Department of Biochemistry and Molecular Biology, Virginia Commonwealth University School of Medicine, Richmond, Virginia, 23298-0614, USA.
Glia. 2012 Jan;60(1):125-36. doi: 10.1002/glia.21253. Epub 2011 Oct 14.
Although the classical function of myelin is the facilitation of saltatory conduction, this membrane and the oligodendrocytes, the cells that make myelin in the central nervous system (CNS), are now recognized as important regulators of plasticity and remodeling in the developing brain. As such, oligodendrocyte maturation and myelination are among the most vulnerable processes along CNS development. We have shown previously that rat brain myelination is significantly altered by buprenorphine, an opioid analogue currently used in clinical trials for managing pregnant opioid addicts. Perinatal exposure to low levels of this drug induced accelerated and increased expression of myelin basic proteins (MBPs), cellular and myelin components that are markers of mature oligodendrocytes. In contrast, supra-therapeutic drug doses delayed MBP brain expression and resulted in a decreased number of myelinated axons. We have now found that this biphasic-dose response to buprenorphine can be attributed to the participation of both the μ-opioid receptor (MOR) and the nociceptin/orphanin FQ receptor (NOP receptor) in the oligodendrocytes. This is particularly intriguing because the NOP receptor/nociceptin system has been primarily linked to behavior and pain regulation, but a role in CNS development or myelination has not been described before. Our findings suggest that balance between signaling mediated by (a) MOR activation and (b) a novel, yet unidentified pathway that includes the NOP receptor, plays a crucial role in the timing of oligodendrocyte maturation and myelin synthesis. Moreover, exposure to opioids could disrupt the normal interplay between these two systems altering the developmental pattern of brain myelination.
虽然髓鞘的经典功能是促进跳跃式传导,但这种膜和少突胶质细胞(中枢神经系统中产生髓鞘的细胞)现在被认为是发育中大脑可塑性和重塑的重要调节因子。因此,少突胶质细胞成熟和髓鞘形成是中枢神经系统发育过程中最脆弱的过程之一。我们之前已经表明,阿片类药物类似物丁丙诺啡显著改变了大鼠大脑的髓鞘形成,丁丙诺啡目前正在临床试验中用于治疗怀孕的阿片类药物成瘾者。在围产期接触低水平的这种药物会加速和增加髓鞘碱性蛋白(MBP)的表达,MBP 是成熟少突胶质细胞的细胞和髓鞘成分标志物。相比之下,超治疗剂量的药物会延迟 MBP 在大脑中的表达,并导致少突胶质细胞包裹的轴突数量减少。我们现在发现,丁丙诺啡的这种双相剂量反应可以归因于 μ 阿片受体(MOR)和孤啡肽/孤啡肽 FQ 受体(NOP 受体)在少突胶质细胞中的共同参与。这尤其令人感兴趣,因为 NOP 受体/孤啡肽系统主要与行为和疼痛调节有关,但以前没有描述过它在中枢神经系统发育或髓鞘形成中的作用。我们的研究结果表明,(a)MOR 激活介导的信号和(b)包括 NOP 受体在内的尚未确定的新途径之间的信号平衡,在少突胶质细胞成熟和髓鞘合成的时间安排中起着至关重要的作用。此外,接触阿片类药物可能会破坏这两个系统之间的正常相互作用,改变大脑髓鞘形成的发育模式。