Literature DB >> 25867583

Clonogenically Culturing and Expanding CD34+ Liver Cancer Stem Cells in Vitro.

Su Cheol Park1,2,3, Changjun Zeng1,2,4, Benjamin Tschudy-Seney1,2, Ngoc Tue Nguyen1,2, Jong Ryeol Eun1,2,5, Yanling Zhang1,2,6, Rajendra Ramsamooj7, Yanghong Zhang7, Min Zhao8, Neil D Theise9, Huaijun Zhou10, Mark A Zern1,2, Yuyou Duan1,2,8.   

Abstract

A large number of cancer stem cells (CSCs) have been isolated and identified; however, none has been cultured in an unlimited manner in vitro without losing tumorigenicity and multipotency. In this study, we successfully clonogenically cultured a newly identified CD34+ liver CSC (LCSC) on feeder cells up to 22 passages (to date) without losing CSC property. Cloned CD34+ LCSC formed a round packed morphology and it could also be cryopreserved and recultured. Stem cell markers, CD34, CD117, and SOX2; normal liver stem cell markers, alpha fetoprotein, CK19, CK18, and OV6; putative CSC markers, CD44, CD133, EpCAM, and CD90; as well as CD31 were expressed in cloned CD34+ LCSC. SOX2 was the major factor in maintaining this LCSC before colonization, and interestingly, OCT4, SOX2, NAONG, Klf4, c-Myc, and Lin28 were upregulated in association with symmetric self-renewal for colony growth of CD34+ LCSC on feeder cells. Gene expression patterns of in vitro differentiation were consistent with our in vivo finding; furthermore, the tumorigenicity of cloned CD34+ LCSC was not different from uncloned CD34+ LCSC sorted from parental PLC. These results show that our cloned CD34+ LCSC maintained CSC property, including self-renewal, bipotency, and tumorigenicity after long-term culture, demonstrating that this LCSC can be cultured in an unlimited manner in vitro. Thus, establishing pure population of CSCs isolated from the patients will provide an opportunity to explore the mechanisms of tumorigenesis and cancer development, and to identify unique biomarkers presenting potential indicators of drug efficacy against CSCs for establishment of a novel strategy for cancer therapy.

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Year:  2015        PMID: 25867583      PMCID: PMC4499771          DOI: 10.1089/scd.2015.0022

Source DB:  PubMed          Journal:  Stem Cells Dev        ISSN: 1547-3287            Impact factor:   3.272


  34 in total

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  5 in total

1.  Hepatocyte selection medium-enriched hepatocellular carcinoma cells are positive for α-fetoprotein and CD44.

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2.  CD34(+) Liver Cancer Stem Cells Were Formed by Fusion of Hepatobiliary Stem/Progenitor Cells with Hematopoietic Precursor-Derived Myeloid Intermediates.

Authors:  Changjun Zeng; Yanling Zhang; Su Cheol Park; Jong Ryeol Eun; Ngoc Tue Nguyen; Benjamin Tschudy-Seney; Yong Jin Jung; Neil D Theise; Mark A Zern; Yuyou Duan
Journal:  Stem Cells Dev       Date:  2015-08-19       Impact factor: 3.272

Review 3.  Advances in Liver Cancer Stem Cell Isolation and their Characterization.

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Journal:  Stem Cell Rev Rep       Date:  2021-01-11       Impact factor: 5.739

4.  CWP232228 targets liver cancer stem cells through Wnt/β-catenin signaling: a novel therapeutic approach for liver cancer treatment.

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Journal:  Oncotarget       Date:  2016-04-12

Review 5.  CD34 Over-Expression is Associated With Gliomas' Higher WHO Grade.

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  5 in total

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