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新鲜的和体外成骨分化的人羊膜,单独使用或与额外的支架联合使用,均不会在Balb/c小鼠中诱导异位骨形成。

Fresh and in vitro osteodifferentiated human amniotic membrane, alone or associated with an additional scaffold, does not induce ectopic bone formation in Balb/c mice.

作者信息

Laurent Romain, Nallet Aurélie, de Billy Benoit, Obert Laurent, Nicod Laurence, Meyer Christophe, Layrolle Pierre, Zwetyenga Narcisse, Gindraux Florelle

机构信息

Paediatric Surgery Service, University Hospital of Besancon, Besançon, France.

Novotec, Lyon, France.

出版信息

Cell Tissue Bank. 2017 Mar;18(1):17-25. doi: 10.1007/s10561-016-9605-2. Epub 2016 Dec 20.

DOI:10.1007/s10561-016-9605-2
PMID:27999996
Abstract

The human amniotic membrane (hAM) has been successfully used as a natural carrier containing amniotic mesenchymal stromal cells, epithelial cells and growth factors. It has a little or no immunogenicity, and possesses useful anti-microbial, anti-inflammatory, anti-fibrotic and analgesic properties. It has been used for many years in several indications for soft tissue repair. We previously reported that hAM represents a natural and preformed sheet containing highly potent stem cells, and could thus be used for bone repair. Indeed, native hAM possesses pre-osteoblastic potential that can easily be stimulated, even as far as mineralization, by means of in vitro osteogenic culture. However, cell culture induces damage to the tissue, as well as to cell phenotype and function. The aim of this study was to evaluate new bone formation by fresh and in vitro osteodifferentiated hAM, alone or associated with an additional scaffold presenting osteoinductive properties. Moreover, we also aimed to determine the effect of in vitro hAM pre-osteodifferentiation on its in vivo biocompatibility/tissue degradation. Results showed that neither fresh nor osteodifferentiated hAM induced ectopic bone formation, whether or not it was associated with the osteoinductive scaffold. Secondly, fresh and osteodifferentiated hAM presented similar in vivo tissue degradation, suggesting that in vitro hAM pre-osteodifferentiation did not influence its in vivo biocompatibility.

摘要

人羊膜(hAM)已成功用作含有羊膜间充质基质细胞、上皮细胞和生长因子的天然载体。它具有很小的免疫原性或无免疫原性,并具有有益的抗菌、抗炎、抗纤维化和镇痛特性。多年来,它已被用于多种软组织修复适应症。我们之前报道过,hAM是一种含有高效干细胞的天然预制薄片,因此可用于骨修复。事实上,天然hAM具有前成骨细胞潜能,通过体外成骨培养,甚至可以轻易地刺激其矿化。然而,细胞培养会对组织以及细胞表型和功能造成损害。本研究的目的是评估新鲜的和体外成骨分化的hAM单独或与具有骨诱导特性的额外支架联合使用时新骨的形成情况。此外,我们还旨在确定体外hAM前成骨分化对其体内生物相容性/组织降解的影响。结果表明,无论是新鲜的还是成骨分化的hAM,无论是否与骨诱导支架联合使用,均未诱导异位骨形成。其次,新鲜的和成骨分化的hAM在体内呈现出相似的组织降解情况,这表明体外hAM前成骨分化并未影响其体内生物相容性。

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