首页> 美国卫生研究院文献>The Journal of Physiology >Experimentally derived model for the locomotor pattern generator in the Xenopus embryo.
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Experimentally derived model for the locomotor pattern generator in the Xenopus embryo.

机译:非洲爪蟾胚胎中运动模式发生器的实验推导模型。

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摘要

1. Simulations of Xenopus embryo spinal neurons were endowed with Hodgkin-Huxley-style models of voltage-dependent Na+, Ca2+, slow K+ and fast K+ currents together with a Na(+)-dependent K+ current. The parameters describing the activation, inactivation and relaxation of these currents were derived from previous voltage-clamp studies of Xenopus embryo spinal neurons. Each of the currents was present at realistic densities. 2. The model neurons fired repetitively in response to current injection. The Ca2+ current was essential for repetitive firing in response to current injection. The fast K+ current appeared mainly to control spike width, whereas the slow K+ current exerted a powerful influence on the reptitive firing properties of the neurons without markedly affecting spike width. 3. The properties of the model neurons could be made more consistent with those previously reported for Xenopus embryo neurons during intracellular recordings in vivo, if the shunting effect of the sharp microelectrode was incorporated into the model. 4. The model neurons were then used to create a simplified version of the spinal network that controls swimming in the frog embryo. This model network could generate the motor pattern for swimming: the activity between the left and right sides alternated with a cycle period that varied from 50 to 120 ms. This is very similar to the range of cycle periods observed in the real embryo. The shunting effect of the microelectrode was once again taken into account. 5. Reductions of the K+ currents perturbed the motor pattern and gave three forms of aberrant motor activity very similar to those previously seen during the application of K+ channel blockers to the real embryo. The ability to generate the correct motor pattern for swimming in the model depended on the balance between the K+ currents and the inward Na+ and Ca2+ currents rather than their absolute values. 6. The model network could generate a motor pattern for swimming over a very wide range of excitatory (2-10 nS) and inhibitory (2-400 nS) synaptic strengths. Rough estimates of the physiological synaptic strengths in the real circuit (around 20-60 nS for inhibition and 2-5 nS for excitation) fall within the range of synaptic strengths that gave simulation of the swimming motor pattern in the model. 7. The cycle period of the motor activity in the model shortened either as the excitatory synapses were strengthened or as the inhibitory synapses were weakened. 8. The prediction that the strength of the mid-cycle inhibition determines cycle period has been tested by using low levels of strychnine to reduce glycinergic reciprocal inhibition in a graded manner in the real embryo. As the inhibition was reduced, the cycle period of fictive swimming in the embryo shortened by amounts very close to those predicted by the model. 9. This new experimentally derived model can replicate many of the known features of fictive swimming in the real embryo and may be of value as an analytical tool in attempting to understand how the spinal circuitry of the Xenopus embryo and related amphibian embryos control a variety of motor behaviours.
机译:1.爪蟾胚胎脊髓神经元的模拟具有电压依赖性Na +,Ca2 +,慢K +和快K +电流以及Na(+)依赖性K +电流的Hodgkin-Huxley型模型。描述这些电流的激活,失活和弛豫的参数来自非洲爪蟾胚胎脊髓神经元先前的电压钳位研究。每种潮流都以现实的密度出现。 2.模型神经元响应于当前的注射而反复发射。 Ca2 +电流对于响应电流注入的反复点火至关重要。快速的K +电流似乎主要是控制尖峰宽度,而缓慢的K +电流对神经元的复制性发射特性产生了强大的影响,而没有明显影响尖峰宽度。 3.如果将尖锐的微电极的分流效应纳入模型,则可以使模型神经元的特性与先前报道的非洲爪蟾胚胎神经元的特性更加一致。 4.然后,使用模型神经元创建简化版本的脊髓网络,以控制青蛙胚胎中的游泳。该模型网络可以生成游泳运动模式:左侧和右侧之间的活动交替变化,周期从50到120毫秒不等。这与真实胚胎中观察到的周期范围非常相似。再次考虑了微电极的分流效应。 5. K +电流的减少扰乱了运动模式,并产生了三种形式的异常运动活动,这与先前在将K +通道阻滞剂应用于真实胚胎时看到的异常运动活动非常相似。在模型中生成正确的运动模式以进行游泳的能力取决于K +电流与内向Na +和Ca2 +电流之间的平衡,而不是其绝对值。 6.模型网络可以生成一种运动模式,用于在非常大的兴奋性(2-10 nS)和抑制性(2-400 nS)突触强度范围内游泳。真实回路中生理突触强度的粗略估计(抑制约20-60 nS,激发约2-5 nS)落在突触强度范围内,该突触强度可以在模型中模拟游泳运动模式。 7.随着兴奋性突触的增强或抑制性突触的减弱,模型中运动活动的周期缩短。 8.已经通过在真实胚胎中使用低浓度的士丁宁来逐步降低甘氨酸能的相互抑制作用,从而验证了中周期抑制强度决定周期的预测。随着抑制作用的降低,假想游泳在胚胎中的循环周期缩短了非常接近模型预测的周期。 9.这个新的实验衍生模型可以在真实胚胎中复制虚构游泳的许多已知特征,并且在试图理解非洲爪蟾胚胎和相关两栖动物胚胎的脊髓回路如何控制各种不同的行为方面可能具有分析价值。运动行为。

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