Plumbagin protects rat cortical neurons from mechanical trauma injury-induced apoptosis by inhibiting NOX۴/ROS/p۳۸ MAPK pathway

سال انتشار: 1404
نوع سند: مقاله ژورنالی
زبان: انگلیسی
مشاهده: 139

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شناسه ملی سند علمی:

JR_AJP-15-6_006

تاریخ نمایه سازی: 25 مهر 1404

چکیده مقاله:

Objective: The aim of this study was to survey whether plumbagin (PLB), a naturally occurring naphthoquinone found in the plants of Plumbago genus, can protect rat primary cortical neurons against mechanical injury which classically mimics traumatic brain injury (TBI) in vitro.Materials and Methods: Rat primary cortical neurons were isolated from time-mated pregnant Sprague-Dawley rats and cultured in vitro, and then, randomly divided into control group,trauma group,trauma+GKT۱۳۷۸۳۱ (۵۰ μM) group,trauma+PLB (۵ μM) group, trauma+PLB (۱۰ μM) group and trauma+PLB (۲۰ μM) group.The influence of PLB on rat primary cortical neuron viability and morphology was evaluated after mechanical injury. Flow cytometry was applied to examine neuron apoptotic rate and intracellular production of reactive oxygen species (ROS) after the pretreatment of PLB. The expression of NOX۴/p۳۸ MAPK pathway-related proteins was determined by Western blotting.Results: Our results indicated that PLB pretreatment significantly alleviated trauma induced-neuronal injury by restoring cell viability and reducing lactate dehydrogenase (LDH) leakage compared with the trauma group (p<۰.۰۱). The morphology of injured neurons was improved by PLB pretreatment. Also, PLB notably reduced ROS production in cultured rat primary cortical neurons compared with the trauma group (p<۰.۰۱). Furthermore, PLB counteracted the mechanical injury-mediated apoptosis (p<۰.۰۱) and inhibited the expression of NOX۴ protein and p۳۸ MAPK phosphorylation in cortical neurons compared with the trauma group (p<۰.۰۱).Conclusion: The present findings illustrate that PLB can alleviate mechanical trauma injury-induced apoptosis by inhibiting the NOX۴/ROS/p۳۸ MAPK pathway in primary cortical neurons.

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نویسندگان

Qianrui Zhang

Department of Pharmacy, General Hospital of the Yangtze River Shipping, Wuhan Brain Hospital

Haitan Fu

Department of Pharmacy, General Hospital of the Yangtze River Shipping, Wuhan Brain Hospital

Wenjuan Gong

Department of Pharmacy, General Hospital of the Yangtze River Shipping, Wuhan Brain Hospital

Feng Cao

Department of Pharmacy, General Hospital of the Yangtze River Shipping, Wuhan Brain Hospital

Tao Wu

Central Laboratory, Wuhan Institute of Clinical Pharmacy, Wuhan Fourth Hospital