脂联素缺乏是七氟醚暴露后肥胖小鼠认知功能障碍的关键因素。
Adiponectin deficiency is a critical factor contributing to cognitive dysfunction in obese mice after sevoflurane exposure.
机构信息
Department of Anaesthesiology, School of Clinical Medicine, LKS Faculty of Medicine, The University of Hong Kong, Room K424, Queen Mary Hospital, Pokfulam, Hong Kong, HKSAR, China.
Laboratory of Neurodegenerative Disease, School of Biomedical Sciences, LKS Faculty of Medicine, The University of Hong Kong, L4-49, Laboratory Block, 21 Sassoon Road, Hong Kong, HKSAR, China.
出版信息
Mol Med. 2024 Oct 16;30(1):177. doi: 10.1186/s10020-024-00954-0.
BACKGROUND
The number of major operations performed in obese patients is expected to increase given the growing prevalence of obesity. Obesity is a risk factor for a range of postoperative complications including perioperative neurocognitive disorders. However, the mechanisms underlying this vulnerability are not well defined. We hypothesize that obese subjects are more vulnerable to general anaesthesia induced neurotoxicity due to reduced levels of adiponectin. This hypothesis was tested using a murine surgical model in obese and adiponectin knockout mice exposed to the volatile anaesthetic agent sevoflurane.
METHODS
Obese mice were bred by subjecting C57BL/6 mice to a high fat diet. Cognitive function, neuroinflammatory responses and neuronal degeneration were assessed in both obese and lean mice following exposure to 2 h of sevoflurane to confirm sevoflurane-induced neurotoxicity. Thereafter, to confirm the role of adiponectin deficiency in, adiponectin knockout mice were established and exposed to the sevoflurane. Finally, the neuroprotective effects of adiponectin receptor agonist (AdipoRon) were examined.
RESULTS
Sevoflurane triggered significant cognitive dysfunction, neuroinflammatory responses and neuronal degeneration in the obese mice while no significant impact was observed in the lean mice. Similar cognitive dysfunction and neuronal degeneration were also observed in the adiponectin knockout mice after sevoflurane exposure. Administration of AdipoRon partially prevented the deleterious effects of sevoflurane in both obese and adiponectin knockout mice.
CONCLUSIONS
Our findings demonstrate that obese mice are more susceptible to sevoflurane-induced neurotoxicity and cognitive impairment in which adiponectin deficiency is one of the underlying mechanisms. Treatment with adiponectin receptor agonist ameliorates this vulnerability. These findings may have therapeutic implications in reducing the incidence of anaesthesia related neurotoxicity in obese subjects.
背景
鉴于肥胖症的患病率不断上升,预计肥胖患者进行的大型手术数量将会增加。肥胖是一系列术后并发症的一个风险因素,包括围手术期神经认知障碍。然而,其潜在机制尚未明确。我们假设,由于脂联素水平降低,肥胖患者更容易受到全身麻醉诱导的神经毒性影响。该假设通过在肥胖和脂联素敲除小鼠中使用一种手术模型,并将其暴露于挥发性麻醉剂七氟醚中进行了测试。
方法
将 C57BL/6 小鼠置于高脂肪饮食中以培育肥胖小鼠。在肥胖和瘦小鼠中,通过暴露于 2 小时的七氟醚来评估认知功能、神经炎症反应和神经元变性,以确认七氟醚诱导的神经毒性。此后,为了确认脂联素缺乏在其中的作用,建立了脂联素敲除小鼠并将其暴露于七氟醚中。最后,检查了脂联素受体激动剂(AdipoRon)的神经保护作用。
结果
七氟醚在肥胖小鼠中引发了明显的认知功能障碍、神经炎症反应和神经元变性,而在瘦小鼠中则没有观察到明显的影响。在脂联素敲除小鼠中,七氟醚暴露后也观察到了类似的认知功能障碍和神经元变性。AdipoRon 的给药部分预防了肥胖和脂联素敲除小鼠中七氟醚的有害作用。
结论
我们的研究结果表明,肥胖小鼠对七氟醚诱导的神经毒性和认知障碍更为敏感,而脂联素缺乏是其中的一个潜在机制。脂联素受体激动剂的治疗可改善这种易感性。这些发现可能对减少肥胖患者中与麻醉相关的神经毒性的发生率具有治疗意义。
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