人体局部缺血引起的皮肤传入神经兴奋性指标的变化。
Changes in excitability indices of cutaneous afferents produced by ischaemia in human subjects.
作者信息
Grosskreutz J, Lin C, Mogyoros I, Burke D
机构信息
Department of Neurology, The Prince Henry and Prince of Wales Hospitals, Prince of Wales Medical Research Institute, and University of New South Wales, Sydney, Australia.
出版信息
J Physiol. 1999 Jul 1;518(Pt 1):301-14. doi: 10.1111/j.1469-7793.1999.0301r.x.
Abstract
- The present study was undertaken to determine whether mechanisms other than membrane depolarization contribute to the changes in excitability of cutaneous afferents of the median nerve under ischaemic conditions. 2. In six healthy subjects, axonal excitability was measured as the reciprocal of the threshold for a compound sensory action potential (CSAP) of 50% maximal amplitude. Refractoriness and supernormality were measured as threshold changes 2 and 7 ms, respectively, after supramaximal conditioning stimuli. The strength-duration time constant (tauSD) was calculated from the thresholds for unconditioned CSAPs using test stimuli of 0.1 and 1.0 ms duration. Changes in these indices were measured when subthreshold polarizing currents lasting 10 or 100 ms were applied, before, during and after ischaemia for 13 min. 3. At rest, the change in supernormality produced by polarizing currents was greater with the longer polarizing current, indicating that it took up to 100 ms to charge the internodal capacitance. 4. Refractoriness and its dependence on excitability increased more than expected during ischaemia. Supernormality was abolished during ischaemia, and reached a maximum after ischaemia but was then barely altered by polarizing current. tauSD had a similar relationship to excitability before, during and after ischaemia. 5. By contrast, during continuous depolarizing current for 8 min to mimic the depolarization produced by ischaemia, the relationship between excitability and refractoriness was the same during the depolarization as before it. 6. It is suggested that the large increase in refractoriness during ischaemia might be due to interference with the recovery from inactivation of transient sodium channels by an intra-axonal substrate of ischaemia. The post-ischaemic increase in supernormality and the lack of change with changes in axonal excitability can be explained by blockage of voltage-dependent potassium channels.
摘要
- 本研究旨在确定在缺血条件下,除膜去极化以外的机制是否会导致正中神经皮肤传入纤维兴奋性的变化。2. 在六名健康受试者中,轴突兴奋性通过复合感觉动作电位(CSAP)达到最大幅度50%时阈值的倒数来测量。不应期和超常期分别通过在超强条件刺激后2毫秒和7毫秒时的阈值变化来测量。强度 - 时间常数(tauSD)通过使用持续时间为0.1毫秒和1.0毫秒的测试刺激对未条件化CSAP的阈值来计算。在缺血13分钟之前、期间和之后,当施加持续10或100毫秒的阈下极化电流时,测量这些指标的变化。3. 在静息状态下,极化电流产生的超常期变化在极化电流较长时更大,这表明给节间电容充电需要长达100毫秒。4. 在缺血期间,不应期及其对兴奋性的依赖性增加超过预期。超常期在缺血期间消失,并在缺血后达到最大值,但随后几乎不受极化电流影响。tauSD在缺血之前、期间和之后与兴奋性具有相似的关系。5. 相比之下,在持续8分钟的去极化电流以模拟缺血产生的去极化过程中,去极化期间兴奋性和不应期之间的关系与之前相同。6. 提示缺血期间不应期的大幅增加可能是由于缺血的轴突内底物干扰了瞬时钠通道失活后的恢复。缺血后超常期的增加以及轴突兴奋性变化时缺乏改变可以通过电压依赖性钾通道的阻断来解释。
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