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特定胶原蛋白-弹性蛋白支架在幼年和成年大鼠中的组织反应,特别关注钙化情况。

Tissue response of defined collagen-elastin scaffolds in young and adult rats with special attention to calcification.

作者信息

Daamen W F, Nillesen S T M, Hafmans T, Veerkamp J H, van Luyn M J A, van Kuppevelt T H

机构信息

Department of Biochemistry 194, NCMLS, University Medical Centre Nijmegen, P.O. Box 9101, Nijmegen 6500 HB, The Netherlands.

出版信息

Biomaterials. 2005 Jan;26(1):81-92. doi: 10.1016/j.biomaterials.2004.02.011.

Abstract

Collagen-elastin scaffolds may be valuable biomaterials for tissue engineering because they combine tensile strength with elasticity. In this study, the tissue response to and the calcification of these scaffolds were evaluated. In particular, the hypothesis was tested that calcification, a common phenomenon in biomaterials, may be due to microfibrils within the elastic fibre, and that these microfibrils might generate a tissue response. Four scaffolds were subcutaneously implanted, viz. collagen, collagen + pure elastin, collagen+microfibril-containing, and collagen + pulverised elastic ligament (the source for elastin). Explants were evaluated at day 3, 7 and 21. In young Sprague Dawley rats, collagen + ligament calcified substantially, whereas collagen + elastin (with and without microfibrils) calcified less, and collagen did not. Calcification started at elastic fibres. In both Sprague Dawley and Wistar adult rats, however, none of the scaffolds calcified. Mononuclear cell infiltration was prominent in young and adult Sprague Dawley rats. In adult Wistar rats, this infiltration was associated with the presence of microfibrils. Degradation of scaffolds and new matrix formation were related with cellular influx and degree of vascularisation. In conclusion, absence of microfibrils from the elastic fibre does not prevent calcification in young Sprague Dawley rats, but does reduce the tissue response in adult Wistar rats. Cellular response and calcification differs with age and strain and therefore the choice of animal model is of key importance in biomaterial evaluation.

摘要

胶原蛋白 - 弹性蛋白支架可能是组织工程中有价值的生物材料,因为它们兼具拉伸强度和弹性。在本研究中,评估了这些支架的组织反应和钙化情况。具体而言,对以下假设进行了测试:钙化是生物材料中的常见现象,可能归因于弹性纤维内的微原纤维,并且这些微原纤维可能引发组织反应。皮下植入了四种支架,即胶原蛋白、胶原蛋白 + 纯弹性蛋白、含微原纤维的胶原蛋白以及胶原蛋白 + 粉碎的弹性韧带(弹性蛋白来源)。在第3、7和21天对外植体进行评估。在幼年斯普拉格 - 道利大鼠中,胶原蛋白 + 韧带大量钙化,而胶原蛋白 + 弹性蛋白(含或不含微原纤维)钙化较少,胶原蛋白则未钙化。钙化始于弹性纤维。然而,在成年斯普拉格 - 道利大鼠和成年Wistar大鼠中,所有支架均未钙化。在幼年和成年斯普拉格 - 道利大鼠中,单核细胞浸润明显。在成年Wistar大鼠中,这种浸润与微原纤维的存在有关。支架的降解和新基质的形成与细胞流入和血管化程度有关。总之,弹性纤维中不存在微原纤维并不能防止幼年斯普拉格 - 道利大鼠钙化,但确实会降低成年Wistar大鼠的组织反应。细胞反应和钙化因年龄和品系而异,因此动物模型的选择在生物材料评估中至关重要。

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