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肝脏支架支持多能性新生儿同种异体细胞的存活和代谢功能。

Liver Scaffolds Support Survival and Metabolic Function of Multilineage Neonatal Allogenic Cells.

机构信息

1 Department of Surgery, University of Maryland School of Medicine , Baltimore, Maryland.

2 Department of Pathology, University of Maryland School of Medicine , Baltimore, Maryland.

出版信息

Tissue Eng Part A. 2018 May;24(9-10):786-793. doi: 10.1089/ten.TEA.2017.0279. Epub 2017 Nov 30.

Abstract

Organ scaffold bioengineering is currently limited by the inability to effectively repopulate the scaffold with appropriately distributed functional cells. We examined the feasibility of a decellularized liver scaffold to support the growth and function of multilineage allogenic cells derived from either adult or neonatal liver cells. Cell slurries from neonatal and adult rat livers containing hepatocytes, cholangiocytes, and endothelial cells were introduced into decellularized adult rat liver scaffolds via the bile duct. Recellularized grafts were perfused with cell growth medium through the portal vein for 7 days. Concurrently, the same cell slurries were incubated on culture dishes. Albumin levels were measured from graft perfusates and cell culture media. Immunofluorescent assays were used to verify the colocalization of cholangiocytes, hepatocytes, endothelial cells, and Kupffer cells in the recellularized grafts by using anti-CK7, anti-hepatocyte antigen, anti-CD34, and anti-CD68, respectively. More robust albumin production was detected in the perfusate of scaffolds recellularized with a neonatal liver cell slurry compared with those with an adult liver cell slurry. The perfusates from all recellularized grafts showed increasing albumin concentration over 7 days; higher levels were detected in the constructs compared with the cell culture. Scaffolds seeded with a neonatal liver cell slurry showed the presence of hepatocytes, cholangiocytes, endothelial cells, and Kupffer cells. Results demonstrated the superiority of neonatal allogenic cells over adult cells of the same origin, possibly because of their pluripotent behavior. Liver bio-scaffolds supported the growth of four different liver cell lines. Recellularized grafts exhibited preserved functionality as demonstrated by albumin production, and constructs seeded with a neonatal cell slurry demonstrated proliferation on Ki-67 assay, thus representing a promising model for a transplantable construct.

摘要

器官支架生物工程目前受到限制,无法有效地将适当分布的功能性细胞重新填充到支架中。我们研究了脱细胞化肝脏支架支持多谱系同种异体细胞生长和功能的可行性,这些细胞来自成年或新生儿肝脏细胞。含有肝细胞、胆管细胞和内皮细胞的新生和成年大鼠肝细胞细胞匀浆通过胆管被引入脱细胞成年大鼠肝支架中。再细胞化的移植物通过门静脉用细胞生长培养基灌注 7 天。同时,将相同的细胞匀浆在培养皿中孵育。从移植物灌流液和细胞培养物中测量白蛋白水平。通过使用抗 CK7、抗肝细胞抗原、抗 CD34 和抗 CD68,免疫荧光测定分别验证了再细胞化移植物中胆管细胞、肝细胞、内皮细胞和库普弗细胞的共定位。与使用成年肝细胞浆再细胞化的支架相比,使用新生肝细胞浆再细胞化的支架的灌流液中检测到更丰富的白蛋白产生。所有再细胞化移植物的灌流液在 7 天内显示出白蛋白浓度增加;与细胞培养物相比,在构建物中检测到更高的水平。用新生肝细胞浆接种的支架显示存在肝细胞、胆管细胞、内皮细胞和库普弗细胞。结果表明,来自同一来源的新生同种异体细胞优于成年细胞,可能是因为它们具有多能性。肝生物支架支持四种不同的肝细胞系的生长。再细胞化移植物表现出保留的功能,如白蛋白产生,并且用新生细胞浆接种的构建物在 Ki-67 测定中显示出增殖,因此代表了可移植构建物的有前途的模型。

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