Freitas-Ribeiro Sara, Moreira Helena, da Silva Lucília P, Noro Jennifer, Sampaio-Marques Belém, Ludovico Paula, Jarnalo Mariana, Horta Ricardo, Marques Alexandra P, Reis Rui L, Pirraco Rogério P
3B's Research Group, I3Bs - Research Institute on Biomaterials, Biodegradables and Biomimetics, University of Minho, Headquarters of the European Institute of Excellence on Tissue Engineering and Regenerative Medicine, AvePark, Parque de Ciência e Tecnologia, Zona Industrial da Gandra, 4805-017, Barco, Guimarães, Portugal.
ICVS/3B's-PT Government Associate Laboratory, Braga/Guimarães, Portugal.
Bioact Mater. 2024 Mar 28;37:253-268. doi: 10.1016/j.bioactmat.2024.02.035. eCollection 2024 Jul.
The chronic shortage of organs and tissues for transplantation represents a dramatic burden on healthcare systems worldwide. Tissue engineering offers a potential solution to address these shortages, but several challenges remain, with prevascularization being a critical factor for in vivo survival and integration of tissue engineering products. Concurrently, a different challenge hindering the clinical implementation of such products, regards their efficient preservation from the fabrication site to the bedside. Hypothermia has emerged as a potential solution for this issue due to its milder effects on biologic systems in comparison with other cold preservation methodologies. Its impact on prevascularization, however, has not been well studied. In this work, 3D prevascularized constructs were fabricated using adipose-derived stromal vascular fraction cells and preserved at 4 °C using Hypothermosol or basal culture media (α-MEM). Hypothermosol efficiently preserved the structural and cellular integrity of prevascular networks as compared to constructs before preservation. In contrast, the use of α-MEM led to a clear reduction in prevascular structures, with concurrent induction of high levels of apoptosis and autophagy at the cellular level. In vivo evaluation using a chorioallantoic membrane model demonstrated that, in opposition to α-MEM, Hypothermosol preservation retained the angiogenic potential of constructs before preservation by recruiting a similar number of blood vessels from the host and presenting similar integration with host tissue. These results emphasize the need of studying the impact of preservation techniques on key properties of tissue engineering constructs such as prevascularization, in order to validate and streamline their clinical application.
器官和组织移植的长期短缺给全球医疗系统带来了巨大负担。组织工程为解决这些短缺问题提供了一种潜在的解决方案,但仍存在一些挑战,其中预血管化是组织工程产品在体内存活和整合的关键因素。同时,阻碍此类产品临床应用的另一个挑战是如何从制造地点到床边对其进行有效保存。与其他低温保存方法相比,低温因其对生物系统的影响较小而成为解决这一问题的潜在方案。然而,其对预血管化的影响尚未得到充分研究。在这项工作中,使用脂肪来源的基质血管成分细胞制备了三维预血管化构建体,并使用低温保存液或基础培养基(α-MEM)在4°C下保存。与保存前的构建体相比,低温保存液有效地保存了预血管网络的结构和细胞完整性。相反,使用α-MEM导致预血管结构明显减少,同时在细胞水平上诱导高水平的细胞凋亡和自噬。使用尿囊膜模型进行的体内评估表明,与α-MEM相反,低温保存液保存通过从宿主招募相似数量的血管并与宿主组织呈现相似的整合,保留了保存前构建体的血管生成潜力。这些结果强调了研究保存技术对组织工程构建体关键特性(如预血管化)的影响的必要性,以便验证和简化其临床应用。
