Expansion of primary human hepatocyte populations by retroviral gene transfer and adenovirus-mediated CRE/LOXP site-specific recombination

N. Kobayashi; H. Noguchi; T. Fujiwara; N. Tanaka; K. A. Westerman; P. Leboulch

doi:10.1097/00002480-200003000-00314

Expansion of primary human hepatocyte populations by retroviral gene transfer and adenovirus-mediated CRE/LOXP site-specific recombination

N. Kobayashi, H. Noguchi, T. Fujiwara, N. Tanaka, K. A. Westerman, P. Leboulch

Research output: Contribution to journal › Conference article › peer-review

Abstract

Human primary hepatocytes are ideal for bioartificial liver (BAL), however, the shortage of human livers available for hepatocyte isolation severely limits the use of this modality. To resolve this issue, adult human hepatocytes were immortalized with a retrovector containing the genes encoding Simian virus 40 T antigen flanked by a pair of Ioxp recombination target that was subsequently excised by Cre recombinase. Based on the observations, a reversible immortalization system in primary adult human hepatocytes was established.

Original language	English
Number of pages	1
Journal	ASAIO Journal
Volume	46
Issue number	2
DOIs	https://doi.org/10.1097/00002480-200003000-00314
Publication status	Published - Jan 1 2000
Event	46th Annual Conference and Exposition of ASAIO - New York, NY, USA Duration: Jun 28 2000 → Jul 1 2000

ASJC Scopus subject areas

Biophysics
Bioengineering
Biomaterials
Biomedical Engineering

Access to Document

10.1097/00002480-200003000-00314

Cite this

@article{9704d735fdf74f829a27955d4fa001e0,

title = "Expansion of primary human hepatocyte populations by retroviral gene transfer and adenovirus-mediated CRE/LOXP site-specific recombination",

abstract = "Human primary hepatocytes are ideal for bioartificial liver (BAL), however, the shortage of human livers available for hepatocyte isolation severely limits the use of this modality. To resolve this issue, adult human hepatocytes were immortalized with a retrovector containing the genes encoding Simian virus 40 T antigen flanked by a pair of Ioxp recombination target that was subsequently excised by Cre recombinase. Based on the observations, a reversible immortalization system in primary adult human hepatocytes was established.",

author = "N. Kobayashi and H. Noguchi and T. Fujiwara and N. Tanaka and Westerman, {K. A.} and P. Leboulch",

year = "2000",

month = jan,

day = "1",

doi = "10.1097/00002480-200003000-00314",

language = "English",

volume = "46",

journal = "ASAIO Journal",

issn = "1058-2916",

publisher = "Lippincott Williams and Wilkins",

number = "2",

note = "46th Annual Conference and Exposition of ASAIO ; Conference date: 28-06-2000 Through 01-07-2000",

}

TY - JOUR

T1 - Expansion of primary human hepatocyte populations by retroviral gene transfer and adenovirus-mediated CRE/LOXP site-specific recombination

AU - Kobayashi, N.

AU - Noguchi, H.

AU - Fujiwara, T.

AU - Tanaka, N.

AU - Westerman, K. A.

AU - Leboulch, P.

PY - 2000/1/1

Y1 - 2000/1/1

N2 - Human primary hepatocytes are ideal for bioartificial liver (BAL), however, the shortage of human livers available for hepatocyte isolation severely limits the use of this modality. To resolve this issue, adult human hepatocytes were immortalized with a retrovector containing the genes encoding Simian virus 40 T antigen flanked by a pair of Ioxp recombination target that was subsequently excised by Cre recombinase. Based on the observations, a reversible immortalization system in primary adult human hepatocytes was established.

AB - Human primary hepatocytes are ideal for bioartificial liver (BAL), however, the shortage of human livers available for hepatocyte isolation severely limits the use of this modality. To resolve this issue, adult human hepatocytes were immortalized with a retrovector containing the genes encoding Simian virus 40 T antigen flanked by a pair of Ioxp recombination target that was subsequently excised by Cre recombinase. Based on the observations, a reversible immortalization system in primary adult human hepatocytes was established.

UR - http://www.scopus.com/inward/record.url?scp=0034158726&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=0034158726&partnerID=8YFLogxK

U2 - 10.1097/00002480-200003000-00314

DO - 10.1097/00002480-200003000-00314

M3 - Conference article

AN - SCOPUS:0034158726

SN - 1058-2916

VL - 46

JO - ASAIO Journal

JF - ASAIO Journal

IS - 2

T2 - 46th Annual Conference and Exposition of ASAIO

Y2 - 28 June 2000 through 1 July 2000

ER -

Expansion of primary human hepatocyte populations by retroviral gene transfer and adenovirus-mediated CRE/LOXP site-specific recombination

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this