Literature DB >> 10933966

CD34 splice variant: an attractive marker for selection of gene-modified cells.

B Fehse1, A Richters, K Putimtseva-Scharf, H Klump, Z Li, W Ostertag, A R Zander, C Baum.   

Abstract

This study presents a promising selection system for gene-modified cells other than human hematopoietic progenitor and endothelial cells based on transgenic expression of human CD34. Three retrovirally transduced variants of CD34 were compared, differing in the length of their cytoplasmic domains. These were the full-length transmembrane protein (flCD34), a truncated form (tCD34) that is found as a naturally occurring splice variant and has a partial deletion of the cytoplasmic domain for signal transduction, and an engineered variant which is completely deprived of its cytoplasmic tail (dCD34). All three variants allowed selection of gene-modified cells using commercially available immunoaffinity technology. However, examination by flow cytometry as well as by Southern, Northern, and Western blot revealed that dCD34, as opposed to tCD34, is not stably anchored in the membrane and thus is expressed at low levels on the surface of transduced cells. Therefore, tCD34 was chosen as the more promising candidate for a clinically applicable cell surface marker. We show that gene-modified human primary T lymphocytes expressing tCD34 can be enriched to high purity (>95%) using clinically approved immunoaffinity columns. In addition, we demonstrate the utility of tCD34 for surface marking of murine hematopoietic cells in vivo, including primary T lymphocytes detected 9 weeks after bone marrow transplantation.

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Year:  2000        PMID: 10933966     DOI: 10.1006/mthe.2000.0068

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  24 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2015-02-04       Impact factor: 11.205

3.  A transgene-encoded cell surface polypeptide for selection, in vivo tracking, and ablation of engineered cells.

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4.  Analysis of transgene-specific immune responses that limit the in vivo persistence of adoptively transferred HSV-TK-modified donor T cells after allogeneic hematopoietic cell transplantation.

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Review 5.  Contributions of gene marking to cell and gene therapies.

Authors:  Cecilia N Barese; Cynthia E Dunbar
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6.  Magnetic-activated cell sorting of TCR-engineered T cells, using tCD34 as a gene marker, but not peptide-MHC multimers, results in significant numbers of functional CD4+ and CD8+ T cells.

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7.  CD34-based enrichment of genetically engineered human T cells for clinical use results in dramatically enhanced tumor targeting.

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Journal:  Gene Ther       Date:  2016-05-19       Impact factor: 5.250

9.  Genetic control of wayward pluripotent stem cells and their progeny after transplantation.

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10.  Gamma-retroviral vector design for the co-expression of artificial microRNAs and therapeutic proteins.

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Journal:  Nucleic Acid Ther       Date:  2014-07-14       Impact factor: 5.486

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