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混合凝血酶激活的富血小板血浆:成骨/血管生成移植物工程中胎牛血清的替代品。

Pooled thrombin-activated platelet-rich plasma: a substitute for fetal bovine serum in the engineering of osteogenic/vasculogenic grafts.

作者信息

Tchang Laurent A, Pippenger Benjamin E, Todorov Atanas, Wolf Francine, Burger Maximilian G, Jaquiery Claude, Bieback Karen, Martin Ivan, Schaefer Dirk J, Scherberich Arnaud

机构信息

Department of Plastic, Reconstructive, Aesthetic and Hand Surgery, University Hospital of Basel, Switzerland.

Laboratory of Tissue Engineering, Department of Biomedicine, University and University Hospital of Basel, Switzerland.

出版信息

J Tissue Eng Regen Med. 2017 May;11(5):1542-1552. doi: 10.1002/term.2054. Epub 2015 Jun 15.

Abstract

The use of fetal bovine serum (FBS) as a culture medium supplement in cell therapy and clinical tissue engineering is challenged by immunological concerns and the risk of disease transmission. Here we tested whether human, thrombin-activated, pooled, platelet-rich plasma (tPRP) can be substituted for FBS in the engineering of osteogenic and vasculogenic grafts, using cells from the stromal vascular fraction (SVF) of human adipose tissue. SVF cells were cultured under perfusion flow into porous hydroxyapatite scaffolds for 5 days, with the medium supplemented with either 10% tPRP or 10% FBS and implanted in an ectopic mouse model. Following in vitro culture, as compared to FBS, the use of tPRP did not modify the fraction of clonogenic cells or the different cell phenotypes, but increased by 1.9-fold the total number of cells. After 8 weeks in vivo, bone tissue was formed more reproducibly and in higher amounts (3.7-fold increase) in constructs cultured with tPRP. Staining for human-specific ALU sequences and for the human isoforms of CD31/CD34 revealed the human origin of the bone, the formation of blood vessels by human vascular progenitors and a higher density of human cells in implants cultured with tPRP. In summary, tPRP supports higher efficiency of bone formation by SVF cells than FBS, likely by enhancing cell expansion in vitro while maintaining vasculogenic properties. The use of tPRP may facilitate the clinical translation of osteogenic grafts with intrinsic capacity for vascularization, based on the use of adipose-derived cells. Copyright © 2015 John Wiley & Sons, Ltd.

摘要

在细胞治疗和临床组织工程中,将胎牛血清(FBS)用作培养基补充剂受到免疫方面的担忧以及疾病传播风险的挑战。在此,我们测试了人凝血酶激活的混合富血小板血浆(tPRP)是否可以替代FBS用于成骨和血管生成移植物的工程构建,使用的是人脂肪组织基质血管部分(SVF)的细胞。将SVF细胞在灌注流条件下培养于多孔羟基磷灰石支架中5天,培养基中添加10% tPRP或10% FBS,然后植入异位小鼠模型。体外培养后,与FBS相比,使用tPRP并未改变克隆形成细胞的比例或不同的细胞表型,但细胞总数增加了1.9倍。体内8周后,在用tPRP培养的构建物中,骨组织形成更具可重复性且数量更多(增加了3.7倍)。对人特异性ALU序列以及CD31/CD34的人异构体进行染色,揭示了骨的人源性质、人血管祖细胞形成血管以及在用tPRP培养的植入物中人类细胞密度更高。总之,tPRP支持SVF细胞形成骨的效率高于FBS,这可能是通过在体外增强细胞扩增同时维持血管生成特性实现 的。基于脂肪来源细胞,tPRP的使用可能会促进具有内在血管化能力的成骨移植物的临床转化。版权所有© 2015约翰威立父子有限公司。

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