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编码人VEGF165的腺相关病毒载体转导的耻骨肌肌瓣通过在组织工程体内腔室中诱导血管生成增加新组织的形成:一种增强显微外科工程组织中的组织和血管的技术。

AAV vector encoding human VEGF165-transduced pectineus muscular flaps increase the formation of new tissue through induction of angiogenesis in an in vivo chamber for tissue engineering: A technique to enhance tissue and vessels in microsurgically engineered tissue.

作者信息

Moimas Silvia, Manasseri Benedetto, Cuccia Giuseppe, Stagno d'Alcontres Francesco, Geuna Stefano, Pattarini Lucia, Zentilin Lorena, Giacca Mauro, Colonna Michele R

机构信息

Molecular Medicine Laboratory, International Centre for Genetic Engineering and Biotechnology (ICGEB), Trieste, Italy; Department of Medical Sciences, Faculty of Medicine, University of Trieste, Trieste, Italy.

Plastic Surgery Unit, Niguarda Ca' Granda Hospital, Milan, Italy.

出版信息

J Tissue Eng. 2015 Dec 7;6:2041731415611717. doi: 10.1177/2041731415611717. eCollection 2015 Jan-Dec.

Abstract

In regenerative medicine, new approaches are required for the creation of tissue substitutes, and the interplay between different research areas, such as tissue engineering, microsurgery and gene therapy, is mandatory. In this article, we report a modification of a published model of tissue engineering, based on an arterio-venous loop enveloped in a cross-linked collagen-glycosaminoglycan template, which acts as an isolated chamber for angiogenesis and new tissue formation. In order to foster tissue formation within the chamber, which entails on the development of new vessels, we wondered whether we might combine tissue engineering with a gene therapy approach. Based on the well-described tropism of adeno-associated viral vectors for post-mitotic tissues, a muscular flap was harvested from the pectineus muscle, inserted into the chamber and transduced by either AAV vector encoding human VEGF165 or AAV vector expressing the reporter gene β-galactosidase, as a control. Histological analysis of the specimens showed that muscle transduction by AAV vector encoding human VEGF165 resulted in enhanced tissue formation, with a significant increase in the number of arterioles within the chamber in comparison with the previously published model. Pectineus muscular flap, transduced by adeno-associated viral vectors, acted as a source of the proangiogenic factor vascular endothelial growth factor, thus inducing a consistent enhancement of vessel growth into the newly formed tissue within the chamber. In conclusion, our present findings combine three different research fields such as microsurgery, tissue engineering and gene therapy, suggesting and showing the feasibility of a mixed approach for regenerative medicine.

摘要

在再生医学中,创建组织替代物需要新方法,不同研究领域(如组织工程、显微外科和基因治疗)之间的相互作用必不可少。在本文中,我们报告了对已发表的组织工程模型的一种改进,该模型基于包裹在交联胶原 - 糖胺聚糖模板中的动静脉环,此模板充当血管生成和新组织形成的隔离腔室。为了促进腔室内的组织形成(这需要新血管的发育),我们想知道是否可以将组织工程与基因治疗方法相结合。基于腺相关病毒载体对有丝分裂后组织的明确嗜性,从耻骨肌获取一块肌瓣,插入腔室并用编码人VEGF165的腺相关病毒载体或表达报告基因β - 半乳糖苷酶的腺相关病毒载体进行转导,作为对照。对标本的组织学分析表明,用编码人VEGF165的腺相关病毒载体转导肌肉导致组织形成增强,与先前发表的模型相比,腔室内小动脉数量显著增加。由腺相关病毒载体转导的耻骨肌肌瓣充当促血管生成因子血管内皮生长因子的来源,从而诱导血管向腔室内新形成的组织生长持续增强。总之,我们目前的研究结果结合了显微外科、组织工程和基因治疗这三个不同的研究领域,表明并展示了再生医学混合方法的可行性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed84/4734212/bf8e578c1eaa/10.1177_2041731415611717-fig1.jpg

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