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The neurotoxic effect of clindamycin - induced gut bacterial imbalance and orally administered propionic acid on DNA damage assessed by the comet assay: protective potency of carnosine and carnitine

机译:通过彗星试验评估了克林霉素诱导的肠道细菌失衡和口服丙酸对DNA损伤的神经毒性作用:肌肽和肉碱的保护效力

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Background Comet assay is a quick method for assessing DNA damage in individual cells. It allows the detection of single and double DNA strand breaks, which represent the direct effect of some damaging agents. This study uses standard comet quantification models to compare the neurotoxic effect of orally administered propionic acid (PA) to that produced as a metabolite of bacterial overgrowth induced by clindamycin. Additionally, the protective effect of carnosine and carnitine as natural dietary supplements is assessed. Methods Single cell gel electrophoresis (comet assays) were performed on brain cortex and medulla samples after removal from nine groups of hamsters including: a control (untreated) group; PA-intoxicated group; clindamycin treated group; clindamycin-carnosine group and; clindamycin-carnitine group. Results There were significant double strand breaks recorded as tail length, tail moment and % DNA damage in PA and clindamycin-treated groups for the cortex and medulla compared to the control group. Neuroprotective effects of carnosine and carnitine were observed. Receiver Operating Characteristics curve (ROC) analysis showed satisfactory values of sensitivity and specificity of the comet assay parameters. Conclusion Percentage DNA damage, tail length, and tail moment are adequate biomarkers of PA neurotoxicity due to oral administration or as a metabolite of induced enteric bacterial overgrowth. Establishing biomarkers of these two exposures is important for protecting children’s health by documenting the role of the imbalance in gut microbiota in the etiology of autism through the gut-brain axis. These outcomes will help efforts directed at controlling the prevalence of autism, a disorder recently related to PA neurotoxicity.
机译:背景彗星分析是一种评估单个细胞DNA损伤的快速方法。它可以检测单链和双链DNA断裂,这代表了某些破坏剂的直接作用。这项研究使用标准的彗星量化模型来比较口服丙酸(PA)与克林霉素诱导的细菌过度生长的代谢产物所产生的神经毒性作用。此外,评估了肌肽和肉碱作为天然膳食补充剂的保护作用。方法从9组仓鼠中取出大脑皮层和延髓样品后,进行单细胞凝胶电泳(彗星试验),包括:对照组(未治疗);和对照组。 PA中毒组;克林霉素治疗组;克林霉素-肌肽组;和克林霉素肉碱组。结果与对照组相比,PA和克林霉素治疗组的皮质和延髓有明显的双链断裂,如尾长,尾矩和DNA损伤百分比。观察到肌肽和肉碱的神经保护作用。接收器工作特性曲线(ROC)分析显示了令人满意的彗星测定参数灵敏度和特异性值。结论DNA损伤百分比,尾巴长度和尾矩是口服或作为诱导性肠细菌过度生长的代谢产物而引起的PA神经毒性的适当生物标志物。建立这两种接触的生物标记物对肠道微生物群失衡在肠道脑轴上的自闭症病因中的作用进行记录,对于保护儿童的健康至关重要。这些结果将有助于控制自闭症的患病率,自闭症是最近与PA神经毒性相关的疾病。

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