Ethanol treatment of nanoPGA/PCL composite scaffolds enhances human chondrocyte development in the cellular microenvironment of tissue-engineered auricle constructs.

PloS one 2021 Vol.16(7) p. e0253149

Hirano N, Kusuhara H, Sueyoshi Y, Teramura T, Murthy A, Asamura S, Isogai N, Jacquet RD, Landis WJ

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Abstract

A major obstacle for tissue engineering ear-shaped cartilage is poorly developed tissue comprising cell-scaffold constructs. To address this issue, bioresorbable scaffolds of poly-ε-caprolactone (PCL) and polyglycolic acid nanofibers (nanoPGA) were evaluated using an ethanol treatment step before auricular chondrocyte scaffold seeding, an approach considered to enhance scaffold hydrophilicity and cartilage regeneration. Auricular chondrocytes were isolated from canine ears and human surgical samples discarded during otoplasty, including microtia reconstruction. Canine chondrocytes were seeded onto PCL and nanoPGA sheets either with or without ethanol treatment to examine cellular adhesion in vitro. Human chondrocytes were seeded onto three-dimensional bioresorbable composite scaffolds (PCL with surface coverage of nanoPGA) either with or without ethanol treatment and then implanted into athymic mice for 10 and 20 weeks. On construct retrieval, scanning electron microscopy showed canine auricular chondrocytes seeded onto ethanol-treated scaffolds in vitro developed extended cell processes contacting scaffold surfaces, a result suggesting cell-scaffold adhesion and a favorable microenvironment compared to the same cells with limited processes over untreated scaffolds. Adhesion of canine chondrocytes was statistically significantly greater (p ≤ 0.05) for ethanol-treated compared to untreated scaffold sheets. After implantation for 10 weeks, constructs of human auricular chondrocytes seeded onto ethanol-treated scaffolds were covered with glossy cartilage while constructs consisting of the same cells seeded onto untreated scaffolds revealed sparse connective tissue and cartilage regeneration. Following 10 weeks of implantation, RT-qPCR analyses of chondrocytes grown on ethanol-treated scaffolds showed greater expression levels for several cartilage-related genes compared to cells developed on untreated scaffolds with statistically significantly increased SRY-box transcription factor 5 (SOX5) and decreased interleukin-1α (inflammation-related) expression levels (p ≤ 0.05). Ethanol treatment of scaffolds led to increased cartilage production for 20- compared to 10-week constructs. While hydrophilicity of scaffolds was not assessed directly in the present findings, a possible factor supporting the summary data is that hydrophilicity may be enhanced for ethanol-treated nanoPGA/PCL scaffolds, an effect leading to improvement of chondrocyte adhesion, the cellular microenvironment and cartilage regeneration in tissue-engineered auricle constructs.

추출된 의학 개체 (NER)

유형영어 표현한국어 / 풀이UMLS CUI출처등장
재료 pcl 폴리카프로락톤 dict 5
시술 otoplasty 귀성형술 dict 1
해부 cellular scispacy 1
해부 auricle scispacy 1
해부 tissue scispacy 1
해부 cell-scaffold scispacy 1
해부 auricular chondrocyte scispacy 1
해부 cartilage scispacy 1
해부 Auricular chondrocytes scispacy 1
해부 chondrocytes scispacy 1
해부 cell scispacy 1
해부 cells scispacy 1
해부 connective tissue scispacy 1
해부 chondrocyte scispacy 1
약물 Ethanol C0001962
ethanol
scispacy 1
약물 poly-ε-caprolactone scispacy 1
약물 polyglycolic acid C0032502
polyglycolic acid
scispacy 1
기타 human chondrocyte scispacy 1
기타 canine ears scispacy 1
기타 human scispacy 1
기타 Human chondrocytes scispacy 1
기타 mice scispacy 1
기타 canine chondrocytes scispacy 1
기타 human auricular chondrocytes scispacy 1
기타 cartilage-related scispacy 1
기타 SRY-box scispacy 1
기타 SOX5 → SRY-box transcription factor 5 scispacy 1

MeSH Terms

Animals; Cell Culture Techniques; Cell Differentiation; Cells, Cultured; Cellular Microenvironment; Chondrocytes; Chondrogenesis; Congenital Microtia; Dogs; Ear Auricle; Ear Cartilage; Ear, External; Ethanol; Female; Humans; Male; Mice; Mice, Nude; Nanofibers; Polyglycolic Acid; Tissue Engineering; Tissue Scaffolds

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