Beta-Myrcene as a Sedative-Hypnotic Component from Lavender Essential Oil in DL-4-Chlorophenylalanine-Induced-Insomnia Mice.
Study Design
- Type d'étude
- animal experimental
- Durée
- 1 weeks
- Intervention
- Beta-Myrcene as a Sedative-Hypnotic Component from Lavender Essential Oil in DL-4-Chlorophenylalanine-Induced-Insomnia Mice. None
- Comparateur
- Placebo
- Direction de l'effet
- Positive
- Risque de biais
- Moderate
Abstract
With the increasing prevalence of insomnia-related diseases, the effective treatment of insomnia has become an important health research topic. Lavender (Lavandula angustifolia Mill.) essential oil (LEO) is a commonly used medicine for the treatment of insomnia and neurological disorders. However, neither the active components nor its sedative-hypnotic mechanism have been fully discovered. This study aimed to screen the main active terpenes and discover the possible mechanism of LEO through network pharmacology in the treatment of insomnia-related diseases, as well as to verify our hypothesis in insomnia mice. The results showed that, in LEO's 15 potential active ingredients, beta-myrcene had strong sedative-hypnotic effects through the serotonergic synaptic pathway according to the network pharmacological prediction. Further, PCPA(DL-4-chlorophenylalanine)-induced insomnia mice were treated with beta-myrcene for one day or seven days. The quiet state of insomnia mice was increased effectively, and the hypnotic effect was enhanced by anaobarbital sodium by prolonging sleep duration, decreasing sleep latency, and increasing the rate of falling asleep. Beta-myrcene reduced the damage to hypothalamic neuron cells induced by PCPA and increased neurotransmitter levels of GABA, 5-HT, and Glu in the serum and hypothalamus of insomnia mice. Meanwhile, beta-myrcene exerted an improvement in insomnia by upregulating relevant genes and protein expression in the serotonergic synaptic pathway. These results support the merit of the sedative-hypnotic activity of LEO. Beta-myrcene, a terpene in LEO, may be the main source of its sedative-hypnotic properties. It may serve as a good potential compound in future clinical studies on coping with insomnia.
Full Text
Figures
Tables
Table 3
| Mouse |
|
|
|
| GABAARγ2 | F 5′ AGAATATGGCTATGAGTGTTTGGATGG 3′ | 27 | |
| R 5′ GGCTCCTGTTCGGCAATCTTC 3′ | 21 | ||
| GABAARα1 | F 5′ CCGTTCAGTGGTTGTAGCAGAAG 3′ | 23 | |
| R 5′ TTCAAGTGGAAGTGAGTCGTCATAAC 3′ | 26 | ||
| 5-HT1A | F 5′ TTCTATATTCCGCTGCTGCTCATG 3′ | 24 | |
| R 5′ CCACCTTCTTGACCGTCTTGC 3′ | 21 | ||
| GLUR1 | F 5′ ACAACTCAAGCGTCCAGAATAGAAC 3′ | 25 | |
| R 5′ CCTCATAGCGGTCATTGCCTTC 3′ | 22 | ||
| β-actin | F 5′ GAGGGAAATCGTGCGTGAC 3′ | 19 | |
| R 5′ GCTGGAAGGTGGACAGTGAG 3′ | 20 |
Table 4
| OMIM | Online Mendelian Inheritance in Man |
| TTD | Therapeutic Target Database |
| PCPA | DL-4-chlorophenylalanine |
| LEO | Lavender essential oil |
| GO | Gene Ontology |
| KEGG | Kyoto Encyclopedia of Genes and Genomes |
| 5-HT | 5-hydroxytryptamine |
| GABA | gamma-aminobutyric acid |
| PKA | protein kinase A |
| GLU | Glutamic acid |
| CC | cellular components |
| MF | molecular functions |
| BP | biological processes |
| HE | Histopathological examinations |
| ELISA | Enzyme-linked immunosorbent assay |
| SOD | Superoxide dismutase |
| MDA | Malondialdehyde |
| Rt-PCR | Real-time polymerase chain reaction |
| ECL | Electroche miluminescence |
| GAD67 | glutamate decarboxylase 67 |
| GAD65 | glutamate decarboxylase 65 |
| 5-HT1AR | 5-hydroxytryptamine receptor 1A |
| PVDF | polyvinylidene difluoride |
References
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