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源自L-亮氨酸的新型聚(酯脲):负载抗菌药物和酶的电纺支架

New poly(ester urea) derived from L-leucine: electrospun scaffolds loaded with antibacterial drugs and enzymes.

作者信息

Díaz Angélica, del Valle Luis J, Tugushi David, Katsarava Ramaz, Puiggalí Jordi

机构信息

Departament d'Enginyeria Química, Universitat Politècnica de Catalunya, Av. Diagonal 647, Barcelona E-08028, Spain.

Institute of Chemistry and Molecular Engineering, Agricultural University of Georgia, 13km. David Aghmashenebeli Alley, Tblisi 0131, Georgia.

出版信息

Mater Sci Eng C Mater Biol Appl. 2015 Jan;46:450-62. doi: 10.1016/j.msec.2014.10.055. Epub 2014 Oct 23.

Abstract

Electrospun scaffolds from an amino acid containing poly(ester urea) (PEU) were developed as promising materials in the biomedical field and specifically in tissue engineering applications. The selected poly(ester urea) was obtained with a high yield and molecular weight by reaction of phosgene with a bis(α-aminoacyl)-α,ω-diol-diester monomer. The polymer having L-leucine, 1,6-hexanediol and carbonic acid units had a semicrystalline character and relatively high glass transition and melting temperatures. Furthermore it was highly soluble in most organic solvents, an interesting feature that facilitated the electrospinning process and the effective incorporation of drugs with bactericidal activity (e.g. biguanide derivatives such as clorhexidine and polyhexamethylenebiguanide) and enzymes (e.g. α-chymotrypsin) that accelerated the degradation process. Continuous micro/nanofibers were obtained under a wide range of processing conditions, being diameters of electrospun fibers dependent on the drug and solvent used. Poly(ester urea) samples were degradable in media containing lipases and proteinases but the degradation rate was highly dependent on the surface area, being specifically greater for scaffolds with respect to films. The high hydrophobicity of new scaffolds had repercussions on enzymatic degradability since different weight loss rates were found depending on how samples were exposed to the medium (e.g. forced or non-forced immersion). New scaffolds were biocompatible, as demonstrated by adhesion and proliferation assays performed with fibroblast and epithelial cells.

摘要

由含氨基酸的聚(酯脲)(PEU)制成的电纺支架被开发为生物医学领域尤其是组织工程应用中有前景的材料。所选的聚(酯脲)通过光气与双(α-氨基酰基)-α,ω-二醇二酯单体反应以高产率和高分子量获得。具有L-亮氨酸、1,6-己二醇和碳酸单元的聚合物具有半结晶特性以及相对较高的玻璃化转变温度和熔点。此外,它在大多数有机溶剂中高度可溶,这一有趣特性促进了电纺过程以及具有杀菌活性的药物(例如洗必泰和聚六亚甲基双胍等双胍衍生物)和加速降解过程的酶(例如α-胰凝乳蛋白酶)的有效掺入。在广泛的加工条件下获得了连续的微/纳米纤维,电纺纤维的直径取决于所使用的药物和溶剂。聚(酯脲)样品在含有脂肪酶和蛋白酶的介质中可降解,但降解速率高度依赖于表面积,对于支架而言相对于薄膜尤其更大。新支架的高疏水性对酶促降解性有影响,因为根据样品暴露于介质的方式(例如强制或非强制浸泡)发现了不同的失重率。如用成纤维细胞和上皮细胞进行的粘附和增殖试验所表明的,新支架具有生物相容性。

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