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通过明胶海绵缓慢释放碱性成纤维细胞生长因子实现气管软骨再生。

Tracheal cartilage regeneration by slow release of basic fibroblast growth factor from a gelatin sponge.

作者信息

Igai Hitoshi, Yamamoto Yasumichi, Chang Sung Soo, Yamamoto Masaya, Tabata Yasuhiko, Yokomise Hiroyasu

机构信息

Second Department of Surgery, Kagawa University, Kita-gun, Kagawa, Japan.

出版信息

J Thorac Cardiovasc Surg. 2007 Jul;134(1):170-5. doi: 10.1016/j.jtcvs.2007.02.022.

Abstract

OBJECTIVE

We investigated whether implantation of a gelatin sponge, releasing basic fibroblast growth factor slowly (b-FGF) into a tracheal cartilage defect, would induce regeneration of autologous tracheal cartilage.

METHODS

We created a 1-cm defect in the midventral portion of each of 10 consecutive cervical tracheal cartilage rings in 12 experimental dogs. In the control group (n = 4), the resulting defects were left untreated. In the gelatin group (n = 4), empty gelatin sponges were implanted in the defects. In the basic fibroblast growth factor group (n = 4), gelatin sponges incorporating 100 microg of b-FGF solution were implanted in the defects. We killed the 4 dogs in each group at 1, 3, 6, and 12 months after implantation, respectively, and examined the implant sites macro- and microscopically.

RESULTS

In the control and gelatin groups, no regenerated cartilage was observed in the tracheal cartilage defects, and the width of the gap between the host cartilage stumps had shrunk. In the b-FGF group, regenerated cartilage was observed in all dogs. The proportion of the defect in the host cartilage occupied by regenerated cartilage was 13%, 84%, 75%, and 69% at 1, 3, 6, and 12 months, respectively. The regenerated cartilage was fibrous cartilage covered with perichondrium, which grew from the host perichondrium and showed continuity with the host cartilage stumps.

CONCLUSIONS

Implantation of a gelatin sponge slowly releasing basic fibroblast growth factor induces tracheal cartilage regeneration, which subsequently fills a large proportion of experimentally created tracheal cartilage defects within 12 months after implantation.

摘要

目的

我们研究了向气管软骨缺损处植入缓慢释放碱性成纤维细胞生长因子(b-FGF)的明胶海绵是否会诱导自体气管软骨再生。

方法

我们在12只实验犬的连续10个颈段气管软骨环的腹中部制造了1厘米的缺损。对照组(n = 4),缺损处不做处理。明胶组(n = 4),向缺损处植入空的明胶海绵。碱性成纤维细胞生长因子组(n = 4),向缺损处植入含100微克b-FGF溶液的明胶海绵。分别在植入后1、3、6和12个月处死每组中的4只犬,并对植入部位进行大体和显微镜检查。

结果

在对照组和明胶组中,气管软骨缺损处未观察到再生软骨,宿主软骨残端之间的间隙宽度缩小。在b-FGF组中,所有犬均观察到再生软骨。再生软骨在1、3、6和12个月时分别占宿主软骨缺损的13%、84%、75%和69%。再生软骨为覆盖有软骨膜的纤维软骨,其从宿主软骨膜生长并与宿主软骨残端相连。

结论

植入缓慢释放碱性成纤维细胞生长因子的明胶海绵可诱导气管软骨再生,随后在植入后12个月内可填充大部分实验性气管软骨缺损。

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