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凝血酶对前交叉韧带成纤维细胞与胶原水凝胶相互作用的影响。

The effect of thrombin on ACL fibroblast interactions with collagen hydrogels.

作者信息

Murray M M, Forsythe B, Chen F, Lee S J, Yoo J J, Atala A, Steinert A

机构信息

Department of Orthopaedic Surgery, Children's Hospital of Boston, 300 Longwood Avenue, Boston, Massachusetts 02115, USA.

出版信息

J Orthop Res. 2006 Mar;24(3):508-15. doi: 10.1002/jor.20054.

Abstract

Premature loss of provisional scaffold formation has been identified as one of the factors responsible for poor healing of intraarticular tissues. To address this deficiency, substitute provisional scaffolds are being developed. The function of these scaffolds can be enhanced by the addition of specific extracellular matrix proteins. In this study, it was hypothesized that the addition of thrombin to a provisional scaffold material would result in increases in cell proliferation, collagen production, and cell migration within the scaffold. These three parameters are thought to be critical components of wound healing. Gels containing fibrin and collagen supplemented with either 0, 10.5, 21, or 42 U/mL of thrombin were placed in contact with explants of tissue from the anterior cruciate ligament. The addition of thrombin stimulated cell migration at low concentrations and impaired migration at higher concentrations, and had no significant effect on cell proliferation or collagen production. The use of all concentrations of thrombin resulted in mechanically weaker gels. Thus, the use of thrombin to optimize a collagen-platelet rich plasma (PRP) provisional scaffold must be done with caution, and use of high concentrations of thrombin (>42 IU/mL) should be avoided specifically in situations where gel strength or cell ingrowth is important. Use of low concentrations of thrombin (10.5 IU/mL) may be beneficial in applications where a faster set time and enhanced cell migration are desirable and the gel mechanical strength is of secondary importance.

摘要

临时支架形成过早丧失已被确定为关节内组织愈合不良的原因之一。为解决这一缺陷,正在开发替代临时支架。通过添加特定的细胞外基质蛋白可以增强这些支架的功能。在本研究中,假设向临时支架材料中添加凝血酶会导致支架内细胞增殖、胶原蛋白产生和细胞迁移增加。这三个参数被认为是伤口愈合的关键组成部分。将含有纤维蛋白和胶原蛋白并补充有0、10.5、21或42 U/mL凝血酶的凝胶与前交叉韧带的组织外植体接触。添加凝血酶在低浓度时刺激细胞迁移,在高浓度时损害迁移,并且对细胞增殖或胶原蛋白产生没有显著影响。使用所有浓度的凝血酶都会导致凝胶的机械强度较弱。因此,使用凝血酶优化富含胶原蛋白的血小板血浆(PRP)临时支架时必须谨慎,特别是在凝胶强度或细胞向内生长很重要的情况下,应避免使用高浓度的凝血酶(>42 IU/mL)。在需要更快凝固时间和增强细胞迁移且凝胶机械强度次要的应用中,使用低浓度的凝血酶(10.5 IU/mL)可能是有益的。

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