| Literature DB >> 24250486 |
Zhen Liu1, Wenyuan Gao, Jingze Zhang, Jing Hu.
Abstract
The seed of Croton tiglium L. (SCT) is a well known folk medicine. In China, it has used to treat gastrointestinal disorders, intestinal inflammation, rheumatism, and so on. Previous studies established its purgative and inflammation properties. In addition, the effects of essential oil of SCT on intestinal transit and gastrointestinal tract has been studied. In the present study, we evaluated the antinociceptive effect of SCT through the writhing test in mice, investigated the effects of it on spontaneous smooth muscle contractions of isolated rabbit jejunum and examined the in-vitro results through the in-vivo small intestine propulsion. We further investigated the possible compounds using HPLC-MS, and six compounds were tentatively identified as phorbol esters. Furthermore, the possible fragmentation pathways of phorbol esters were proposed, and we also detected the possible compounds in the active parts.Entities:
Keywords: Antinociceptive; Croton tiglium L; Intestinal propulsion; Phorbol esters; Rabbit jejunum; Smooth muscle
Year: 2012 PMID: 24250486 PMCID: PMC3832157
Source DB: PubMed Journal: Iran J Pharm Res ISSN: 1726-6882 Impact factor: 1.696
Figure 1Representative intensity (A) and tension (B) or Frequency (C) on the smooth muscle contractions in isolated rabbit jejunum induced by SCTm, SCTp and SCTe with five different doses (0-0.2 mg/mL). The dates were measured by isometric force transducers before (5 min) and after (5 min) treatment of each parts. Each point represents mean ± SEM. of six tissues (n = 6). * p < 0.05 **, p < 0.01 compared to the corresponding values of basal contractility.
Possible compounds from SCTp and SCTe by HPLC-ESI(+)/MSn.
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| Deoxyphorbol acetate methylbutanoate | C27H38O7 | 475.1 | 355.3, 311.0, 277.0, 293.0, 265.1 |
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| Phorbol acetate methylbutenoate | C27H36O8 | 489.2 | 429.3, 389.3, 311.2, 293.0, 265.1 |
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| Deoxyphorbol acetate methylbutenoate | C27H36O7 | 473.0 | 391.0, 311.2, 293.1, 265.1 |
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| Phorbol methylbutanoate isobutyrate | C29H42O8 | 519.6 | 311.0, 293.0, 265.1 |
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| Phorbol decanoate acetate | C32H48O8 | 583.3 | 501.8, 311.1, 293.1, 269.0, 265.1 |
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| Phorbol acetate butyrate | C26H36O8 | 499.1 | 417.3, 311.2, 293.1, 265.0 |
Figure 2Proposed fragmentation pathways and characteristic ions of Phorbol esters: (׀) phorbol 12,13-diesters; (׀׀) Deoxy phorbol-13,20-diesters.
Figure 3Proposed fragmentation pathways and characteristic ions of compound 1 and compound 2.
Effects of SCT extract on acetic acid-induced abdominal writhing in mice.
| Treatment | Dose (mg/Kg) | Acetic acid-induced writhing test | |
|---|---|---|---|
| Number of writhes (30 min) | Inhibition (%) | ||
| Vehicle (p.o | - | 24.5± | - |
| SCTm (p.o | 25 | 20.5± | 16.3% |
| 50 | 17.0± | 30.6% | |
| 100 | 13.3± | 45.7% | |
| 200 | 21.7± | 11.4% | |
| 250 | 23.3± | 1.2% | |
| 300 | 23.8± | 2.9% | |
| SCTe (p.o | 20 | 15.5± | 36.7% |
| SCTp (p.o | 20 | 15.2± | 38.0% |
| Aspirin (p.o | 100 | 8.1± | 80.0% |
Values represent the mean ±SEM of 7 mice.* Significantly different from control group: p < 0.05.** Significantly different from control group: p < 0.01.
Effects of SCT extracts on small intestine propulsion in mice (x±s, n = 10).
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| Control | - | 57.94 ± 10.82 |
| SCT | 200 | 75.06 ± 10.53 ** |
| SCTm | 50 | 77.62 ± 12.98 ** |
| SCTp | 20 | 83.23 ± 10.72 ** |
| SCTe | 10 | 100.00 ± 0.00 ** |
* Significantly different from control group: p < 0.05.** Significantly different from control group: p < 0.01.