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胆管细胞标志物阳性和阴性的胎肝细胞在再生暴露于倒千里光碱的成年大鼠肝脏的能力上存在显著差异。

Cholangiocyte marker-positive and -negative fetal liver cells differ significantly in their ability to regenerate the livers of adult rats exposed to retrorsine.

作者信息

Simper-Ronan Rhonda, Brilliant Kate, Flanagan Donna, Carreiro Marie, Callanan Helen, Sabo Edmond, Hixson Douglas C

机构信息

Department of Medicine, Division of Hematology and Oncology, Rhode Island Hospital and the Graduate Program in Pathobiology, Brown University Medical School, Providence, RI 02903, USA.

出版信息

Development. 2006 Nov;133(21):4269-79. doi: 10.1242/dev.02589. Epub 2006 Oct 4.

Abstract

We have used monoclonal antibodies against cell-surface developmental epitopes in combination with micromagnetic beads to isolate phenotypically defined subpopulations of cholangiocyte marker-positive fetal liver epithelial cells (CMP-FLEC). Differentiation potential was evaluated by injecting cell isolates from dipeptidyl peptidase IV (DPPIV) positive (DPPIV+) Fischer donor rats into the spleen of partially hepatectomized, DPPIV negative (DPPIV-) Fischer host rats exposed to retrorsine. At various time points, liver tissue was harvested and cells in DPPIV+ colonies were phenotyped by immunofluorescence and histochemical protocols. Functional differentiation and liver replacement were determined by comparing donor and host hepatocyte protein expression patterns and DPPIV enzyme activity in extracts from livers of host rats receiving CMP-FLEC. Our results showed that bipotentiality was retained during differentiation and maturation of CMP-FLEC, indicating that the acquisition of ductal morphology and phenotype were not indicative of lineage commitment. CMP-FLEC transplanted into the adult rat liver lost ductal and gained hepatocyte markers, and acquired protein expression patterns in 2D gels with a close similarity (>75% spot match) to host hepatocytes but differing significantly from the transplanted CMP-FLEC cell isolate (<25% spot match). The average size of donor hepatocyte colonies increased with time so that by 1 year, up to 70% of the host rat liver was replaced by CMP-FLEC derived DPPIV+ hepatocytes. Depletion of CMP-FLEC from fetal liver isolates resulted in a marked decrease in adult liver colonization, suggesting that a high percentage of the hepatocyte colonies in animals receiving total fetal liver isolates are derived from CMP-FLEC.

摘要

我们使用了针对细胞表面发育表位的单克隆抗体,并结合微磁珠来分离胆管细胞标志物阳性的胎肝上皮细胞(CMP-FLEC)的表型定义亚群。通过将来自二肽基肽酶IV(DPPIV)阳性(DPPIV+)的Fischer供体大鼠的细胞分离物注射到接受过部分肝切除、暴露于倒千里光碱的DPPIV阴性(DPPIV-)的Fischer宿主大鼠的脾脏中,来评估分化潜能。在不同时间点,收集肝脏组织,并通过免疫荧光和组织化学方法对DPPIV+集落中的细胞进行表型分析。通过比较供体和宿主肝细胞蛋白表达模式以及接受CMP-FLEC的宿主大鼠肝脏提取物中的DPPIV酶活性,来确定功能分化和肝脏替代情况。我们的结果表明,CMP-FLEC在分化和成熟过程中保留了双能性,这表明导管形态和表型的获得并不意味着细胞谱系的确定。移植到成年大鼠肝脏中的CMP-FLEC失去了导管标志物并获得了肝细胞标志物,并且在二维凝胶中获得的蛋白表达模式与宿主肝细胞非常相似(>75%斑点匹配),但与移植的CMP-FLEC细胞分离物有显著差异(<25%斑点匹配)。供体肝细胞集落的平均大小随时间增加,以至于到1年时,高达70%的宿主大鼠肝脏被CMP-FLEC来源的DPPIV+肝细胞所替代。从胎肝分离物中去除CMP-FLEC导致成年肝脏定植显著减少,这表明接受全胎肝分离物的动物中,很大一部分肝细胞集落来源于CMP-FLEC。

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