脱细胞神经移植物的血管生成和轴突伸长依赖于周围血管环境。

Kaguna Tanimoto, Akira Kodama, Atsushi Kunisaki, Masaru Munemori, Naosuke Kamei, Nobuo Adachi
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摘要

背景:去细胞神经移植治疗周围神经损伤的疗效有限。在这项研究中,我们验证了一个假设,即通过周围的血流环境增加去细胞化神经的血液循环可以促进神经再生。方法:将20 mm脱细胞神经移植到雌性大鼠(12周龄)坐骨神经缺损中。肌内注射组将脱细胞神经植入股二头肌内,覆盖于股二头肌外,提供血液循环。无血管组将脱细胞神经与坐骨神经缝合,烧灼周围的神经床,形成一个不出血的野。在肌内不修复组,脱细胞神经植入股二头肌,但不与坐骨神经缝合。3周后,采用矢状面和横切面抗神经丝、抗s100和抗cd31抗体免疫组织化学方法评估轴突伸长和血管生成。结果:肌内注射组单位面积神经丝数及S100均高于其他各组(p < 0.05)。肌内组以CD31染色为主。神经轴向图像证实了cd31阳性细胞的定位,肌内注射组的去细胞化神经中心发现了阳性细胞。结论:富血管组织包裹脱细胞神经移植物可促进移植物血管生成,防止移植物中枢缺血,从而促进神经再生。
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Angiogenesis and Axonal Elongation in Decellularised Nerve Grafts Depend on the Surrounding Vascular Environment.

Background: Decellularised nerve transplantation has limited therapeutic efficacy for peripheral nerve injuries. In this study, we tested the hypothesis that nerve regeneration can be promoted by increasing blood circulation to the decellularised nerve through the surrounding blood-flow environment. Methods: We transplanted 20 mm decellularised nerves into sciatic nerve defects in Sprague-Dawley rats (female, 12 weeks old). In the intramuscular group, the decellularised nerve was implanted into the biceps femoris muscle and covered with the muscle to provide blood circulation. In the avascular group, the decellularised nerve was sutured to the sciatic nerve and the surrounding nerve bed was cauterised to create a non-bleeding field. In the intramuscular without repair group, the decellularised nerve was implanted in the biceps femoris muscle, but not sutured to the sciatic nerve. Axonal elongation and angiogenesis were evaluated immunohistochemically using anti-neurofilament, anti-S100 and anti-CD31 antibodies in sagittal and transverse sections of the nerve 3 weeks later. Results: In the intramuscular group, the number of neurofilaments per unit area and S100 were higher than those in the other groups (p < 0.05). CD31 staining was predominant in the intramuscular group. Axial images of the nerves confirmed the localisation of CD31-positive cells, and positive cells were found in the centre of the decellularised nerves in the intramuscular group. Conclusions: Decellularised nerve grafts wrapped with vascular-rich tissue promoted nerve regeneration by enhancing angiogenesis in transplanted nerve grafts and preventing ischemia in the centre of the nerve graft.

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