γ1 GABAA Receptors in Spinal Nociceptive Circuits.

IF 4.4 2区 医学 Q1 NEUROSCIENCES
Elena Neumann, Teresa Cramer, Mario A Acuña, Louis Scheurer, Camilla Beccarini, Bernhard Luscher, Hendrik Wildner, Hanns Ulrich Zeilhofer
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Abstract

GABAergic neurons and GABAA receptors (GABAARs) are critical elements of almost all neuronal circuits. Most GABAARs of the CNS are heteropentameric ion channels composed of two α, two β, and one γ subunits. These receptors serve as important drug targets for benzodiazepine (BDZ) site agonists, which potentiate the action of GABA at GABAARs. Most GABAAR classifications rely on the heterogeneity of the α subunit (α1-α6) included in the receptor complex. Heterogeneity of the γ subunits (γ1-γ3), which mediate synaptic clustering of GABAARs and contribute, together with α subunits, to the benzodiazepine (BDZ) binding site, has gained less attention, mainly because γ2 subunits greatly outnumber the other γ subunits in most brain regions. Here, we have investigated a potential role of non-γ2 GABAARs in neural circuits of the spinal dorsal horn, a key site of nociceptive processing. Female and male mice were studied. We demonstrate that besides γ2 subunits, γ1 subunits are significantly expressed in the spinal dorsal horn, especially in its superficial layers. Unlike global γ2 subunit deletion, which is lethal, spinal cord-specific loss of γ2 subunits was well tolerated. GABAAR clustering in the superficial dorsal horn remained largely unaffected and antihyperalgesic actions of HZ-166, a nonsedative BDZ site agonist, were partially retained. Our results thus suggest that the superficial dorsal horn harbors functionally relevant amounts of γ1 subunits that support the synaptic clustering of GABAARs in this site. They further suggest that γ1 containing GABAARs contribute to the spinal control of nociceptive information flow.

脊髓痛觉回路中的γ1 GABAA受体
GABA 能神经元和 GABAA 受体(GABAAR)是几乎所有神经元回路的关键要素。中枢神经系统中的大多数 GABAAR 都是由两个 α、两个 β 和一个 γ 亚基组成的异五聚体离子通道。这些受体是苯并二氮杂卓(BDZ)部位激动剂的重要药物靶点,BDZ 可增强 GABA 在 GABAARs 上的作用。大多数 GABAAR 的分类依赖于受体复合物中包含的 α 亚基(α1 - α6)的异质性。γ亚基(γ1 - γ3)介导 GABAARs 的突触集群,并与α亚基一起构成苯并二氮杂卓(BDZ)的结合位点,但γ亚基的异质性较少受到关注,这主要是因为在大多数脑区,γ2 亚基的数量大大超过其他γ亚基。在这里,我们研究了非γ2 GABAARs 在脊髓背角神经回路中的潜在作用,脊髓背角是痛觉处理的关键部位。研究对象为雌性和雄性小鼠。我们证明,除了γ2亚基外,γ1亚基在脊髓背角也有显著表达,尤其是在其浅层。与致死性的全局性γ2亚基缺失不同,脊髓特异性γ2亚基缺失具有良好的耐受性。背角浅层的 GABAAR 聚集基本未受影响,非镇静性 BDZ 位点激动剂 HZ-166 的抗过痛作用也得到了部分保留。因此,我们的研究结果表明,背角浅层藏有功能相关的γ1亚基,它们支持 GABAARs 在该部位的突触集群。意义声明 我们的研究结果首次发现了一个中枢神经系统区域(脊髓背角),其中含有γ1亚基的非典型GABAA受体在GABAA受体的突触集群中发挥着生理作用。他们还表明,通过一种非镇静性 GABAA 受体调节剂对 γ1 GABAA 受体进行药理调节,可减轻神经病理性小鼠的慢性疼痛。
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来源期刊
Journal of Neuroscience
Journal of Neuroscience 医学-神经科学
CiteScore
9.30
自引率
3.80%
发文量
1164
审稿时长
12 months
期刊介绍: JNeurosci (ISSN 0270-6474) is an official journal of the Society for Neuroscience. It is published weekly by the Society, fifty weeks a year, one volume a year. JNeurosci publishes papers on a broad range of topics of general interest to those working on the nervous system. Authors now have an Open Choice option for their published articles
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