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在人类大脑皮层或感觉传入诱发的初级传入纤维去极化(PAD)期间,促进向运动神经元的感觉传递。

Facilitation of sensory transmission to motoneurons during cortical or sensory-evoked primary afferent depolarization (PAD) in humans.

机构信息

Biomedical Engineering, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Canada.

Neuroscience and Mental Health Institute, University of Alberta, Edmonton, Canada.

出版信息

J Physiol. 2023 May;601(10):1897-1924. doi: 10.1113/JP284275. Epub 2023 Mar 27.

Abstract

Sensory and corticospinal tract (CST) pathways activate spinal GABAergic interneurons that have axoaxonic connections onto proprioceptive (Ia) afferents that cause long-lasting depolarizations (termed primary afferent depolarization, PAD). In rodents, sensory-evoked PAD is produced by GABA receptors at nodes of Ranvier in Ia afferents, rather than at presynaptic terminals, and facilitates spike propagation to motoneurons by preventing branch-point failures, rather than causing presynaptic inhibition. We examined in 40 human participants whether putative activation of Ia-PAD by sensory or CST pathways can also facilitate Ia afferent activation of motoneurons via the H-reflex. H-reflexes in several leg muscles were facilitated by prior conditioning from low-threshold proprioceptive, cutaneous or CST pathways, with a similar long-lasting time course (∼200 ms) to phasic PAD measured in rodent Ia afferents. Long trains of cutaneous or proprioceptive afferent conditioning produced longer-lasting facilitation of the H-reflex for up to 2 min, consistent with tonic PAD in rodent Ia afferents mediated by nodal α5-GABA receptors for similar stimulation trains. Facilitation of H-reflexes by this conditioning was likely not mediated by direct facilitation of the motoneurons because isolated stimulation of sensory or CST pathways did not alone facilitate the tonic firing rate of motor units. Furthermore, cutaneous conditioning increased the firing probability of single motor units (motoneurons) during the H-reflex without increasing their firing rate at this time, indicating that the underlying excitatory postsynaptic potential was more probable, but not larger. These results are consistent with sensory and CST pathways activating nodal GABA receptors that reduce intermittent failure of action potentials propagating into Ia afferent branches. KEY POINTS: Controlled execution of posture and movement requires continually adjusted feedback from peripheral sensory pathways, especially those that carry proprioceptive information about body position, movement and effort. It was previously thought that the flow of proprioceptive feedback from Ia afferents was only reduced by GABAergic neurons in the spinal cord that sent axoaxonic projections to the terminal endings of sensory axons (termed GABA neurons). Based on new findings in rodents, we provide complementary evidence in humans to suggest that sensory and corticospinal pathways known to activate GABA neurons that project to dorsal parts of the Ia afferent also increase the flow of proprioceptive feedback to motoneurons in the spinal cord. These findings support a new role for spinal GABA neurons in facilitating afferent feedback to the spinal cord during voluntary or reflexive movements.

摘要

感觉和皮质脊髓束(CST)通路激活脊髓 GABA 能中间神经元,它们具有轴突轴突连接到本体感受(Ia)传入纤维上,导致持久的去极化(称为初级传入去极化,PAD)。在啮齿动物中,感觉诱发的 PAD 是由 Ia 传入纤维的郎飞结处的 GABA 受体产生的,而不是在突触前末端产生的,并且通过防止分支点故障来促进尖峰向运动神经元的传播,而不是引起突触前抑制。我们在 40 名人类参与者中检查了感觉或 CST 通路对 Ia-PAD 的假定激活是否也可以通过 H 反射促进 Ia 传入纤维对运动神经元的激活。通过低阈值本体感受、皮肤或 CST 通路的先前条件作用,几个腿部肌肉的 H 反射得到了促进,其持续时间(约 200ms)与在啮齿动物 Ia 传入纤维中测量的相同时相 PAD 相似。较长时间的皮肤或本体感受传入纤维的条件作用产生了长达 2 分钟的 H 反射的更长时间的易化,这与由类似刺激的郎飞结处的α5-GABA 受体介导的啮齿动物 Ia 传入纤维中的紧张性 PAD 一致。这种条件作用对 H 反射的易化可能不是通过直接易化运动神经元来介导的,因为单独刺激感觉或 CST 通路本身并不能促进运动单位的紧张性放电率。此外,皮肤条件作用增加了 H 反射期间单个运动单位(运动神经元)的放电概率,而此时它们的放电率没有增加,这表明基础兴奋性突触后电位更有可能,但不一定更大。这些结果与感觉和 CST 通路激活郎飞结处的 GABA 受体一致,这些受体减少了沿 Ia 传入纤维传播的动作电位间歇性失败。关键点:姿势和运动的受控执行需要不断调整来自外周感觉通路的反馈,特别是那些携带有关身体位置、运动和努力的本体感受信息的通路。以前认为,来自 Ia 传入纤维的本体感受反馈的流动仅被脊髓中发送轴突轴突投射到感觉轴突末端的 GABA 神经元减少(称为 GABA 神经元)。基于在啮齿动物中的新发现,我们在人类中提供了补充证据,表明已知激活投射到 Ia 传入纤维背侧部分的 GABA 神经元的感觉和皮质脊髓束也增加了向脊髓运动神经元的本体感受反馈。这些发现支持脊髓 GABA 神经元在自主或反射运动期间促进传入反馈到脊髓中的新作用。

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