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缬草烯酸和缬草提取物可延迟成年斑马鱼由戊四氮(PTZ)诱导的癫痫发作的起始时间。

Valerenic acid and Valeriana officinalis extracts delay onset of Pentylenetetrazole (PTZ)-Induced seizures in adult Danio rerio (Zebrafish).

作者信息

Torres-Hernández Bianca A, Del Valle-Mojica Lisa M, Ortíz José G

机构信息

Neuropharmacology Laboratory, Pharmacology and Toxicology, Department University of Puerto Rico- Medical Science Campus, PO Box 365067, San Juan, 00936-5067, Puerto Rico.

出版信息

BMC Complement Altern Med. 2015 Jul 14;15:228. doi: 10.1186/s12906-015-0731-3.

Abstract

BACKGROUND

Anticonvulsant properties have been attributed to extracts of the herbal medicine Valeriana officinalis. Our aims were to examine the anticonvulsant properties of valerenic acid and valerian extracts and to determine whether valerian preparations interact with the activity of other anti-epileptic drugs (phenytoin or clonazepam). To achieve these goals, we validated the adult zebrafish, Danio rerio, as an animal model for studying anticonvulsant drugs.

METHODS

All drug treatments were administered by immersion in water containing the drug. For assays of anticonvulsant activity, zebrafish were pretreated with: anti-epileptic drugs, valerenic acid, aqueous or ethanolic valerian extracts, or mixtures (phenytoin or clonazepam with valerenic acid or valerian extracts). Seizures were then induced with pentylenetetrazole (PTZ). A behavioral scale was developed for scoring PTZ-induced seizures in adult zebrafish. The seizure latency was evaluated for all pretreatments and control, untreated fish. Valerenic acid and both aqueous and ethanolic extracts of valerian root were also evaluated for their ability to improve survival after pentylenetetrazole-challenge. The assay was validated by comparison with well-studied anticonvulsant drugs (phenytoin, clonazepam, gabapentin and valproate). One-way ANOVA followed by Tukey post-hoc test was performed, using a p < 0.05 level of significance. All treatments were compared with the untreated animals and with the other pretreatments.

RESULTS

After exposure to pentylenetetrazole, zebrafish exhibited a series of stereotypical behaviors prior to the appearance of clonic-like movements--convulsions. Both valerenic acid and valerian extracts (aqueous and ethanolic) significantly extended the latency period to the onset of seizure (convulsion) in adult zebrafish. The ethanolic valerian extract was a more potent anticonvulsant than the aqueous extract. Valerenic acid and both valerian extracts interacted synergistically with clonazepam to extended the latency period to the onset of seizure. Phenytoin showed interaction only with the ethanolic valerian extracts.

CONCLUSIONS

Valerenic acid and valerian extracts have anticonvulsant properties in adult zebrafish. Valerian extracts markedly enhanced the anticonvulsant effect of both clonazepam and phenytoin, and could contribute to therapy of epileptic patients.

摘要

背景

草药缬草的提取物具有抗惊厥特性。我们的目的是研究缬草素和缬草提取物的抗惊厥特性,并确定缬草制剂是否与其他抗癫痫药物(苯妥英或氯硝西泮)的活性相互作用。为实现这些目标,我们验证了成年斑马鱼(Danio rerio)作为研究抗惊厥药物的动物模型。

方法

所有药物处理均通过将鱼浸泡在含有药物的水中进行。为了测定抗惊厥活性,斑马鱼先用以下物质预处理:抗癫痫药物、缬草素、缬草水提取物或乙醇提取物,或混合物(苯妥英或氯硝西泮与缬草素或缬草提取物)。然后用戊四氮(PTZ)诱导癫痫发作。制定了一种行为评分量表,用于对成年斑马鱼中PTZ诱导的癫痫发作进行评分。评估了所有预处理组和未处理的对照鱼的癫痫发作潜伏期。还评估了缬草素以及缬草根部的水提取物和乙醇提取物在戊四氮攻击后提高存活率的能力。通过与经过充分研究的抗惊厥药物(苯妥英、氯硝西泮、加巴喷丁和丙戊酸盐)进行比较来验证该试验。使用p < 0.05的显著性水平进行单因素方差分析,随后进行Tukey事后检验。将所有处理组与未处理的动物以及其他预处理组进行比较。

结果

暴露于戊四氮后,斑马鱼在出现阵挛样运动(惊厥)之前表现出一系列刻板行为。缬草素和缬草提取物(水提取物和乙醇提取物)均显著延长了成年斑马鱼癫痫发作(惊厥)开始的潜伏期。缬草乙醇提取物比水提取物具有更强的抗惊厥作用。缬草素和两种缬草提取物与氯硝西泮协同作用,延长了癫痫发作开始的潜伏期。苯妥英仅与缬草乙醇提取物有相互作用。

结论

缬草素和缬草提取物在成年斑马鱼中具有抗惊厥特性。缬草提取物显著增强了氯硝西泮和苯妥英的抗惊厥作用,可能有助于癫痫患者的治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/daf0/4501072/9031e8b6e7d8/12906_2015_731_Fig1_HTML.jpg

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