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Immortalization without neoplastic transformation of human mesenchymal stem cells by transduction with HPV16E6/E7 genes

Authors :
Shih-Chieh Hung
Jih Shiuan Wang
Larry L.T. Ho
Wen-Kuang Yang
Ching-Fang Chang
Ruey-Jen Lin
Den Mei Yang
Source :
International Journal of Cancer. 110:313-319
Publication Year :
2004
Publisher :
Wiley, 2004.

Abstract

hMSCs derived from bone marrow are useful as a species-specific cell culture system for studying cell lineage differentiation and tissue remodeling. However, hMSCs usually have a short in vitro life span due to replicative senescence. We therefore used a high dose of retroviral vector LXSN-16E6E7 to transduce hMSCs of an aging donor and obtained an actively proliferating cell line, designated KP-hMSCs, which expressed HPV16 E6/E7 mRNA. Whereas parental hMSCs ceased to grow after 30 PDs, KP-hMSCs could be propagated beyond 100 PDs. With culture procedures to avoid selection pressure and crowded cell growth, KP-hMSCs showed no signs of neoplastic transformation as examined by soft-agar anchorage-independent growth and NOD-SCID mouse tumorigenicity assays. KP-hMSCs gave similar cytofluorimetric profiles of 31 CD markers to those of the parental primary hMSCs, except with some morphologic changes and expansion of an originally very minor CD34(dim)CD38(+)CD50+ cell population. Upon exposure to specific stimulating conditions in vitro, KP-hMSCs could respond and differentiate along the mesenchymal (bone, fat and cartilage) and nonmesenchymal (neuron) cell lineages. Our results indicated that hMSCs could be immortalized by transduction with HPV16 E6/E7, maintained without neoplastic transformation by careful culture procedures and thus useful for stem cell research and clinical application.

Details

ISSN :
10970215 and 00207136
Volume :
110
Database :
OpenAIRE
Journal :
International Journal of Cancer
Accession number :
edsair.doi.dedup.....82a739d239a7acf16a675eb85d42eabb
Full Text :
https://doi.org/10.1002/ijc.20126