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同群Ⅰ传入激活长潜伏期抑制性脊髓通路至踝屈肌。

Long-latency, inhibitory spinal pathway to ankle flexors activated by homonymous group 1 afferents.

机构信息

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

Department of Surgery, University of Alberta, Edmonton, Canada; Centre for Neuroscience, University of Alberta, Edmonton, Canada; Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Canada.

出版信息

J Neurophysiol. 2014 Jun 15;111(12):2544-53. doi: 10.1152/jn.00673.2013. Epub 2014 Mar 26.

Abstract

Inhibitory feedback from sensory pathways is important for controlling movement. Here, we characterize, for the first time, a long-latency, inhibitory spinal pathway to ankle flexors that is activated by low-threshold homonymous afferents. To examine this inhibitory pathway in uninjured, healthy participants, we suppressed motor-evoked potentials (MEPs), produced in the tibialis anterior (TA), by a prior stimulation to the homonymous common peroneal nerve (CPN). The TA MEP was suppressed by a triple-pulse stimulation to the CPN, applied 40, 50, and 60 ms earlier and at intensities of 0.5-0.7 times motor threshold (average suppression of test MEP was 33%). Whereas the triple-pulse stimulation was below M-wave and H-reflex threshold, it produced a long-latency inhibition of background muscle activity, approximately 65-115 ms after the CPN stimulation, a time period that overlapped with the test MEP. However, not all of the MEP suppression could be accounted for by this decrease in background muscle activity. Evoked responses from direct activation of the corticospinal tract, at the level of the brain stem or thoracic spinal cord, were also suppressed by low-threshold CPN stimulation. Our findings suggest that low-threshold muscle and cutaneous afferents from the CPN activate a long-latency, homonymous spinal inhibitory pathway to TA motoneurons. We propose that inhibitory feedback from spinal networks, activated by low-threshold homonymous afferents, helps regulate the activation of flexor motoneurons by the corticospinal tract.

摘要

感觉通路的抑制性反馈对于控制运动很重要。在这里,我们首次描述了一种长潜伏期的抑制性脊髓途径,该途径作用于踝关节屈肌,由低阈值同源传入激活。为了在未受伤的健康参与者中研究这种抑制性途径,我们通过对同名腓总神经(CPN)的预先刺激来抑制在前胫骨(TA)中产生的运动诱发电位(MEP)。通过在 40、50 和 60 ms 之前施加强度为 0.5-0.7 倍运动阈值的三脉冲刺激到 CPN,TA 的 MEP 被抑制(测试 MEP 的平均抑制率为 33%)。虽然三脉冲刺激低于 M 波和 H 反射阈值,但它产生了背景肌肉活动的长潜伏期抑制,大约在 CPN 刺激后 65-115 ms,这一时间与测试 MEP 重叠。然而,并非所有的 MEP 抑制都可以通过这种背景肌肉活动的减少来解释。直接在脑干或胸段脊髓激活皮质脊髓束产生的诱发电应也被低阈值 CPN 刺激抑制。我们的发现表明,来自 CPN 的低阈值肌肉和皮肤传入激活了 TA 运动神经元的长潜伏期同源性脊髓抑制途径。我们提出,由低阈值同源传入激活的脊髓网络的抑制性反馈有助于调节皮质脊髓束对屈肌运动神经元的激活。

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