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持续的炎症改变了大鼠皮肤 DRG 神经元亚群中电压激活钙通道的密度和分布。

Persistent inflammation alters the density and distribution of voltage-activated calcium channels in subpopulations of rat cutaneous DRG neurons.

机构信息

Department of Medicine, Division of Gastroenterology, Hepatology and Nutrition, University of Pittsburgh, Pittsburgh, PA 15213, USA Department of Neurobiology, University of Pittsburgh, Pittsburgh, PA 15213, USA The Pittsburgh Center for Pain Research, University of Pittsburgh, Pittsburgh, PA 15213, USA Department of Anesthesiology & Perioperative Care, School of Medicine, University of California, Irvine, CA 92697, USA.

出版信息

Pain. 2010 Dec;151(3):633-643. doi: 10.1016/j.pain.2010.08.030. Epub 2010 Sep 29.

Abstract

The impact of persistent inflammation on voltage-activated Ca(2+) channels in cutaneous DRG neurons from adult rats was assessed with whole cell patch clamp techniques, sqRT-PCR and Western blot analysis. Inflammation was induced with a subcutaneous injection of complete Freund's adjuvant (CFA). DiI was used to identify DRG neurons innervating the site of inflammation. Three days after CFA injection, high threshold Ca(2+) current (HVA) density was significantly reduced in small and medium, but not large diameter neurons, reflecting a decrease in N-, L- and P/Q-type currents. This decrease in HVA current was associated with an increase in mRNA encoding the α2δ1-subunit complex, but no detectable change in N-type subunit (Ca(V)2.2) mRNA. An increase in both α2δ1 and Ca(V)2.2 protein was detected in the central nerves arising from L4 and L5 ganglia ipsilateral to the site of inflammation. In current clamp experiments on small and medium diameter cutaneous DRG neurons from naïve rats, blocking ∼40% of HVA current with Cd(2+) (5μM), had opposite effects on subpopulations of cutaneous DRG neurons (increasing excitability and action potential duration in some and decreasing excitability in others). The alterations in the density and distribution of voltage-activated Ca(2+) channels in subpopulations of cutaneous DRG neurons that develop following CFA injection should contribute to changes in sensory transmission observed in the presence of inflammation.

摘要

使用全细胞膜片钳技术、sqRT-PCR 和 Western blot 分析评估了持续性炎症对成年大鼠皮肤 DRG 神经元电压激活 Ca(2+)通道的影响。通过皮下注射完全弗氏佐剂 (CFA) 诱导炎症。DiI 用于识别支配炎症部位的 DRG 神经元。在 CFA 注射后 3 天,小和中直径神经元的高阈值 Ca(2+)电流 (HVA) 密度显着降低,反映出 N-、L- 和 P/Q 型电流减少。这种 HVA 电流的减少与编码 α2δ1-亚基复合物的 mRNA 增加有关,但 N 型亚基 (Ca(V)2.2) mRNA 没有可检测到的变化。在来自炎症部位同侧 L4 和 L5 神经节的中枢神经中,检测到 α2δ1 和 Ca(V)2.2 蛋白均增加。在来自未处理大鼠的小和中直径皮肤 DRG 神经元的电流钳实验中,用 Cd(2+)(5μM)阻断约 40%的 HVA 电流对皮肤 DRG 神经元亚群具有相反的影响(增加一些神经元的兴奋性和动作电位持续时间,而降低另一些神经元的兴奋性)。在 CFA 注射后发展的皮肤 DRG 神经元亚群中,电压激活 Ca(2+)通道的密度和分布的改变,应该有助于解释在炎症存在时观察到的感觉传递变化。

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