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Are all spinal segments equal: intrinsic membrane properties of superficial dorsal horn neurons in the developing and mature mouse spinal cord

机译:所有的脊柱节段是否相等:发育中和成熟的小鼠脊髓中浅表背角神经元的固有膜特性

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摘要

Neurons in the superficial dorsal horn (SDH; laminae I–II) of the spinal cord process nociceptive information from skin, muscle, joints and viscera. Most of what we know about the intrinsic properties of SDH neurons comes from studies in lumbar segments of the cord even though clinical evidence suggests nociceptive signals from viscera and head and neck tissues are processed differently. This ‘lumbar-centric’ view of spinal pain processing mechanisms also applies to developing SDH neurons. Here we ask whether the intrinsic membrane properties of SDH neurons differ across spinal cord segments in both the developing and mature spinal cord. Whole cell recordings were made from SDH neurons in slices of upper cervical (C2–4), thoracic (T8–10) and lumbar (L3–5) segments in neonatal (P0–5) and adult (P24–45) mice. Neuronal input resistance (RIN), resting membrane potential, AP amplitude, half-width and AHP amplitude were similar across spinal cord regions in both neonates and adults (∼100 neurons for each region and age). In contrast, these intrinsic membrane properties differed dramatically between neonates and adults. Five types of AP discharge were observed during depolarizing current injection. In neonates, single spiking dominated (∼40%) and the proportions of each discharge category did not differ across spinal regions. In adults, initial bursting dominated in each spinal region, but was significantly more prevalent in rostral segments (49% of neurons in C2–4 vs. 29% in L3–5). During development the dominant AP discharge pattern changed from single spiking to initial bursting. The rapid A-type potassium current (IAr) dominated in neonates and adults, but its prevalence decreased (∼80%vs. ∼50% of neurons) in all regions during development. IAr steady state inactivation and activation also changed in upper cervical and lumbar regions during development. Together, our data show the intrinsic properties of SDH neurons are generally conserved in the three spinal cord regions examined in both neonate and adult mice. We propose the conserved intrinsic membrane properties of SDH neurons along the length of the spinal cord cannot explain the marked differences in pain experienced in the limbs, viscera, and head and neck.
机译:脊髓浅背角(SDH;层I–II)中的神经元处理来自皮肤,肌肉,关节和内脏的伤害性信息。尽管临床证据表明,来自内脏和头颈部组织的伤害感受信号处理方式不同,但我们对SDH神经元固有特性的大多数了解都来自于脐带腰段的研究。这种以腰部为中心的脊柱疼痛处理机制的观点也适用于发育中的SDH神经元。在这里,我们要问SDH神经元的内在膜特性在发育中的脊髓和成熟的脊髓中是否在整个脊髓节段上都不同。从SDH神经元在新生儿(P0-5)和成年(P24-45)小鼠的上颈段(C2-4),胸段(T8-10)和腰段(L3-5)的切片中记录全细胞。新生儿和成年人的脊髓区域神经元输入阻力(RIN),静息膜电位,AP振幅,半角和AHP振幅相似(每个区域和年龄约100个神经元)。相反,这些固有的膜特性在新生儿和成年人之间差异很大。在去极化电流注入期间观察到五种类型的AP放电。在新生儿中,单次突触占主导地位(约40%),并且各个放电类别的比例在整个脊柱区域没有差异。在成人中,最初的爆发主要发生在每个脊柱区域,但在鼻端节段中更为普遍(C2-4中的神经元占49%,L3-5中的29%)。在开发过程中,主要的AP放电模式从单尖峰变为初始突波。在新生儿和成人中,快速的A型钾电流(IAr)占主导地位,但在整个发育过程中,其流行率在所有地区均下降(约80%,约占神经元的50%)。在发育过程中,IAr稳态失活和激活在上颈椎和腰椎区域也发生了变化。在一起,我们的数据显示SDH神经元的内在属性通常在新生和成年小鼠中检查的三个脊髓区域中均是保守的。我们提出,SDH神经元沿脊髓长度的保守内在膜特性无法解释四肢,内脏和头颈部疼痛的明显差异。

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