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冷冻保存和去细胞化气管移植物的开发及体外/体内比较特性研究。

Development and In Vitro/In Vivo Comparative Characterization of Cryopreserved and Decellularized Tracheal Grafts.

机构信息

Section of Human Anatomy, Department of Neuroscience, University of Padova, 35121 Padova, Italy.

L.i.f.e.L.a.b. Program, Consorzio per la Ricerca Sanitaria (CORIS), Veneto Region, 35128 Padova, Italy.

出版信息

Cells. 2023 Mar 13;12(6):888. doi: 10.3390/cells12060888.

Abstract

Tracheal reconstruction represents a challenge when primary anastomosis is not feasible. Within this scenario, the study aim was to develop a new pig-derived decellularized trachea (DecellT) to be compared with the cryopreserved counterpart (CryoT) for a close predictive analysis. Tracheal segments underwent decellularization by a + method (12 cycles); in parallel, cryopreserved samples were also prepared. Once decellularized (histology/DNA quantification), the two groups were characterized for Alpha-Gal epitopes/structural proteins (immunohistochemistry/histology/biochemical assays/second harmonic generation microscopy)/ultrastructure (Scanning Electron Microscopy (SEM))/mechanical behaviour. Cytotoxicity absence was assessed in vitro (extract-test assay/direct seeding, HM1SV40 cell line) while biocompatibility was verified in BALB/c mice, followed by histological/immunohistochemical analyses and SEM (14 days). Decellularization effectively removed Alpha-Gal epitopes; cartilage histoarchitecture was retained in both groups, showing chondrocytes only in the CryoT. Cryopreservation maintained few respiratory epithelium sparse cilia, not detectable in DecellT. Focusing on ECM, preserved structural/ultrastructural organization and collagen content were observed in the cartilage of both; conversely, the GAGs were significantly reduced in DecellT, as confirmed by mechanical study results. No cytotoxicity was highlighted by CryoT/DecellT in vitro, as they were also corroborated by a biocompatibility assay. Despite some limitations (cells presence/GAGs reduction), CryoT/DecellT are both appealing options, which warrant further investigation in comparative in vivo studies.

摘要

当无法进行原发性吻合时,气管重建是一个挑战。在这种情况下,研究目的是开发一种新的猪源性脱细胞气管(DecellT),并与冷冻保存的气管(CryoT)进行对比分析,以进行密切预测。气管段通过 + 方法(12 个循环)进行脱细胞处理;同时,也制备了冷冻保存的样本。一旦脱细胞(组织学/DNA 定量),就对两组进行 Alpha-Gal 表位/结构蛋白(免疫组织化学/组织学/生化分析/二次谐波产生显微镜)/超微结构(扫描电子显微镜(SEM))/机械性能进行特征描述。体外评估了细胞毒性缺失(提取测试分析/直接接种,HM1SV40 细胞系),同时在 BALB/c 小鼠中验证了生物相容性,随后进行了组织学/免疫组织化学分析和 SEM(14 天)。脱细胞处理有效地去除了 Alpha-Gal 表位;两组的软骨组织形态学都得到了保留,仅在 CryoT 中观察到软骨细胞。冷冻保存仅保留了少量稀疏的呼吸上皮纤毛,在 DecellT 中不可检测。在 ECM 方面,两组软骨中均观察到保存的结构/超微结构组织和胶原蛋白含量;相反,在 DecellT 中 GAGs 显著减少,机械研究结果证实了这一点。CryoT/DecellT 在体外没有显示出细胞毒性,它们也通过生物相容性试验得到了证实。尽管存在一些局限性(细胞存在/GAGs 减少),但 CryoT/DecellT 都是有吸引力的选择,这需要进一步在比较体内研究中进行研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a894/10047860/99aeeec3ebb2/cells-12-00888-g001.jpg

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