The Burke Medical Research Institute, 785 Mamaroneck Avenue, White Plains, NY 10605, USA.
J Neurotrauma. 2012 Aug 10;29(12):2226-43. doi: 10.1089/neu.2012.2377.
Several recent studies suggest that predegenerated nerves (PDNs) or dissociated PDNs (dPDNs) can improve behavioral and histological outcomes following transplantation into the injured rat spinal cord. In the current study we tested the efficacy of dPDN transplantation by grafting cells isolated from the sciatic nerve 7 days after crush. We did not replicate one study, but rather assessed what appeared, based on five published reports, to be a reported robust effect of dPDN grafts on corticospinal tract (CST) regeneration and locomotor recovery. Using a standardized rodent spinal cord injury model (200 kD IH contusion) and transplantation procedure (injection of GFP⁺ cells 7 days post-SCI), we demonstrate that dPDN grafts survive within the injured spinal cord and promote the ingrowth of axons to a similar extent as purified Schwann cell (SC) grafts. We also demonstrate for the first time that while both dPDN and SC grafts promote the ingrowth of CGRP axons, neither graft results in mechanical or thermal hyperalgesia. Unlike previous studies, dPDN grafts did not promote long-distance axonal growth of CST axons, brainstem spinal axons, or ascending dorsal column sensory axons. Moreover, using a battery of locomotor tests (Basso Beattie Bresnahan [BBB] score, BBB subscore, inked footprint, Catwalk, and ladderwalk), we failed to detect any beneficial effects of dPDN transplantation on the recovery of locomotor function after SCI. We conclude that dPDN transplants are not sufficient to promote CST regeneration or locomotor recovery after SCI.
几项最近的研究表明,预变性神经(PDN)或分离的 PDN(dPDN)可以改善损伤大鼠脊髓移植后的行为和组织学结果。在本研究中,我们通过移植损伤后 7 天从坐骨神经分离的细胞来测试 dPDN 移植的疗效。我们没有复制一项研究,而是根据五项已发表的报告评估了 dPDN 移植物对皮质脊髓束(CST)再生和运动功能恢复的所谓显著作用。使用标准化的啮齿动物脊髓损伤模型(200 kD IH 挫伤)和移植程序(SCI 后 7 天注射 GFP⁺细胞),我们证明 dPDN 移植物在损伤的脊髓内存活,并促进轴突的生长程度与纯化的 Schwann 细胞(SC)移植物相似。我们还首次证明,虽然 dPDN 和 SC 移植物都促进 CGRP 轴突的生长,但两者都不会导致机械或热痛觉过敏。与之前的研究不同,dPDN 移植物不会促进 CST 轴突、脑干脊髓轴突或上升的背柱感觉轴突的远距离轴突生长。此外,使用一系列运动测试(Basso Beattie Bresnahan [BBB] 评分、BBB 子评分、墨迹足迹、Catwalk 和 ladderwalk),我们未能检测到 dPDN 移植对 SCI 后运动功能恢复的任何有益影响。我们得出结论,dPDN 移植物不足以促进 SCI 后 CST 再生或运动功能恢复。