Protecting the Nerve Coaptation: Connector-Assisted Nerve Repair in Complex Injuries

Q3 Medicine
Nesreen Zoghoul Alsmadi PhD , Curt Deister PhD , Peter Evans MD, PhD , Tamer Ghanem MD, PhD , Brandon Smetana MD , Deana Mercer MD
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Abstract

Purpose

This study evaluated differences in outcomes of peripheral nerve repair using connector-assisted repair (CAR) or direct repair (DR) in an injured soft tissue bed.

Methods

The sciatic nerve of the right leg in 20 male Lewis rats was exposed and transected. We simulated a traumatized wound bed by cauterizing the underlying muscle bed with a bipolar coagulator. Nerves were repaired with either DR or CAR using porcine small intestine submucosa conduits. At 6 weeks, adhesions were assessed semiquantitiatively, and the gastrocnemius wet muscle weight of each hind limb was recorded to evaluate muscle atrophy. Histology of the nerve was evaluated immediately distal to the nerve repair site. Data were analyzed for differences between repair methods.

Results

The DR group had a considerably higher area of foamy phagocytes and CD68-stained macrophages than that of the CAR group. There were considerably more blood vessels and axons in the CAR group than in the DR group. There were no differences between DR and CAR with respect to gastrocnemius muscle wet weight, extraneural adhesions, or intraneural collagen-to-cell ratio.

Conclusions

There was less area occupied by macrophages and foamy phagocytes in the CAR group, which was indicative of lower inflammatory response and resolving Wallerian degeneration. The CAR group also had more blood vessels and axons compared to that of the DR group, indicating more robust nerve regeneration. Gastrocnemius muscle weight between groups was similar, indicating that nerve regeneration was incomplete in both groups at the 6-week timepoint. These results highlight the potential benefits of CAR in protecting the nerve during the healing process.

Clinical relevance

This in vivo study evaluates histological changes in peripheral nerves during regeneration following transection with either CAR or DR.
保护神经适应:神经连接辅助修复复杂损伤
目的:本研究评估神经连接辅助修复(CAR)和直接修复(DR)在损伤软组织床上修复周围神经的效果差异。方法对20只雄性Lewis大鼠右腿坐骨神经进行暴露和横断。我们通过用双极凝固器烧灼下面的肌肉床来模拟创伤的伤口床。采用猪小肠粘膜下导管行DR或CAR修复神经。6周时,半定量评估粘连情况,记录各后肢腓肠肌湿肌重量,评估肌肉萎缩情况。神经组织学立即评估远端神经修复部位。分析不同修复方法的数据差异。结果DR组泡沫吞噬细胞和cd68染色巨噬细胞面积明显高于CAR组。CAR组血管和轴突明显多于DR组。DR和CAR在腓肠肌湿重、神经外粘连或神经内胶原细胞比方面没有差异。结论CAR组巨噬细胞和泡沫吞噬细胞占据的面积更小,炎症反应较低,可缓解沃勒氏变性。与DR组相比,CAR组也有更多的血管和轴突,表明神经再生更强劲。两组腓肠肌重量相近,提示在6周时两组腓肠肌神经再生不完全。这些结果强调了CAR在愈合过程中保护神经的潜在益处。该体内研究评估了CAR或DR横断再生过程中周围神经的组织学变化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
1.10
自引率
0.00%
发文量
111
审稿时长
12 weeks
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