Anti-Inflammatory Cycloartane-Type Saponins of Astragalus membranaceus
by
,
Dae-Young Lee
1
,
Hyung-Jun Noh
1, 
Jehun Choi
1,
Kyeong-Hee Lee
1,
Min-Ho Lee
2,
Ji-Hyun Lee
1,
Yoonpyo Hong
1,
Seung-Eun Lee
1,
Seung-Yu Kim
1 and
Geum-Soog Kim
1,* 1
Department of Herbal Crop Research, National Institute of Horticultural and Herbal Science, RDA, Eumseong 369-873, Korea
2
Department of Food Technology and Services, Eulji University, Seongnam 461-723, Korea
*
Author to whom correspondence should be addressed.
Molecules 2013, 18(4), 3725-3732; https://doi.org/10.3390/molecules18043725
Submission received: 1 February 2013
/
Revised: 19 March 2013
/
Accepted: 20 March 2013
/
Published: 25 March 2013
(This article belongs to the Special Issue Triterpenes and Triterpenoids 2013)
Abstract
:A new cycloartane-type triterpene glycoside, agroastragaloside V (1) was isolated from the roots of Astragalus membranaceus. The structure was identified as 3-O-β-(2'-O-acetyl)-d-xylopyranosyl-6-O-β-d-glucopyranosyl-(24S)-3β,6α,24α,25-tetrahydroxy-9,19-cyclolanostane, by means of spectroscopic methods, including HR-FAB/MS, 1D NMR (1H, 13C, DEPT), 2D NMR (gCOSY, gHSQC, gHMBC, NOESY), and IR spectroscopy. Four known cycloartane glycosides, namely, agroastragaloside I (2), agroastragaloside II (3), isoastragaloside II (4) and astragaloside IV (5) were also isolated. All isolated compounds were tested for the ability to inhibit LPS-induced nitric oxide production in RAW264.7 macrophages.
1. Introduction
Astragalus species are among the most widely distributed in northern temperate regions and tropical African mountains [1]. Five species have been identified in Korea and the primary parts used for medicinal purposes, are cylindrical, but not usually branched, measure around 30–90 cm in length, and are covered with a tough, yellowish-brown skin with a sweet white inner pulp [2]. Radix astragali, the dried root of Astragalus membranaceus (FISCH.) BGE., known as Huangqi in China and Korea, is one of the most widely used medicinal herbs prescribed in many Chinese formulas to reinforce “Qi” (the vital energy) [3]. Studies of its pharmacological and clinical uses have demonstrated that Astragali Radix has many biological functions, including hepatoprotection [4], neuroprotection [5], cardiotonic [6], anti-aging activity [7], anti-cancer effects [8], and anti-inflammatory effects [9]. Astragalus species are rich in cycloartane-type triterpene glycosides that possess diverse biological activities. Some cycloartane triterpene glycosides have been shown to have antitumor activity [10]. Astragaloside IV, a cycloartane triterpene glycoside extracted from Radix Astragali, has a broad range of pharmacological properties, including antiapoptotic [11], anti-inflammatory and antihypertensive [12] effects.
As part of our efforts to isolate the chemical constituents of Astragali Radix to evaluate A. membranaceus qualitatively, we report herein on the isolation of a new minor saponin, agroastragaloside V (1), obtained from the roots of A. membranaceus cultivated in Korea, together with four known compounds 2–5, and the structural determination of these substances using extensive spectroscopic methods. Several previous studies have provided immune stimulant effects of several cycloartane-type triterpene glycosides and the extracts on macrophage activation and expression of inflammatory cytokines were investigated from Astragalus species [9,12]. Therefore, isolated compounds 1–5 were evaluated for anti-inflammatory activities through the measurement of nitrite, a soluble oxidation product of nitric oxide (NO), in lipopolysaccharide (LPS)-induced RAW 254.7 macrophage cells.
2. Results and Discussion
A 80% methanolic extract of dried roots of A. membranaceus was suspended in H2O and extracted with EtOAc, and then n-BuOH. The EtOAc soluble fraction was concentrated under reduced pressure to produce a residue which was then subjected to multiple chromatographic steps using silica gel, reversed-phase C18, and Sephadex LH-20, yielding the compounds 1–5 (Figure 1).
Figure 1.
Chemical structures of isolated compounds 1–5.
Compound 1, was obtained as an amorphous white powder from MeOH. High-resolution (HR) FAB-MS exhibited an ion peak for [M−H]− at m/z 811.4777, which is compatible with the molecular formula C43H72O14. The IR spectrum of 1 showed the presence of a hydroxyl group (3433 cm−1) and an ester carbonyl group (1,724 cm−1). The 1H-NMR spectrum of 1 (Table 1) revealed the presence of a cyclopropane methylene group with signals at δH 0.17 (1H, d, J = 4.0 Hz) and 0.53 (1H, d, J = 4.0 Hz) and also contained signals for six tertiary methyl groups at δH 0.95, 1.28, 1.38, 1.41, 1.43, and 1.78, and for one acetyl methyl group (δH 2.03) which were correlated in HSQC with carbon signals at δC 19.9, 16.6, 18.6, 25.7, 26.5, 28.3 and acetyl (δC 21.2), respectively. A secondary methyl group at δH 1.07 (3H, d, J = 6.4 Hz) and at δC 18.3, and four oxygen bearing methine proton signals at δH 4.48 (ddd, J = 8.0, 8.0, 5.2 Hz), 3.53 (ddd, J = 9.5, 9.5, 4.5 Hz), 3.41 (dd, J = 10.5, 2.2 Hz) and 3.23 (dd, J = 11.3, 4.0 Hz), which were indicative of secondary alcoholic functions (Table 1), were readily noticed in the 1H-NMR spectrum. Furthermore, the 1H-NMR spectrum of 1 clearly showed two anomeric doublets at δH 4.77 (J = 7.6 Hz), and 4.96 (J = 7.2 Hz) in the downfield region, indicating of the presence of two β-linked sugars. This was supported by the 13C-NMR spectrum, which showed two anomeric carbon signals at δC 104.7 and 105.2. The chemical shifts of the individual protons of the two sugar units were revealed from a combination of 2D-COSY spectral analyses, and 13C chemical shifts of their relative attached carbons were assigned unambiguously from the HSQC and HMBC experiments which led to the identification of a β-xylopyranosyl unit and a β-glucopyranosyl unit. The sites of attachment of the xylose and glucose moieties of 1 were determined by HMBC experiment to be at C-3 and C-6, respectively. In the HMBC spectrum, the first anomeric proton signal at δH 4.77 (H-1') showed long range correlation with the carbon at δC 89.0 (C-3). Also the second anomeric proton signals at δH 4.96 (H-1") showed long-range correlation with the carbons at δC 79.1 (C-6), respectively. Consequently, xylose and glucose should be attached to the hydroxyl groups at C-3 and C-6. The relative configuration of OH-6 was confirmed by a NOESY experiment, which showed a correlation between H-6 and H-28, H-19a, as well as H-8. These NOE correlations indicated that the oxygen at C-6 is α-oriented. In the 1H-NMR spectrum, signals at 2.03 (3H, s), and 13C-NMR signals at 170.0, showed the presence of an acetoxyl group in 1. The NMR data of the acetoxyl moiety of 1 were in good agreement with those reported for agroastagaloside II (3) [13,14]. Also, the cross peak between the oxygenated methine proton signal of xylose (H-2') and the ester carbon signal (δC 170.0) suggested that the acetyl group was linked to the hydroxyl of C-2' of xylose (Figure 2) in the HMBC spectrum. This was confirmed by the down-field shifts of the carbon (δC 75.7) and proton signal (δH 5.52, H-2') owing to the esterification effect. The 13C-NMR spectrum of l displayed a total of 43 carbon signals. Based on a DEPT experiment, the HSQC spectrum, and a comparison with the 13C-NMR data of the related agroastagaloside II (3), all the signals could be assigned (Table 2). These data were similar to agroastagaloside II (3) with the exception of the proton and carbon resonances for the lack of an oxygenated methine moiety at the C-16 position, respectively. The methylene signals due to C-16 in 1 were replaced by those of an oxygenated methine (δH 4.72 and δC 72.1) in agroastagaloside II (3) [14]. The molecular weight of 1 was 16 Da less than that of agroastagaloside II (3), indicating the presence of one less hydroxyl group. This conclusion was also supported by the HMBC spectrum, which showed 2J, 3J, and long range correlation between the proton signal of H-17 (δH 1.51) and the carbon signals of C-13 (δC 45.8), C-16 (δC 28.7), C-20 (δC 28.6), C-18 (δC 18.6) and C-21 (δC 18.3) (Figure 2). The d-configurations of xylose and glucose units were established after hydrolysis of 1 followed by GC analysis [15]. Finally, the structure of 1 was determined to be 3-O-β-(2'-O-acetyl)-d-xylopyranosyl-6-O-β-d-glucopyranosyl-(24S)-3β,6α,24α,25-tetrahydroxy-9,19-cyclolanostane, and named agroastragaloside V. Comparisons of NMR and MS data for the known compounds 2–5 with reported values led to their identification as agroastragaloside I (2) [16], agroastragaloside II (3) [14], isoastragaloside II (4) [13] and astragaloside IV (5) [16], respectively (Figure 1).
Table 1.
1H- (400 MHz) and 13C-NMR (100 MHz) data of compound 1 (in pyridine-d5, δ in ppm, J in Hz) a.
| No. | δH | δC (DEPT) | No. | δH | δC (DEPT) |
|---|---|---|---|---|---|
| 1 | 1.27 b, 1.55 b, m | 32.1 (CH2) | 23 | 1.68 b, 1.96 b, m | 27.9 (CH2) |
| 2 | 1.68 b, 1.94 b, m | 30.0 (CH2) | 24 | 3.91, brd, J = 10.8 | 77.1 (CH) |
| 3 | 3.39, dd, J = 4.4, 11.6 | 89.0 (CH) | 25 | - | 72.5 |
| 4 | - | 42.3 | 26 | 1.43, s | 25.7 (CH3) |
| 5 | 1.93, d, J = 8.8 | 52.5 (CH) | 27 | 1.41, s | 26.5 (CH3) |
| 6 | 3.78, ddd, J = 4.4, 9.6, 9.6 | 79.1 (CH) | 28 | 1.78, s | 28.3 (CH3) |
| 7 | 1.82, 2.25, m | 34.5 (CH2) | 29 | 1.28, s | 16.6 (CH3) |
| 8 | 1.90, m | 45.8 (CH) | 30 | 0.95, s | 19.9 (CH3) |
| 9 | - | 21.5 | 1' | 4.77, d, J = 7.6 | 104.7 (CH) |
| 10 | - | 28.7 | 2' | 5.52, dd, J = 8.0, 8.0 | 75.7 (CH) |
| 11 | 1.15, 1,89 b, m | 26.3 (CH2) | 3' | 4.15 b, m | 76.3 (CH) |
| 12 | 1.64 b, 2.35 b, m | 33.2 (CH2) | 4' | 4.14 b, m | 71.4 (CH) |
| 13 | - | 45.8 | 5' | 4.27 b, m, H-5'a 3.62, dd, J = 9.6, 11.6, H-5'b | 67.1 (CH2) |
| 14 | - | 46.9 | 1'' | 4.96, d, J = 7.2 | 105.2 (CH) |
| 15 | 1.45 b, 1.66 b, m | 30.0 (CH2) | 2'' | 4.00, dd, J = 8.0, 8.0 | 75.6 (CH) |
| 16 | 1.33 b, 1.54 b, m | 28.7 (CH2) | 3'' | 4.29, m | 79.1 (CH) |
| 17 | 1.51 b, m | 49.7 (CH) | 4'' | 4.10, dd, J = 8.8, 8.8 | 72.0 (CH) |
| 18 | 1.38, s | 18.6 (CH3) | 5'' | 3.88, m | 78.1 (CH) |
| 19 | 0.17, d, J = 4.0, H-19a 0.53, d, J = 4.0, H-19b | 28.4 (CH2) | 6'' | 4.42, dd, J = 2.4, 11.2, H-6''a 4.29, dd, J = 3.6, 11.2, H-6''b | 63.2 (CH2) |
| 20 | 2.39 b, m | 28.6 (CH) | COCH3 | - | 170.0 |
| 21 | 1.07, d, J = 6.4 | 18.3 (CH3) | COCH3 | 2.03, s | 21.2 (CH3) |
| 22 | 1.40, 1.99 b, m | 33.0 (CH2) |
a Assignments were confirmed by 1H-1H COSY, HSQC, and HMBC. b Signals are unclear due to overlapping.
Figure 2.
Key 1H-1H COSY (bold dash) and HMBC (blue arrow) correlations of compound 1.
Previous studies have already reported on the anti-inflammatory effects of components obtained from A. membranaceus [9,12]. Thus, we also investigated the inhibitory effects of compounds 1–5 on NO production by using the Griess reaction to measure nitrite, a soluble oxidation product of NO, in the culture medium of LPS-induced RAW 264.7 macrophages. As shown in Table 2, compounds 1–5 inhibited NO production with IC50 values in the range of 1.38 to 4.70 μM, respectively. Some cell toxicity was observed in cells treated with compounds 2, 3 and 4, whereas other compounds had no influence on cell viability.
Table 2.
Inhibitory effects of compounds 1–5 against LPS-Induced NO production in RAW 264.7 macrophage cells.
| Compound | IC50 (μM) a | cell viability (%) b |
|---|---|---|
| 1 | 1.85 ± 0.24 | 93.15 ± 6.96 |
| 2 | 1.38 ± 0.15 | 54.54 ± 1.21 |
| 3 | 2.31 ± 0.47 | 47.56 ± 3.40 |
| 4 | 4.70 ± 1.77 | 68.98 ± 1.82 |
| 5 | 2.09 ± 0.27 | 94.42 ± 4.33 |
| Caffeic acid c | 0.83 ± 1.15 | 82.20 ± 1.64 |
a The IC50 value of each compound was defined as the concentration (μM) that caused 50% inhibition of NO production in LPS-activated RAW 264.7 macrophage cells. Cells were pretreated for 1 h with compounds before stimulation with LPS (1 μg/mL) for 7 h; b Cell viability indicates mean maximum inhibitory effect, at a concentration of 100 μM, expressed as a percentage inhibition of nitrite production induced by LPS (1 μg/mL) in the presence of vehicle; c Positive control. The results are averages of three independent experiments, and the data are expressed as mean ± SD.
3. Experimental
3.1. General
1H-, 13C-, and 2D-NMR spectra were recorded on a Varian Unity Inova AS 400 FT-NMR instrument, and the chemical shifts were given in δ (ppm) based on the use of tetramethylsilane (TMS) as an internal standard. Optical rotations were measured on a JASCOP-1010 digital polarimeter. IR spectra were run on a Perkin Elmer Spectrum One FT-IR spectrometer. HR-FABMS spectra were obtained using a JEOL JMS-700 mass spectrometer (Tokyo, Japan). A Shimadzu gas chromatograph (GC-14B) equipped with an on-column injection system and flame ionization detector (FID) was used (Tokyo, Japan). Silica gel 60 (Merck, 230–400 mesh), LiChroprep RP-18 (Merck, 40–63 μm), and Sephadex LH-20 (Amersham Pharmacia Biotech., Uppsala, Sweden) were used for column chromatography (CC). Pre-coated silica gel plates (Merck, Kieselgel 60 F254, 0.25 mm) and pre-coated RP-18 F254s plates (Merck) were used for analytical thin-layer chromatography analyses. Spots were visualized by spraying with 10% aqueous H2SO4 solution followed by heating.
3.2. Plant Material
The roots of A. membranaceus were cultivated in Jecheon, Chungbuk Province, Korea, for one year, harvested in September 2011, and identified by Dr. Jung-Hun Lee, National Institute of Horticultural and Herbal Science (NIHHS), Rural Development Administration (RDA). A voucher specimen (MPS00874) was preserved at the NIHHS, RDA.
3.3. Extraction and Isolation
The roots of A. membranaceus (10 kg) were powdered and extracted three times with 36 L of aqueous 80% MeOH at room temperature for 24 h. After concentration in vacuo, the MeOH extract (1,387 g) was suspended in H2O (3 L) and then partitioned with EtOAc (3 L × 3) followed by concentration to give the EtOAc fraction (E, 57 g). Fraction E (ARE, 57 g) was subjected to a silica gel CC (10 × 21 cm) using a gradient of CH2Cl2–MeOH–H2O (15:3:1→12:3:1→9:3:1→7:3:1→MeOH, each 2.5 L to yield 23 fractions (E1 to E23). Fraction E10 [2.51 g, elution volume/total volume (Ve/Vt) 0.45–0.57] was subjected to the RP-18 silica gel CC [4.5 × 12 cm, MeOH–H2O (1:1.8, 2.5 L)] to give compound 2 [184 mg, Ve/Vt 0.43–0.65, (RP-18 F254s) Rf 0.50, MeOH–H2O (5:1)]. Subfraction E17 (400 mg, Ve/Vt 0.66–0.70) was separated by CC [RP-18 (4.5 × 8 cm), MeOH–H2O (2.5:1, 1.5 L)] to give compound 4 [25 mg, Ve/Vt 0.38–0.45, TLC (RP-18 F254s) Rf 0.30, MeOH–H2O (3:1)]. Fraction E21 [140 mg, Ve/Vt 0.88–0.92] was subjected to the RP-18 CC [3.5 × 7.5 cm, MeOH–H2O (3:1) to give five subfractions (E21-1 to E21-5). Subfraction E21-3 (22 mg, Ve/Vt 0.59–0.68) was fractionated using a Sephadex LH 20 CC [2.5 × 50 cm, MeOH–H2O (4:1, 800 L)] and yielded compound 1 [12 mg, Ve/Vt 0.66–0.85, TLC (RP-18 F254s) Rf 0.40, MeOH–H2O (5:1)]. Subfraction E21-6+7 (45 mg, Ve/Vt 0.59–0.68) was subjected to the RP-18 CC [2.5 × 7.5 cm, MeOH–H2O (3:1) to give compound 5 [18 mg, Ve/Vt 0.67–0.90, TLC (RP-18 F254s) Rf 0.35, MeOH–H2O (5:1)]. Fraction E22 [140 mg, Ve/Vt 0.93–0.98] was subjected to the RP-18 CC [3.5 × 6 cm, MeOH–H2O (3:1) to give five subfractions (E22-1 to E22-6). Subfraction E22-4 (78 mg, Ve/Vt 0.72–0.81) was fractionated using a RP-18 CC [2.5 × 5 cm, MeOH–H2O (2.5:1, 800 L)] and yielded compound 3 [33 mg, Ve/Vt 0.65–0.80, TLC (RP-18 F254s) Rf 0.50, MeOH–H2O (5:1)].
3.4. Spectroscopic Data
Agroastragaloside V (1). Amorphous white powder; ![Molecules 18 03725 i001]()
−18.5° (c = 0.15, MeOH); IR (CaF2 window) cm−1: 3433, 1724, 1510, 1245, 1065; HR-FAB/MS m/z 811.4777 [M−H]− (calcd for C43H71O14, 811.4843); 1H- and 13C-NMR data, see Table 1.
−18.5° (c = 0.15, MeOH); IR (CaF2 window) cm−1: 3433, 1724, 1510, 1245, 1065; HR-FAB/MS m/z 811.4777 [M−H]− (calcd for C43H71O14, 811.4843); 1H- and 13C-NMR data, see Table 1.3.5. Acid Hydrolysis and GC Analysis
A solution of compound 1 (3 mg) in 2 N HCl (2 ml) was heated at 80 °C for 6 h. The mixture was cooled at 0 °C and neutralization with 2 N NaOH in H2O (2 mL) and then extracted with CHCl3. The aqueous layer was concentrated under a vacuum to give a residue of the sugar fraction. The residue was dissolved in pyridine (100 μL), and then 0.1 M L-cysteine methyl ester hydrochloride (150 μL) was added. After reacting at 60 °C for 90 min, the reaction mixture was dried under a vacuum. For derivatization, 100 μL of N-methyl-N-(trimethylsilyl)trifluoroacetamide (MSTFA) was added and the mixture incubated at 37 °C for 30 min. Then, the mixture was subjected to GC analysis under the following conditions: capillary column, DB-5 (30 m × 0.32 mm × 0.25 μm); detector, FID; detector temperature, 280 °C; injector temperature, 250 °C; carrier, N2 gas (20.4 mL/min); oven temperature, 170–250 °C with a rate of 5 °C/min, with one μL of each sample injected directly into the inject port (split-less mode). The peaks from the hydrolyrate of 1 were detected at 9.24 and 10.02 (d-xylose) and 12.66 min d-glucose). The retention times for authentic samples in the same experimental conditions were detected at 9.24 and 10.02 (d-xylose, Sigma), and 12.66 min (d-glucose, Sigma), respectively.
3.6. Measurement of NO Production and Cell Viability
Assays for NO production and cell viability were carried out as previously described [17]. Briefly, RAW 264.7 macrophages were harvested and seeded in 24-well plates (3 × 105 cells/well) for the measurement of NO production. The plates were pretreated with various concentrations of samples for 1 h and incubated with LPS (1 μg/mL) for 7 h. The amount of NO was determined by the nitrite concentration in the cultured RAW264.7 macrophage supernatants using the Griess reagent. The cell viability was evaluated by MTT reduction.
4. Conclusions
The new compound 3-O-β-(2'-O-acetyl)-d-xylopyranosyl-6-O-β-d-glucopyranosyl-(24S)-3β,6α, 24α,25-tetrahydroxy-9,19-cyclolanostane, named agroastragaloside V (1), was isolated from Astragalus membranaceus, together with four known cycloartane glycosides. According to previous investigations of the various Astragalus species, we have evaluated the inhibitory activities of all compounds against LPS-induced NO production in RAW264.7 macrophages. Agroastragaloside V and astragaloside IV showed significant inhibition of NO production without cytotoxicity. The results provide a potential explanation for the use of this plant as a herbal medicine in the treatment of inflammatory diseases, and they merit consideration as leads for anti-inflammatory agents.
Supplementary Materials
1H-NMR, 13C-NMR, and HR-FABMS spectra of 1 are available free of charge via the internet at https://www.mdpi.com/1420-3049/18/4/3725/s1.
Acknowledgments
This work was supported by 2013 Post-Doctoral Fellowship Program of NIHH and Cooperative Research Program for Agricultural Science & Technology Development (Project No. PJ008465), Rural Development Administration, Korea.
References
- Evans, W.C. Trease and Evans Pharmacognosy, 15th ed.; Elsevier Science Ltd.: London, UK, 2002; p. 26. [Google Scholar]
- Jung, B.S.; Shin, M.K. Hyang Yak Dae Sa Jeon, 3rd ed.; Young Lim Sa Publisher: Seoul, Korea, 2003; pp. 662–664. [Google Scholar]
- Tang, W.; Eisenbrand, G. Chinese Drugs of Plant Origin: Chemistry, Phamocology and Use in Traditional and Modern Medicine; Springer-Verlag: Berlin, Germany, 1992; pp. 191–197. [Google Scholar]
- Rios, J.L.; Waterman, P.G. A review on the pharmacology and toxicology of Astragalus. Phytother. Res. 1997, 11, 411–418. [Google Scholar] [CrossRef]
- Tohda, C.; Tamura, T.; Matsuyama, S.; Komatsu, K. Promotion of axonal maturation and prevention of memory loss in mice by extracts of Astragalus mongholicus. Br. J. Pharmacol. 2006, 149, 532–541. [Google Scholar] [CrossRef]
- Zhang, W.D.; Chen, H.; Zhang, C.; Liu, R.H.; Li, H.L.; Chen, H.Z. Astragaloside IV from Astragalus membranaceus shows cardioprotection during myocardial ischemia in vivo and in vitro. Planta Med. 2006, 72, 4–8. [Google Scholar] [CrossRef]
- Lei, H.; Wang, B.; Li, W.P.; Yang, Y.; Zhou, A.W.; Chen, M.Z. Anti-aging effect of astragalosides and its mechanism of action. Acta Pharmacol. Sin. 2003, 24, 230–234. [Google Scholar]
- Cho, W.C.S.; Leung, K.N. In vitro and in vivo anti-tumor effects of Astragalus membranaceus. Cancer Lett. 2007, 252, 43–54. [Google Scholar] [CrossRef]
- Zhang, W.J.; Hufnag, P.; Binder, B.R.; Wojta, J. Anti-inflammatory activity of astragaloside IV is mediated by inhibition of NF-kappaB activation and adhesion molecule expression. Thromb. Haemost. 2003, 90, 904–914. [Google Scholar]
- Tin, M.M.Y.; Cho, C.H.; Chan, K.; James, A.E.; Ko, J.K. stragalus saponins induce growth inhibition and apoptosis in human colon cancer cells and tumor xenograft. Carcinogenesis 2007, 28, 1347–1355. [Google Scholar] [CrossRef]
- Xu, M.E.; Xiao, S.Z.; Sun, Y.H.; Ou-Yang, Y.; Zheng, X.X. Effects of astragaloside IV on pathogenesis of metabolic syndrome in vitro. Acta Pharmacol. Sin. 2006, 27, 229–236. [Google Scholar] [CrossRef]
- Zhang, Y.D.; Wang, Y.L.; Shen, J.P. Effects of Astragalous saponins on antiinflammation and antihypertension. Acta Pharmacol. Sin. 1984, 19, 333–337. [Google Scholar]
- Kim, J.S.; Yean, M.H.; Lee, E.J.; Kang, S.S. Phytochemical studies on Astragalus root (1)-Saponins. Nat. Prod. Sci. 2008, 14, 37–46. [Google Scholar]
- Hirotani, M.; Zhou, Y.; Rui, H.; Furuya, T. Cycloartane triterpene glycosides from the hairy root cultures of Astragalus membranaceus. Phytochemistry 1994, 37, 1403–1407. [Google Scholar] [CrossRef]
- Lee, D.Y.; Seo, K.H.; Lee, D.S.; Kim, Y.C.; Chung, I.S.; Kim, G.W.; Cheoi, D.S.; Baek, N.I. 172 Bioactive 3,4-seco-triterpenoids from the fruits of Acanthopanax sessiliflorus. J. Nat. Prod. 2012, 75, 1138–1144. [Google Scholar] [CrossRef]
- Hirotani, M.; Zhou, Y.; Lui, H.; Furuya, T. Astragalosides from hairy root cultures of Astragalus membranaceus. Phytochemistry 1994, 36, 665–670. [Google Scholar] [CrossRef]
- Jung, L.H.; Lee, D.Y.; Cho, J.G.; Lee, S.M.; Kang, H.C.; Seo, W.D.; Kang, H.W.; Kim, J.Y.; Baek, N.I. A new flavonolignan from the aerial parts of Oryza sativa L. inhibits nitric oxide production in RAW 264.7 macrophage cells. J. Korean Soc. Appl. 2011, 54, 865–870. [Google Scholar] [CrossRef]
- Sample Availability: Samples of the compounds 1–5 are available from the authors.
© 2013 by the authors; licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/).
Share and Cite
MDPI and ACS Style
Lee, D.-Y.; Noh, H.-J.; Choi, J.; Lee, K.-H.; Lee, M.-H.; Lee, J.-H.; Hong, Y.; Lee, S.-E.; Kim, S.-Y.; Kim, G.-S. Anti-Inflammatory Cycloartane-Type Saponins of Astragalus membranaceus. Molecules 2013, 18, 3725-3732. https://doi.org/10.3390/molecules18043725
AMA Style
Lee D-Y, Noh H-J, Choi J, Lee K-H, Lee M-H, Lee J-H, Hong Y, Lee S-E, Kim S-Y, Kim G-S. Anti-Inflammatory Cycloartane-Type Saponins of Astragalus membranaceus. Molecules. 2013; 18(4):3725-3732. https://doi.org/10.3390/molecules18043725
Chicago/Turabian StyleLee, Dae-Young, Hyung-Jun Noh, Jehun Choi, Kyeong-Hee Lee, Min-Ho Lee, Ji-Hyun Lee, Yoonpyo Hong, Seung-Eun Lee, Seung-Yu Kim, and Geum-Soog Kim. 2013. "Anti-Inflammatory Cycloartane-Type Saponins of Astragalus membranaceus" Molecules 18, no. 4: 3725-3732. https://doi.org/10.3390/molecules18043725
APA StyleLee, D. -Y., Noh, H. -J., Choi, J., Lee, K. -H., Lee, M. -H., Lee, J. -H., Hong, Y., Lee, S. -E., Kim, S. -Y., & Kim, G. -S. (2013). Anti-Inflammatory Cycloartane-Type Saponins of Astragalus membranaceus. Molecules, 18(4), 3725-3732. https://doi.org/10.3390/molecules18043725
