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功能性人诱导多能干细胞衍生气道上皮贴片中短期临床前应用。

Short-Term Preclinical Application of Functional Human Induced Pluripotent Stem Cell-Derived Airway Epithelial Patches.

机构信息

Latner Thoracic Surgery Laboratories, Toronto General Hospital Research Institute, University Health Network, Toronto General Hospital, University of Toronto, 101 College St, Toronto, ON, M5G 0A3, Canada.

Institute of Biomedical Engineering (BME), University of Toronto, 164 College St, Toronto, ON, M5S 3G9, Canada.

出版信息

Adv Healthc Mater. 2021 Nov;10(21):e2100957. doi: 10.1002/adhm.202100957. Epub 2021 Sep 26.

Abstract

Airway pathologies including cancer, trauma, and stenosis lack effective treatments, meanwhile airway transplantation and available tissue engineering approaches fail due to epithelial dysfunction. Autologous progenitors do not meet the clinical need for regeneration due to their insufficient expansion and differentiation, for which human induced pluripotent stem cells (hiPSCs) are promising alternatives. Airway epithelial patches are engineered by differentiating hiPSC-derived airway progenitors into physiological proportions of ciliated (73.9 ± 5.5%) and goblet (2.1 ± 1.4%) cells on a silk fibroin-collagen vitrigel membrane (SF-CVM) composite biomaterial for transplantation in porcine tracheal defects ex vivo and in vivo. Evaluation of ex vivo tracheal repair using hiPSC-derived SF-CVM patches demonstrate native-like tracheal epithelial metabolism and maintenance of mucociliary epithelium to day 3. In vivo studies demonstrate SF-CVM integration and maintenance of airway patency, showing 80.8 ± 3.6% graft coverage with an hiPSC-derived pseudostratified epithelium and 70.7 ± 2.3% coverage with viable cells, 3 days postoperatively. The utility of bioengineered, hiPSC-derived epithelial patches for airway repair is demonstrated in a short-term preclinical survival model, providing a significant leap for airway reconstruction approaches.

摘要

气道病变包括癌症、创伤和狭窄,缺乏有效治疗方法,同时由于上皮功能障碍,气道移植和现有的组织工程方法也失败了。由于其扩增和分化不足,自体祖细胞无法满足再生的临床需求,而人诱导多能干细胞(hiPSC)是很有前途的替代品。通过在丝素蛋白-胶原蛋白 vitrigel 膜(SF-CVM)复合生物材料上将 hiPSC 衍生的气道祖细胞分化为具有生理比例的纤毛(73.9 ± 5.5%)和杯状细胞(2.1 ± 1.4%),来构建气道上皮贴片,用于体外和体内猪气管缺损的移植。使用 hiPSC 衍生的 SF-CVM 贴片进行体外气管修复的评估表明,具有类似于天然的气管上皮代谢和黏液纤毛上皮的维持,可维持 3 天。体内研究表明 SF-CVM 整合和气道通畅的维持,术后 3 天,具有 hiPSC 衍生的假复层上皮的移植物覆盖率为 80.8 ± 3.6%,有活力的细胞覆盖率为 70.7 ± 2.3%。在短期临床前存活模型中,生物工程、hiPSC 衍生的上皮贴片在气道修复方面的应用得到了证明,为气道重建方法提供了重大突破。

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