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电针对 TRPV1 的靶向作用及基因敲除减轻小鼠晕动病症状。

Targeting TRPV1 to relieve motion sickness symptoms in mice by electroacupuncture and gene deletion.

机构信息

College of Chinese Medicine, Graduate Institute of Acupuncture Science International Master Program, China Medical University, Taichung, 404, Taiwan.

Chinese Medicine Research Center, China Medical University, Taichung, 404, Taiwan.

出版信息

Sci Rep. 2018 Jul 9;8(1):10365. doi: 10.1038/s41598-018-23793-6.

Abstract

Motion sickness (MS) is an acute disorder that occurs in healthy individuals worldwide regardless of gender, age, or ethnicity. Our study used a mouse model to rule out the effects of any psychological factors related to MS and EA. Subjects were randomly separated into four groups, namely the control group (Con), motion sickness inducing group (MS), mentioning sickness inducing with electroacupuncture treatment group (EA) and motion sickness inducing only in TRPV1 knockout mice group (TRPV1). The consumption of kaolin, a non-nutrient substance, was measured as a behavior observed response of an emetic reflex in a murine model. This behavior is referred to as pica behavior. Our results showed that pica behavior was observed in the MS group. Moreover, kaolin consumption in the EA group decreased to the average baseline of the control group. A similar result was observed in TRPV1 null mice. We also observed an increase of TRPV1 and related molecules in the thalamus, hypothalamic and brain stem after MS stimulation and a significant decrease in the EA and TRPV1 null groups. This is the first study to demonstrate that TRPV1 pathways are possibly associated with mechanisms of MS, and can be attended through EA or TRPV1 genetic manipulation.

摘要

运动病(MS)是一种急性疾病,发生在全球范围内的健康人群中,无论性别、年龄或种族如何。我们的研究使用了一种小鼠模型来排除与 MS 和 EA 相关的任何心理因素的影响。实验对象被随机分为四组,分别为对照组(Con)、运动病诱导组(MS)、电针治疗运动病诱导组(EA)和 TRPV1 基因敲除小鼠运动病诱导组(TRPV1)。高岭土是一种非营养物质,其消耗量被作为一种观察到的呕吐反射行为反应的指标,这种行为被称为异嗜行为。我们的研究结果表明,在 MS 组中观察到了异嗜行为。此外,EA 组的高岭土摄入量减少到了对照组的平均基线水平。在 TRPV1 基因敲除小鼠中也观察到了类似的结果。我们还观察到,在 MS 刺激后,丘脑、下丘脑和脑干中的 TRPV1 和相关分子增加,而在 EA 和 TRPV1 基因敲除组中则显著减少。这是首次研究表明 TRPV1 途径可能与 MS 的机制有关,并且可以通过 EA 或 TRPV1 基因操作来调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6fe2/6037734/58d0433af522/41598_2018_23793_Fig1_HTML.jpg

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