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L-NAME处理大鼠肌腱愈合过程中胶原束的组织形态

Organization of collagen bundles during tendon healing in rats treated with L-NAME.

作者信息

Tomiosso Tatiana Carla, Nakagaki Wilson Romero, Gomes Laurecir, Hyslop Stephen, Pimentel Edson Rosa

机构信息

Department of Anatomy, Cell Biology, Physiology and Biophysics, Institute of Biology, State University of Campinas, UNICAMP, SP, Brazil.

出版信息

Cell Tissue Res. 2009 Aug;337(2):235-42. doi: 10.1007/s00441-009-0819-5. Epub 2009 Jun 9.

Abstract

The Achilles tendon can support high tension forces and may experience lesions. The damaged tissue does not regenerate completely, with the organization and mechanical properties of the repaired tendon being inferior to those of a healthy tendon. Nitric oxide (NO) plays an important role in wound repair. We have examined the structural reorganization and repair in Achilles tendon after injury in rats treated with the NO synthase inhibitor L-NAME. The right Achilles tendon of male Wistar rats was partially transected. One group of rats was treated with L-NAME (~300 mg/kg per day, given in drinking water) for 4 days prior to tendon sectioning and throughout the post-operative period. Control rats received water without L-NAME. The tendons were excised at 7, 14, and 21 days post-injury and used to quantify hydroxyproline and for mechanical tests. Tendons were also processed for histomorphological analysis by polarized light microscopy, which showed that the collagen fibers were disorganized by day 7 in non-treated and L-NAME-treated rats. In non-treated rats, the organization of the extracellular matrix was more homogeneous by days 14 and 21 compared with day 7, although this homogeneity was less than that in normal tendon. In contrast, in injured tendons from L-NAME-treated rats, the collagen fibers were still disorganized on day 21. Tendons from treated rats had more hydroxyproline but lower mechanical properties compared with those from non-treated rats. Thus, NO modulates tendon healing, with a reduction in NO biosynthesis delaying reorganization of the extracellular matrix, especially collagen.

摘要

跟腱能够承受高张力,且可能会出现损伤。受损组织无法完全再生,修复后的跟腱在组织结构和力学性能方面均不如健康跟腱。一氧化氮(NO)在伤口修复中起着重要作用。我们研究了用NO合酶抑制剂L-NAME处理的大鼠跟腱损伤后的结构重组和修复情况。雄性Wistar大鼠的右跟腱被部分横断。一组大鼠在肌腱切断术前4天及整个术后期间用L-NAME(约300mg/kg/天,通过饮用水给予)处理。对照大鼠饮用不含L-NAME的水。在损伤后7天、14天和21天切除肌腱,用于定量羟脯氨酸并进行力学测试。肌腱还通过偏振光显微镜进行组织形态学分析,结果显示,在未处理和L-NAME处理的大鼠中,到第7天时胶原纤维已紊乱。在未处理的大鼠中,与第7天相比,在第14天和21天时细胞外基质的组织更均匀,尽管这种均匀性低于正常肌腱。相比之下,在L-NAME处理的大鼠的损伤肌腱中,到第21天时胶原纤维仍然紊乱。与未处理大鼠的肌腱相比,处理过的大鼠的肌腱含有更多的羟脯氨酸,但力学性能更低。因此,NO调节肌腱愈合,NO生物合成的减少会延迟细胞外基质尤其是胶原的重组。

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