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BICOMPONENT FIBROUS SCAFFOLDS OF CONTROLLED COMPOSITION FOR TISSUE ENGINEERING APPLICATIONS

机译:用于组织工程应用的控制组合物的双组分纤维支架

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Electrospinning has been widely studied for constructing tissue engineering scaffolds because of the morphological and size effects of electrospun fibers on cell behavior. Research on electrospun tissue engineering scaffolds has been based mainly on using solutions of single polymer or blends of polymers dissolved in common solvents, which has put limitations to scaffolds that can be built. There is an increasing need for using the multi-source and multi-power electrospinning approach to fabricate multicomponent fibrous scaffolds because these scaffolds have great potential for tissue engineering and controlled (drug) release applications. In the present study, bicomponent fibrous scaffolds were fabricated through dualsource and dual-power electrospinning using poly(L-lactic acid) (PLLA) and gelatin polymers. The experimental setup ensured that the solution and electrospinning parameters for each electrospun fibrous component were controlled separately and hence the morphology of electrospun fibers could be controlled and optimized. By adjusting the number of syringes that fed polymer solutions, the composition of bicomponent scaffolds (i.e. the weight percentage of gelatin varying from 0 to 100%) could also be controlled. Such controls would yield scaffolds of desired properties (hydrophilicity, degradation rate, strength, etc.) After electrospinning, pure gelatin scaffolds and bicomponent scaffolds were crosslinked by glutaraldehyde (GA) and genipin, respectively, using different crosslinking methods. Both crosslinked and non-crosslinked scaffolds were studied using various techniques (scanning electron microscopy (SEM) for scaffold morphology, differential scanning calorimetry (DSC) for polymer crystallinity, contact angle measurement for hydrophilicity, tensile testing for mechanical properties and crosslinking efficiency, etc.). It was found that the bicomponent scaffolds were more hydrophilic than pure PLLA scaffolds due to the presence of gelatin fibers. The tensile strength of bicomponent scaffolds was also increased after crosslinking. Using our experimental setup, bicomponent scaffolds could be constructed for tissue engineering with enhanced mechanical properties, biocompatibility and biodegradability. Furthermore, in the bicomponent scaffolds, while PLLA fibers could act as the structural component with a slower degradation rate, the gelatin fibers could be used as a carrier for therapeutic agents (drugs and therapeutic biomolecules). With controlled degrees of the crosslinking of gelatin, the release of therapeutic agents from gelatin fibers would be controlled.
机译:由于电纺纤维对细胞行为的形态和尺寸效应,静电纺丝已被广泛研究用于构建组织工程支架。电动纺织组织工程支架的研究主要是基于使用溶解在普通溶剂中的单一聚合物或聚合物的共混物的溶液,这对可构建的支架施加限制。越来越需要使用多源和多功能静电纺丝方法来制造多组分纤维支架,因为这些支架具有巨大的组织工程和控制(药物)释放应用。在本研究中,通过使用聚(L-乳酸)(PLLA)和明胶聚合物来制造双组分纤维支架和双功率静电。实验装置确保了每个电纺器纤维组分的溶液和静电纺丝参数单独控制,因此可以控制和优化电纺纤维的形态。通过调节喂养聚合物溶液的注射器的数量,也可以控制双组分支架的组成(即从0到100%的明胶的重量百分比)。这种对照将在静电纺丝后产生所需性质(亲水性,降解速率,强度等)的支架,使用不同的交联方法,分别通过戊二醛(GA)和Genipin通过戊二醛(GA)和Genipin交联。使用各种技术(扫描电子显微镜(SEM)进行交联和非交联的支架,用于支架形态,用于聚合物结晶度的差示扫描量热法(DSC),用于亲水性的接触角测量,机械性能和交联效率的拉伸试验等。 )。结果发现,由于明胶纤维的存在,双组分支架比纯PLLA支架更亲水。交联后,双组分支架的拉伸强度也增加。使用我们的实验装置,可以为组织工程构建双组分支架,具有增强的机械性能,生物相容性和生物降解性。此外,在双组分支架中,虽然PLLA纤维可以用作具有较慢降解速率的结构组分,但明胶纤维可以用作治疗剂的载体(药物和治疗生物分子)。对于明胶的交联程度,可以控制来自明胶纤维的治疗剂的释放。

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