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用于软组织应用的线性和支化 l-缬氨酸基聚(酯脲)的临床前体外和体内评估

Preclinical in Vitro and in Vivo Assessment of Linear and Branched l-Valine-Based Poly(ester urea)s for Soft Tissue Applications.

作者信息

Dreger Nathan Z, Wandel Mary B, Robinson Lindsay L, Luong Derek, Søndergaard Claus S, Hiles Michael, Premanandan Christopher, Becker Matthew L

机构信息

Cook Biotech Incorporated, West Lafayette, Indiana 47906, United States.

Department of Veterinary Biosciences, College of Veterinary Medicine, The Ohio State University, Columbus, Ohio 43210, United States.

出版信息

ACS Biomater Sci Eng. 2018 Apr 9;4(4):1346-1356. doi: 10.1021/acsbiomaterials.7b00920. Epub 2018 Mar 6.

Abstract

New polymers are needed to address the shortcomings of commercially available materials for soft tissue repair. Herein, we investigated a series of l-valine-based poly(ester urea)s (PEUs) that vary in monomer composition and the extent of branching as candidate materials for soft tissue repair. The preimplantation Young's moduli (105 ± 30 to 269 ± 12 MPa) for all the PEUs are comparable to those of polypropylene (165 ± 5 MPa) materials currently employed in hernia-mesh repair. The 2% branched poly(1-VAL-8) maintained the highest Young's modulus following 3 months of in vivo implantation (78 ± 34 MPa) when compared to other PEU analogues (20 ± 6-45 ± 5 MPa). Neither the linear or branched PEUs elicited a significant inflammatory response in vivo as noted by less fibrous capsule formation after 3 months of implantation (80 ± 38 to 103 ± 33 μm) relative to polypropylene controls (126 ± 34 μm). Mechanical degradation in vivo over three months, coupled with limited inflammatory response, suggests that l-valine-based PEUs are translationally relevant materials for soft tissue applications.

摘要

需要新型聚合物来解决市售软组织修复材料的缺点。在此,我们研究了一系列基于L-缬氨酸的聚(酯脲)(PEU),它们在单体组成和支化程度上有所不同,作为软组织修复的候选材料。所有PEU植入前的杨氏模量(105±30至269±12兆帕)与目前用于疝修补网片的聚丙烯材料(165±5兆帕)相当。与其他PEU类似物(20±6 - 45±5兆帕)相比,2%支化的聚(1-VAL-8)在体内植入3个月后保持最高的杨氏模量(78±34兆帕)。线性或支化的PEU在体内均未引发明显的炎症反应,这一点可从植入3个月后相对于聚丙烯对照(126±34微米)形成的纤维囊较少(80±38至103±33微米)看出。三个月内在体内的机械降解,加上有限的炎症反应,表明基于L-缬氨酸的PEU是适用于软组织应用的具有转化意义的材料。

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