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脊髓中的神经源性疼痛与类固醇合成

Neurogenic pain and steroid synthesis in the spinal cord.

作者信息

Patte-Mensah Christine, Kibaly Cherkaouia, Boudard Domitille, Schaeffer Véronique, Béglé Aurélie, Saredi Simona, Meyer Laurence, Mensah-Nyagan Ayikoe G

机构信息

Institut des Neurosciences Cellulaires et Intégratives-Centre National de la Recherche Scientifique, Université Louis Pasteur, 67084 Strasbourg Cedex, France.

出版信息

J Mol Neurosci. 2006;28(1):17-31. doi: 10.1385/jmn:28:1:17.

Abstract

The spinal cord (SC) is a biosynthetic center for neurosteroids, including pregnenolone (PREG), progesterone (PROG), and 3alpha/5alpha-tetrahydroprogesterone (3alpha/5alpha-THP). In particular, an active form of cytochrome P450 sidechain cleavage (P450scc) has been localized in sensory networks of the rat SC dorsal horn (DH). P450scc is the key enzyme catalyzing the conversion of cholesterol (CHOL) into PREG, the rate-limiting step in the biosynthesis of all classes of steroids. To determine whether neurosteroidogenesis might be involved in the pivotal role played by the DH in nociception, effects of neurogenic pain provoked by sciatic nerve ligature were investigated on P450scc expression, cellular distribution, and activity in the SC. P450scc mRNA concentration was threefold higher in the DH of neuropathic rats than in controls. The nerve ligature also increased the density of P450sccpositive neuronal perykarya and fibers in the ipsilateral DH. Incubation of spinal tissue homogenates with [3H]CHOL revealed that the amount of newly synthesized [3H]PREG from [3H]CHOLwas 80% higher in the DH of neuropathic rats. Radioimmunoassays showed an increase of PREG and 3alpha/5alpha-THP concentrations in neuropathic rat DH. The upregulation of PREG and 3alpha/5alpha-THP biosynthesis might be involved in endogenous mechanisms triggered by neuropathic rats to cope with the chronic pain state. 3alpha/5alpha-THP formation from PREG can also generate PROG, which decreases sensitivity to pain and protects nerve cells against degeneration. Because apoptotic cell death has been demonstrated in the DH during neuropathic pain, activation of neurosteroidogenesis in spinal tissues might also be correlated to the neuroprotective role of steroids in the SC.

摘要

脊髓(SC)是神经甾体的生物合成中心,包括孕烯醇酮(PREG)、孕酮(PROG)和3α/5α-四氢孕酮(3α/5α-THP)。特别是,细胞色素P450侧链裂解酶(P450scc)的一种活性形式已定位在大鼠脊髓背角(DH)的感觉网络中。P450scc是催化胆固醇(CHOL)转化为PREG的关键酶,是所有类固醇生物合成中的限速步骤。为了确定神经甾体生成是否可能参与DH在伤害感受中所起的关键作用,研究了坐骨神经结扎引起的神经源性疼痛对脊髓中P450scc表达、细胞分布和活性的影响。在神经性大鼠的DH中,P450scc mRNA浓度比对照组高两倍。神经结扎还增加了同侧DH中P450scc阳性神经元胞体和纤维的密度。用[3H]CHOL孵育脊髓组织匀浆显示,神经性大鼠DH中从[3H]CHOL新合成的[3H]PREG量高80%。放射免疫分析显示神经性大鼠DH中PREG和3α/5α-THP浓度增加。PREG和3α/5α-THP生物合成的上调可能参与神经性大鼠触发的内源性机制,以应对慢性疼痛状态。PREG生成3α/5α-THP的过程也可以产生PROG,PROG可降低对疼痛的敏感性并保护神经细胞免于退化。因为在神经性疼痛期间已证明DH中有凋亡性细胞死亡,脊髓组织中神经甾体生成的激活也可能与类固醇在脊髓中的神经保护作用相关。

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