Immortalization of human CD8+ T cell clones by ectopic expression of telomerase reverse transcriptase
E Hooijberg, JJ Ruizendaal, PJF Snijders… - The Journal of …, 2000 - journals.aai.org
E Hooijberg, JJ Ruizendaal, PJF Snijders, EWM Kueter, JMM Walboomers, H Spits
The Journal of Immunology, 2000•journals.aai.orgReplicative senescence of T cells is correlated with erosion of telomere ends. Telomerase
plays a key role in maintaining telomere length. Therefore, it is thought that telomerase
regulates the life span of T cells. To test this hypothesis, we have over-expressed human
telomerase reverse transcriptase in human CD8+ T cells. Ectopic expression of human
telomerase reverse transcriptase led to immortalization of these T cells, without altering the
phenotype and without loss of specificity or functionality. As the T cells remained dependent …
plays a key role in maintaining telomere length. Therefore, it is thought that telomerase
regulates the life span of T cells. To test this hypothesis, we have over-expressed human
telomerase reverse transcriptase in human CD8+ T cells. Ectopic expression of human
telomerase reverse transcriptase led to immortalization of these T cells, without altering the
phenotype and without loss of specificity or functionality. As the T cells remained dependent …
Abstract
Replicative senescence of T cells is correlated with erosion of telomere ends. Telomerase plays a key role in maintaining telomere length. Therefore, it is thought that telomerase regulates the life span of T cells. To test this hypothesis, we have over-expressed human telomerase reverse transcriptase in human CD8+ T cells. Ectopic expression of human telomerase reverse transcriptase led to immortalization of these T cells, without altering the phenotype and without loss of specificity or functionality. As the T cells remained dependent on cytokines and Ag stimulation for their in vitro expansion, we conclude that immortalization was achieved without malignant transformation.
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