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组织工程同种异体椎间盘移植治疗退行性椎间盘疾病:比格犬模型的实验研究。

Tissue-engineered allograft intervertebral disc transplantation for the treatment of degenerative disc disease: experimental study in a beagle model.

机构信息

Department of of Orthopedics and Traumatology, Xijing Hospital, The Fourth Military Medical University, Xi'an, China.

出版信息

Tissue Eng Part A. 2013 Jan;19(1-2):143-51. doi: 10.1089/ten.TEA.2012.0255. Epub 2012 Nov 5.

Abstract

OBJECTIVES

To investigate whether the intervention of nucleus pulposus (NP) cells or human telomerase reverse transcriptase (hTERT) gene-transfected NP cells can prevent the degeneration process after allograft total disc transplantation.

METHODS

Eighteen canine lumbar intervertebral discs were obtained from five canines and cryopreserved in liquid nitrogen. Canine nucleus pulposus cells were isolated and transduced with recombinant adeno-associated virus (rAAV)-hTERT. The cells were injected into the discs to construct a tissue-engineered allograft disc (group A). NP cells and DMEM/F12 were used for positive control (group B) and blank control (group C). 18 beagle dogs received the three groups of allograft intervertebral disc (IVD) composites implantation, respectively. Radiographic examinations were performed at 4, 8, and 12 weeks postimplantation. At 12 weeks after operation, all dogs were sacrificed and the lumbar spines were harvested for the biomechanical analysis, and then the allografts underwent histological analysis, ectogenic NP cell tracing, and hTERT mRNA analysis.

RESULTS

Bony fusion between the intervertebral disc allograft and the adjacent host intervertebral body were observed in all animals. The disc height and T2 signal intensity preservation in group A and B was better than group C. Magnetic resonance images (MRI) showed typical degenerative changes in group C. In group A, the normalized grayscale of the transplanted disc on MRI was significant higher compared with the controls at 12 weeks. A biomechanical test showed a poor stability preservation in group C compared to group A and B. PKH-26-positive cells were identified within the allograft discs in group A at 12 weeks, providing evidence of cell survival. Histological analysis showed the NP cell morphology, cell number, and distribution of the allograft discs was better preserved in group A and B compared to group C at a 12-week follow-up.

CONCLUSION

The present study demonstrated that NP cells or hTERT-loaded NP cells intervention could effectively resist the degeneration of the allogenic transplanted intervertebral discs in a beagle model. The hTERT-loaded NP cells had a better antidegeneration effect on the transplanted disc than NP cells. This modified disc regeneration technique through NP cell injection or manipulation may have the potential to ensure the long-term function preservation of allograft disc transplantation.

摘要

目的

研究髓核细胞(NP)或人端粒酶逆转录酶(hTERT)基因转染 NP 细胞的干预是否能防止同种异体全椎间盘移植后的退变过程。

方法

从 5 只犬中取出 18 个犬腰椎间盘,液氮冷冻保存。分离犬髓核细胞,并用重组腺相关病毒(rAAV)-hTERT 转导。将细胞注入椎间盘构建组织工程同种异体椎间盘(A 组)。NP 细胞和 DMEM/F12 用作阳性对照(B 组)和空白对照(C 组)。分别向 18 只比格犬植入 3 组同种异体椎间盘(IVD)复合物。植入后 4、8、12 周进行影像学检查。术后 12 周,处死所有犬,取腰椎进行生物力学分析,然后对同种异体移植物进行组织学分析、外源性 NP 细胞示踪和 hTERT mRNA 分析。

结果

所有动物均观察到椎间盘同种异体与相邻宿主椎体之间的骨融合。A 组和 B 组的椎间盘高度和 T2 信号强度保持较好,C 组较差。磁共振成像(MRI)显示 C 组有典型的退行性改变。A 组在 MRI 上,12 周时移植椎间盘的归一化灰度值明显高于对照组。生物力学试验显示 C 组的稳定性保持明显差于 A 组和 B 组。A 组在 12 周时,在同种异体椎间盘内鉴定出 PKH-26 阳性细胞,证明细胞存活。组织学分析显示,在 12 周随访时,A 组和 B 组同种异体椎间盘的 NP 细胞形态、细胞数量和分布保存较好,C 组较差。

结论

本研究表明,NP 细胞或负载 hTERT 的 NP 细胞干预可有效抵抗犬同种异体移植椎间盘的退变。负载 hTERT 的 NP 细胞对移植椎间盘的抗退变作用优于 NP 细胞。通过 NP 细胞注射或操作对椎间盘进行改良再生技术,可能有潜力确保同种异体椎间盘移植的长期功能保存。

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