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本文引用的文献

1
Orthopedic gene therapy--lost in translation?骨科基因治疗——陷入困境?
J Cell Physiol. 2012 Feb;227(2):416-20. doi: 10.1002/jcp.23031.
2
Animal models for translational research on shoulder pathologies: from bench to bedside.肩部疾病转化研究的动物模型:从实验台到病床边
Sports Med Arthrosc Rev. 2011 Sep;19(3):184-93. doi: 10.1097/JSA.0b013e318205470e.
3
Barriers to the clinical translation of orthopedic tissue engineering.骨科组织工程临床转化的障碍。
Tissue Eng Part B Rev. 2011 Dec;17(6):437-41. doi: 10.1089/ten.TEB.2011.0228. Epub 2011 Aug 8.
4
What are the validated animal models for tendinopathy?有哪些经过验证的腱病动物模型?
Scand J Med Sci Sports. 2011 Feb;21(1):3-17. doi: 10.1111/j.1600-0838.2010.01164.x.
5
Accelerated Achilles tendon healing by PDGF gene delivery with mesoporous silica nanoparticles.通过介孔硅纳米粒子传递 PDGF 基因加速跟腱愈合。
Biomaterials. 2010 Jul;31(19):5237-45. doi: 10.1016/j.biomaterials.2010.02.077. Epub 2010 Mar 23.
6
Use of genetically modified muscle and fat grafts to repair defects in bone and cartilage.利用基因修饰的肌肉和脂肪移植物修复骨和软骨的缺陷。
Eur Cell Mater. 2009 Dec 31;18:96-111. doi: 10.22203/ecm.v018a09.
7
Acute ruptures of the achilles tendon.跟腱急性断裂
Sports Med Arthrosc Rev. 2009 Jun;17(2):127-38. doi: 10.1097/JSA.0b013e3181a3d767.
8
Effects of transforming growth factor-beta1 and vascular endothelial growth factor 165 gene transfer on Achilles tendon healing.转化生长因子-β1和血管内皮生长因子165基因转染对跟腱愈合的影响
Matrix Biol. 2009 Jul;28(6):324-35. doi: 10.1016/j.matbio.2009.04.007. Epub 2009 Apr 21.
9
Horse bone marrow mesenchymal stem cells express embryo stem cell markers and show the ability for tenogenic differentiation by in vitro exposure to BMP-12.马骨髓间充质干细胞表达胚胎干细胞标志物,并通过体外暴露于BMP-12显示出向肌腱分化的能力。
BMC Cell Biol. 2009 Apr 22;10:29. doi: 10.1186/1471-2121-10-29.
10
Mesenchymal stem cells and insulin-like growth factor-I gene-enhanced mesenchymal stem cells improve structural aspects of healing in equine flexor digitorum superficialis tendons.间充质干细胞和胰岛素样生长因子-I基因增强的间充质干细胞可改善马浅屈肌腱愈合的结构方面。
J Orthop Res. 2009 Oct;27(10):1392-8. doi: 10.1002/jor.20887.

利用转染 TGF-β1 cDNA 的肌移植物改善肌腱修复。

Improvement of tendon repair using muscle grafts transduced with TGF-β1 cDNA.

机构信息

Orthopädische Klinik, Universität Basel, Basel, Switzerland.

出版信息

Eur Cell Mater. 2012 Feb 16;23:94-101; discussion 101-2. doi: 10.22203/ecm.v023a07.

DOI:10.22203/ecm.v023a07
PMID:22354460
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4339190/
Abstract

Tendon rupture is a common injury. Inadequate endogenous repair often leaves patients symptomatic, with tendons susceptible to re-rupture. Administration of certain growth factors improves tendon healing in animal models, but their delivery remains a challenge. Here we evaluated the delivery of TGF-β1 to tendon defects by the implantation of genetically modified muscle grafts. Rat muscle biopsies were transduced with recombinant adenovirus encoding TGF-β1 and grafted onto surgically transected Achilles tendons in recipient animals. Tissue regenerates were compared to those of controls by biomechanical testing as well as histochemical and immunohistochemical analyses. Healing was greatly accelerated when genetically modified grafts were implanted into tendon defects, with the resulting repair tissue gaining nearly normal histological appearance as early as 2 weeks postoperatively. This was associated with decreased deposition of type III collagen in favour of large fibre bundles indicative of type I collagen. These differences in tendon composition coincided with accelerated restoration of mechanical strength. Tendon thickness increased in gene-treated animals at weeks 1 and 2, but by week 8 became significantly lower than that of controls suggesting accelerated remodelling. Thus localised TGF-β1 delivery via adenovirus-modified muscle grafts improved tendon healing in this rat model and holds promise for clinical application.

摘要

肌腱断裂是一种常见的损伤。内源性修复不足常使患者出现症状,使肌腱容易再次断裂。在动物模型中,某些生长因子的给药可改善肌腱愈合,但它们的传递仍然是一个挑战。在这里,我们通过植入基因修饰的肌肉移植物来评估 TGF-β1 对肌腱缺损的传递。将编码 TGF-β1 的重组腺病毒转导到大鼠肌肉活检中,并将其移植到接受动物的手术横断的跟腱上。通过生物力学测试以及组织化学和免疫组织化学分析,将组织再生与对照进行比较。当将基因修饰的移植物植入肌腱缺损时,愈合大大加速,术后 2 周即可获得几乎正常的组织学外观的修复组织。这与 III 型胶原的沉积减少有关,有利于指示 I 型胶原的大纤维束。这些在肌腱组成上的差异与机械强度的恢复加速相一致。在基因治疗动物中,肌腱厚度在第 1 周和第 2 周增加,但到第 8 周时明显低于对照组,表明加速重塑。因此,通过腺病毒修饰的肌肉移植物局部递送 TGF-β1 可改善该大鼠模型中的肌腱愈合,并有望在临床上应用。