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通过表达 BDNF、CNTF 或 NT3 的施万细胞的周围神经移植物进行轴突再生的免疫组织化学、超微结构和功能分析。

Immunohistochemical, ultrastructural and functional analysis of axonal regeneration through peripheral nerve grafts containing Schwann cells expressing BDNF, CNTF or NT3.

机构信息

School of Anatomy, Physiology and Human Biology, The University of Western Australia, Crawley, Western Australia, Australia.

出版信息

PLoS One. 2013 Aug 9;8(8):e69987. doi: 10.1371/journal.pone.0069987. eCollection 2013.

Abstract

We used morphological, immunohistochemical and functional assessments to determine the impact of genetically-modified peripheral nerve (PN) grafts on axonal regeneration after injury. Grafts were assembled from acellular nerve sheaths repopulated ex vivo with Schwann cells (SCs) modified to express brain-derived neurotrophic factor (BDNF), a secretable form of ciliary neurotrophic factor (CNTF), or neurotrophin-3 (NT3). Grafts were used to repair unilateral 1 cm defects in rat peroneal nerves and 10 weeks later outcomes were compared to normal nerves and various controls: autografts, acellular grafts and grafts with unmodified SCs. The number of regenerated βIII-Tubulin positive axons was similar in all grafts with the exception of CNTF, which contained the fewest immunostained axons. There were significantly lower fiber counts in acellular, untransduced SC and NT3 groups using a PanNF antibody, suggesting a paucity of large caliber axons. In addition, NT3 grafts contained the greatest number of sensory fibres, identified with either IB4 or CGRP markers. Examination of semi- and ultra-thin sections revealed heterogeneous graft morphologies, particularly in BDNF and NT3 grafts in which the fascicular organization was pronounced. Unmyelinated axons were loosely organized in numerous Remak bundles in NT3 grafts, while the BDNF graft group displayed the lowest ratio of umyelinated to myelinated axons. Gait analysis revealed that stance width was increased in rats with CNTF and NT3 grafts, and step length involving the injured left hindlimb was significantly greater in NT3 grafted rats, suggesting enhanced sensory sensitivity in these animals. In summary, the selective expression of BDNF, CNTF or NT3 by genetically modified SCs had differential effects on PN graft morphology, the number and type of regenerating axons, myelination, and locomotor function.

摘要

我们使用形态学、免疫组织化学和功能评估来确定基因修饰的周围神经(PN)移植物对损伤后轴突再生的影响。移植物由去细胞神经鞘组装而成,这些神经鞘在体外重新填充了表达脑源性神经营养因子(BDNF)的施万细胞(SCs),BDNF 是一种可分泌的睫状神经营养因子(CNTF)或神经营养因子-3(NT3)形式。移植物用于修复大鼠腓神经 1cm 的单侧缺损,10 周后将结果与正常神经和各种对照进行比较:自体移植物、去细胞移植物和未修饰的 SC 移植物。除 CNTF 外,所有移植物中再生的βIII-微管蛋白阳性轴突数量相似,CNTF 中免疫染色的轴突最少。使用 PanNF 抗体,在去细胞、未转导的 SC 和 NT3 组中纤维计数明显较低,提示大口径轴突较少。此外,NT3 移植物含有最多的感觉纤维,用 IB4 或 CGRP 标记物识别。半薄和超薄切片检查显示移植物形态存在明显的异质性,特别是在 BDNF 和 NT3 移植物中,束状组织明显。NT3 移植物中的无髓轴突松散地组织在许多 Remak 束中,而 BDNF 移植物组显示无髓和有髓轴突的比例最低。步态分析显示,在 CNTF 和 NT3 移植物的大鼠中,支撑宽度增加,NT3 移植物大鼠的左后肢受伤的步幅明显更大,这表明这些动物的感觉敏感性增强。总之,基因修饰的 SC 中 BDNF、CNTF 或 NT3 的选择性表达对 PN 移植物形态、再生轴突的数量和类型、髓鞘形成和运动功能有不同的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ac0d/3739754/263a15daad03/pone.0069987.g001.jpg

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