 (Gaussian, Inc., Wallingford, USA). The calculated optical rotation values were expressed as Boltzmann-weighted average of all output data.

2.6. Molecular Docking

Docking studies of 1 and 2, positive reference (kojic acid), and decoy (hypoxanthine) were performed with Molecular Operating Environment 2019 (MOE 2019.0102) suite (Chemical Computing Group ULC, Montreal, Canada). The structures of these compounds were constructed by using the Builder module. Subsequently, all compounds were minimized up to 0.0001 gradients using the Amber12: EHT force field. The crystal structure of the oxy-tyrosinase was taken from the Protein Data Bank (PDB ID : 1WX2). The caddie protein (ORF378) and water molecules were removed. The enzyme structure was prepared using the QuickPrep module. The binding site was determined based on the Propensity for Ligand Binding (PLB) score in the Site Finder module. The molecular docking was performed by Dock Module, using Triangle Matcher Placement, Induced Fit Refinement, London Dg, and GBVI/WSA dG scoring methods. Five top poses showed up based on the negative binding free energy value (S value). The best pose was selected to analyze the receptor–ligand interactions by using BIOVIA Discovery Studio Visualizer 2016 (Dassault Systèmes Americas Corp., Waltham, USA).

3. Results and Discussion

3.1. Extraction and Isolation

The dried powdered stems of S. ilicifolius were exhaustively extracted in a Soxhlet extractor with n-hexane, EtOAc, and MeOH to yield the corresponding fractions. The EtOAc-soluble fraction was repeatedly chromatographed using silica gel CC and preparative TLC to obtain two undescribed stilbene derivatives, strebluses C (1) and D (2) (Figure 1).

Figure 1

Structure of compounds 1 and 2.

3.2. Structural Elucidation of Two New Isolated Compounds from S. ilicifolius

Compound 1, streblus C, showed a molecular formula to be C22H26O5 based on the HRESIMS sodium adduct ion at m/z 393.1704 [M + Na]+ (calcd for C22H26O5Na, 393.1678). The 1H NMR spectrum showed signals for a 1,2,4-trisubstituted aromatic ring [δH 7.48 (d, J = 8.5 Hz, H-6), 6.46 (d, J = 2.4 Hz, H-3), 6.42 (dd, J = 8.5, 2.4 Hz, H-5), two trans-coupling olefinic protons [δH 7.40 (d, J = 16.4 Hz, H-α), 7.01 (d, J = 16.4 Hz, H-β)], an α-olefinic proton of α, β-unsaturated carbonyl group [δH 5.97 (d, J = 2.0 Hz, H-2′)], an oxymethine proton [δH 4.48 (dd, J = 4.3, 1.6 Hz, H-5′)], a prenyl group [δH 2.54 (dd, J = 14.4, 8.0 Hz, H-1″a), 2.39 (dd, J = 14.4, 7.2 Hz, H-1″b), 5.18 (brs, H-2″), 1.68 (s, H3-4″), 1.63 (s, H3-5″)], two methyl groups [δH 1.32 (s, H3-2‴), 1.18 (s, H3-3‴)], and a methylene group [δH 3.19 (dd, J = 18.8, 1.6 Hz, H2-6′a), 2.82 (ddd, J = 18.8, 4.3, 2.0 Hz, H2-6′b)]. The 13C NMR data (Table 1) exhibited resonances for a keto-carbonyl (δC 199.2), six aromatic carbons and six olefinic carbons [δC 103.6–160.8], an acetonide group [δC 108.0, 27.8, 26.8], two oxygenated carbons [δC 82.8, 77.3], two methylene carbons [δC 33.0, 27.4], and two methyl carbons [δC 26.0, 18.1]. The HMBC correlations (Figure 2) from H-3 to C-1, C-2, and C-4, from H-5 to C-1 and C-4, from H-6 to C-2 and C-4, from H-α to C-2 and C-6, and from H-β to C-1, indicated that two hydroxy groups and Cα-Cβ double bond located at C-2, C-4, and C-1, respectively, of the 1,2,4-trisubstituted aromatic ring. The presence of the cyclohex-2-en-1-one 5,6-acetonide moiety in 1 was established based on the observed HMBC correlations. The HMBC correlations from H-α to C-1′ and from H-β to C-1′ and C-2′ were supportive of the Cβ-C1′ linkage. In addition, the prenyl group was determined to be located at C-4′ by the HMBC correlations from H-1″ to C=O, C-4′, and C-5′ and from H-5′ to C-1″. Therefore, 1 was suggested to be a prenylated stilbene-like compound. The difference in chemical shifts of the methyl groups of the dimethylacetonide moiety in 1 is 0.14 ppm, which established the presence of the cis-acetonide [13]. Moreover, it was unambiguously confirmed based on the NOESY correlation between H-5′ and H2-1″ (Figure 2). The preferred conformations of the cis-(R, R)-acetonide 1 were generated by the MM2 calculation using MMFF94 force field [14]. These conformers were reoptimized by DFT-B3LYP method using basis set 6-31G∗, to obtain the most preferred conformer with 92.8% Boltzmann distribution (Table S1). The optical rotation value at sodium D line frequency was computed using B3LYP/6-311++G(2d, 2p) level with IEFPCM solvent model for methanol. The large basis set with diffuse functions such as 6-311++G(2d, 2p) was applied to give very consistent results [15, 16]. The calculated [α]D value of (R,R)-acetonide 1 was −102.36, compared with its experimental value [α]D: −101.7 (c 0.023, MeOH). Thus, a (R, R) absolute configuration was concluded for streblus C (1).

Figure 2

Significant HMBC (solid arrows) and NOESY (blue, dashed arrows) correlations observed for 1 and 2.

A careful HPLC analysis of the EtOAc-soluble fraction was accomplished, which revealed a peak at t 20.766 min in the chromatogram in accord with that of 1 (t 20.800 min) (Figure S1). Thus, the presence of 1 in the EtOAc-soluble fraction from S. ilicifolius was confirmed, and the possibility of 1 being artifact could be ignored.

Compound 2, streblus D, showed a molecular formula to be C19H20O5 based on the HRESIMS sodium adduct ion at m/z 351.1224 [M + Na]+ (calcd for C19H20O5Na, 351.1208). The 1H and 13C NMR data of 2 (Table 1) resembled those of 1, except for the presence of the singlet olefinic proton at δH 7.31 instead of two trans-coupling olefinic protons in 1 and disappearance of the acetonide group. Based on the 13C NMR data and observed HMBC correlations for 2 (Figure 2), the structure of 2 was assigned as a benzofuran-type stilbene. The NOESY correlations between H-5′ and H2-1″ indicated the presence of the cis-diol configuration. The 3JH-5′/H-6′ coupling constants were 5.9 and 2.7 Hz, to suggest the equatorial configuration of H-5′ [17], which was supportive of the (R,R) or (S,S) absolute configurations for 2. The conformational search for (R,R)-2 was generated and optimized to obtain six conformers with total Boltzmann weight >90% (Table S1). The Boltzmann-weighted calculated [α]D value of (R,R)-2 was +301.74, compared with its experimental value [α]D: −228.9 (c 0.002, MeOH). Thus, a (S, S) absolute configuration was concluded for streblus D (2).

3.3. Tyrosinase Inhibitory Activity of Isolated Compounds from S. ilicifolius

Compounds 1 and 2 were tested for their tyrosinase inhibitory activities [18]. Kojic acid, a purported skin lightening agent, was used as a positive control. Streblus C (1) exhibited remarkable inhibitory effect with an IC50 value of 0.01 μM, which was 4400 times more potent than that of kojic acid (IC50, 44.6 μM). Meanwhile, streblus D (2) was inactive with an IC50 value > 100 μM. These results were consistent with a previous report on the structure–activity relationships of stilbene derivatives. Compound 1 having 2,4-resorcinol subunit contributed the most to inhibitory activity [19]. In addition, the 2-arylbenzofuran derivatives showed lower tyrosinase inhibitory activities than the corresponding stilbene derivatives, suggesting that the formation of the five-membered ring led to the loss of inhibitory activity [20].

3.4. Docking Studies of Compounds 1 and 2

Tyrosinase is an oxidase, which is represented as one of four possible forms (deoxy-, oxy-, met-, and deact- forms) [21]. Oxy-tyrosinase form oxidizes both phenols and catechols to o-quinones. Herein, mushroom tyrosinase (EC 1.14.18.1) plays the same role with respect to oxy-tyrosinase form. Two bound Cu2+ ions bind to six histidine residues, and the peroxide group is in the binding site of oxy-tyrosinase, which has a role in the catalytic oxidation [22]. To explore the strong inhibitory activity of 1 against tyrosinase, the molecular docking studies of 1 and 2, respectively, with oxy-tyrosinase (PDB ID : 1WX2) were carried out [23].

The docking studies were performed with MOE. The top-ranked pose with the highest negative binding free energy value (S value) was selected for further interaction analysis with Discovery Studio Visualizer. Following our previous in silico study on tyrosinase inhibition, this docking procedure was already validated based on the docking results of the positive control (kojic acid) and the decoy (hypoxanthine) [12].

In the binding site, compound 1 showed the H-donor interaction between the C-4 hydroxy group and peroxide bridge PER404, presenting the distances of 1.85 Å. The C-3′ carbonyl group formed the H-acceptor interaction with ASN188 residue (Figure 3). The aromatic ring exhibited the π-π stacking interaction with HIS194 residue localized in the active pocket. In addition, two methyls of the acetonide group showed the π-σ interactions with TRP184 residue. Compound 2 did not show any interaction with the catalytic site (i.e., Cu2+ ions and peroxide bridge), whereas kojic acid showed the interactions with a Cu2+ ion, HIS194, and THR203 residues in the binding site. Three hydroxy groups of 2 interacted with ASP45, ALA202, and MET201 residues via the H-donor bonding. The furan ring formed the π-π and π-σ interactions with TRP184 and ILE42 residues, respectively. The S values and these interactions suggested that 1 showed high binding affinity for oxy-tyrosinase than that of 2 (Table 2). This result confirmed that the formation of furan ring in 2 led to the loss of inhibitory activity.

Figure 3

Docked pose of best ranked docking score of compounds 1 (a) and 2 (b).

Table 2

Docking results of 1 and 2 with oxy-tyrosinase.

Compound	oxy-tyrosinase (1 WX2)
	S values	Interactions	Targeting residues	Distance (Å)
1	–6.56	H-donor	PER404	1.85
		H-acceptor	ASN188	2.44
		π-π	HIS194	4.19
		π-σ	TRP184	5.15
				5.06
				5.47
		σ-σ	VAL195	4.09
2	–6.17	H-donor	ASP45	1.71
			ALA202	2.54
			MET201	2.97
		π-π	TRP184	4.98
		π-σ	ILE42	4.66
				4.61
		σ-σ	VAL195	4.73
Kojic acida	–4.50	H-donor	THR203	2.04
		Metal-acceptor	CU401	2.92
		π-π	HIS194	4.30

aPositive control.

4. Conclusions

Two new stilbene derivatives were isolated from the stems of S. ilicifolius. Their structures were elucidated based on the NMR spectroscopic interpretation and optical rotation calculation. Compound 1 was found to possess strong tyrosinase inhibitory activity with an IC50 value of 0.01 μM. Binding interaction analyses between the isolated compounds (1 and 2) and oxy-tyrosinase active site have been performed.