Microtubule-Stabilizer Epothilone B Delays Anesthetic-Induced Unconsciousness in Rats.

IF 2.7 3区 医学 Q3 NEUROSCIENCES
eNeuro Pub Date : 2024-08-29 Print Date: 2024-08-01 DOI:10.1523/ENEURO.0291-24.2024
Sana Khan, Yixiang Huang, Derin Timuçin, Shantelle Bailey, Sophia Lee, Jessica Lopes, Emeline Gaunce, Jasmine Mosberger, Michelle Zhan, Bothina Abdelrahman, Xiran Zeng, Michael C Wiest
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Abstract

Volatile anesthetics are currently believed to cause unconsciousness by acting on one or more molecular targets including neural ion channels, receptors, mitochondria, synaptic proteins, and cytoskeletal proteins. Anesthetic gases including isoflurane bind to cytoskeletal microtubules (MTs) and dampen their quantum optical effects, potentially contributing to causing unconsciousness. This possibility is supported by the finding that taxane chemotherapy consisting of MT-stabilizing drugs reduces the effectiveness of anesthesia during surgery in human cancer patients. In order to experimentally assess the contribution of MTs as functionally relevant targets of volatile anesthetics, we measured latencies to loss of righting reflex (LORR) under 4% isoflurane in male rats injected subcutaneously with vehicle or 0.75 mg/kg of the brain-penetrant MT-stabilizing drug epothilone B (epoB). EpoB-treated rats took an average of 69 s longer to become unconscious as measured by latency to LORR. This was a statistically significant difference corresponding to a standardized mean difference (Cohen's d) of 1.9, indicating a "large" normalized effect size. The effect could not be accounted for by tolerance from repeated exposure to isoflurane. Our results suggest that binding of the anesthetic gas isoflurane to MTs causes unconsciousness and loss of purposeful behavior in rats (and presumably humans and other animals). This finding is predicted by models that posit consciousness as a property of a quantum physical state of neural MTs.

微管稳定剂埃博霉素 B 能延缓麻醉剂引起的大鼠昏迷。
目前认为,挥发性麻醉剂通过作用于一个或多个分子靶点(包括神经离子通道、受体、线粒体、突触蛋白和细胞骨架蛋白)而导致昏迷。包括异氟醚在内的麻醉气体会与细胞骨架微管(MTs)结合,抑制其量子光学效应,从而可能导致昏迷。由微管稳定药物组成的紫杉类化疗降低了人类癌症患者手术过程中的麻醉效果,这一发现支持了这种可能性。为了在实验中评估 MTs 作为挥发性麻醉剂功能相关靶点的贡献,我们测量了雄性大鼠在 4% 异氟醚条件下右侧反射丧失(LORR)的潜伏期,皮下注射了载体或 0.75 mg/kg 的脑穿透性微管稳定药物埃博霉素 B(epoB)。根据 LORR 的潜伏期来衡量,接受过 EpoB 治疗的大鼠昏迷时间平均延长了 69 秒。这一差异在统计学上具有显著性,其标准化平均差异(Cohen's d)为 1.9,表明归一化效应大小为 "大"。反复接触异氟醚产生的耐受性无法解释这种效应。我们的研究结果表明,麻醉气体异氟醚与微管的结合会导致大鼠(可能也包括人类和其他动物)失去知觉并丧失有目的的行为。我们的研究证实,对细胞内微管的作用是吸入性麻醉气体异氟醚诱导大鼠失去知觉的机制或机制之一。这一发现具有潜在的临床意义,有助于了解紫杉类化疗如何干扰人体麻醉,更广泛地说,有助于避免手术过程中的麻醉失败。我们的研究结果还具有重要的理论意义,因为它们为基于微管的麻醉作用和意识理论提供了支持。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
eNeuro
eNeuro Neuroscience-General Neuroscience
CiteScore
5.00
自引率
2.90%
发文量
486
审稿时长
16 weeks
期刊介绍: An open-access journal from the Society for Neuroscience, eNeuro publishes high-quality, broad-based, peer-reviewed research focused solely on the field of neuroscience. eNeuro embodies an emerging scientific vision that offers a new experience for authors and readers, all in support of the Society’s mission to advance understanding of the brain and nervous system.
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