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用于大鼠模型腹疝修复的仿生胶原蛋白/弹性蛋白网片。

Biomimetic collagen/elastin meshes for ventral hernia repair in a rat model.

作者信息

Minardi Silvia, Taraballi Francesca, Wang Xin, Cabrera Fernando J, Van Eps Jeffrey L, Robbins Andrew B, Sandri Monica, Moreno Michael R, Weiner Bradley K, Tasciotti Ennio

机构信息

Center for Biomimetic Medicine, Houston Methodist Research Institute (HMRI), 6670 Bertner Ave., Houston, TX 77030, USA; National Research Council of Italy - Institute of Science and Technology for Ceramics (ISTEC-CNR), Via Granarolo 64, 48018 Faenza, RA, Italy.

Center for Biomimetic Medicine, Houston Methodist Research Institute (HMRI), 6670 Bertner Ave., Houston, TX 77030, USA.

出版信息

Acta Biomater. 2017 Mar 1;50:165-177. doi: 10.1016/j.actbio.2016.11.032. Epub 2016 Nov 18.

Abstract

UNLABELLED

Ventral hernia repair remains a major clinical need. Herein, we formulated a type I collagen/elastin crosslinked blend (CollE) for the fabrication of biomimetic meshes for ventral hernia repair. To evaluate the effect of architecture on the performance of the implants, CollE was formulated both as flat sheets (CollE Sheets) and porous scaffolds (CollE Scaffolds). The morphology, hydrophylicity and in vitro degradation were assessed by SEM, water contact angle and differential scanning calorimetry, respectively. The stiffness of the meshes was determined using a constant stretch rate uniaxial tensile test, and compared to that of native tissue. CollE Sheets and Scaffolds were tested in vitro with human bone marrow-derived mesenchymal stem cells (h-BM-MSC), and finally implanted in a rat ventral hernia model. Neovascularization and tissue regeneration within the implants was evaluated at 6weeks, by histology, immunofluorescence, and q-PCR. It was found that CollE Sheets and Scaffolds were not only biomechanically sturdy enough to provide immediate repair of the hernia defect, but also promoted tissue restoration in only 6weeks. In fact, the presence of elastin enhanced the neovascularization in both sheets and scaffolds. Overall, CollE Scaffolds displayed mechanical properties more closely resembling those of native tissue, and induced higher gene expression of the entire marker genes tested, associated with de novo matrix deposition, angiogenesis, adipogenesis and skeletal muscles, compared to CollE Sheets. Altogether, this data suggests that the improved mechanical properties and bioactivity of CollE Sheets and Scaffolds make them valuable candidates for applications of ventral hernia repair.

STATEMENT OF SIGNIFICANCE

Due to the elevated annual number of ventral hernia repair in the US, the lack of successful grafts, the design of innovative biomimetic meshes has become a prime focus in tissue engineering, to promote the repair of the abdominal wall, avoid recurrence. Our meshes (CollE Sheets and Scaffolds) not only showed promising mechanical performance, but also allowed for an efficient neovascularization, resulting in new adipose and muscle tissue formation within the implant, in only 6weeks. In addition, our meshes allowed for the use of the same surgical procedure utilized in clinical practice, with the commercially available grafts. This study represents a significant step in the design of bioactive acellular off-the-shelf biomimetic meshes for ventral hernia repair.

摘要

未标注

腹疝修补仍然是一项重大的临床需求。在此,我们制备了一种I型胶原蛋白/弹性蛋白交联共混物(CollE),用于制造用于腹疝修补的仿生网片。为了评估结构对植入物性能的影响,CollE被制成平板(CollE片材)和多孔支架(CollE支架)两种形式。分别通过扫描电子显微镜(SEM)、水接触角和差示扫描量热法评估其形态、亲水性和体外降解情况。使用恒定拉伸速率单轴拉伸试验测定网片的刚度,并与天然组织的刚度进行比较。将CollE片材和支架与人骨髓间充质干细胞(h-BM-MSC)进行体外测试,最后植入大鼠腹疝模型中。在6周时,通过组织学、免疫荧光和定量聚合酶链反应(q-PCR)评估植入物内的新生血管形成和组织再生情况。结果发现,CollE片材和支架不仅在生物力学上足够坚固,能够立即修复疝缺损,而且在仅6周内就促进了组织修复。事实上,弹性蛋白的存在增强了片材和支架中的新生血管形成。总体而言,与CollE片材相比,CollE支架表现出更接近天然组织的力学性能,并诱导了所测试的所有标记基因的更高基因表达,这些基因与新生基质沉积、血管生成、脂肪生成和骨骼肌相关。总之,这些数据表明,CollE片材和支架改善的力学性能和生物活性使其成为腹疝修补应用的有价值候选材料。

意义声明

由于美国每年腹疝修补的数量不断增加,且缺乏成功的移植物,设计创新的仿生网片已成为组织工程的首要重点,以促进腹壁修复,避免复发。我们的网片(CollE片材和支架)不仅显示出有前景的力学性能,而且仅在6周内就实现了有效的新生血管形成,导致植入物内形成新的脂肪和肌肉组织。此外,我们的网片允许使用与临床实践中用于市售移植物相同的手术程序。这项研究代表了用于腹疝修补的生物活性无细胞现成仿生网片设计的重要一步。

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