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[Gene-transfer into bone marrow cells]

Authors :
Y, Takahara
K, Hamada
A, Okano
T, Takagi
K, Shimotono
Source :
Human cell. 4(1)
Publication Year :
1991

Abstract

We have intended to improve gene-transfer technique into hematopoietic stem cells for somatic gene therapy. 1) We have developed a new packaging cell line, ampGPE for retroviral production. LTR-less gag, pol or env genes from Moloney murine leukemia virus were separately inserted into BMGNeo vector. Packaging cell lines containing 20-50 copies of these two kinds of plasmid were obtained. Retrovirus stock for gene-transfer have been produced at a high titer (10(5)-10(6) cfu/ml) and without replication-competent viruses by using ampGPE. 2) Retrovirus-transduced murine CFU-GM have been found to selectively proliferate (5-10 fold/week) in liquid capture with recombinant murine IL-3, human IL-6 and G418 to consequently obtain enough amount of, highly concentrated (70-100%), and gene-transferred murine CFU-GM for gene-delivery system.

Details

ISSN :
09147470
Volume :
4
Issue :
1
Database :
OpenAIRE
Journal :
Human cell
Accession number :
edsair.pmid..........7dea7083bb37de4ea00c7f1d987c8999