Development and functional characterization of human bone marrow mesenchymal cells immortalized by enforced expression of telomerase

Development and functional characterization of human bone marrow mesenchymal cells immortalized by enforced expression of telomerase

To create immortal mesenchymal cell lines, we transduced primary human bone marrow mesenchymal cells with telomerase reverse transcriptase (TERT). TERT+ mesenchymal cells continued to grow for > 2 years; parallel TERT– cultures underwent senescence after 15 weeks. TERT+ mesenchymal cells did not...

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Veröffentlicht in:British journal of haematology 2003-03, Vol.120 (5), p.846-849
Hauptverfasser: Mihara, Keichiro, Imai, Chihaya, Coustan‐Smith, Elaine, Dome, Jeffrey S., Dominici, Massimo, Vanin, Elio, Campana, Dario
Format: Artikel
Sprache:eng
Schlagworte:
acute lymphoblastic leukaemia
Animals
Biological and medical sciences
Bone Marrow Cells - cytology
Bone Marrow Cells - enzymology
Cell Differentiation
Cell Division
Cell Line, Transformed
Cellular Senescence
DNA-Binding Proteins
haematopoiesis
Hematologic and hematopoietic diseases
Hematopoietic Stem Cells - cytology
Humans
Leukemias. Malignant lymphomas. Malignant reticulosis. Myelofibrosis
Medical sciences
mesenchymal cells
Mesoderm - cytology
Mice
Neoplasm Transplantation
Telomerase - metabolism
Tumor Cells, Cultured
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Zusammenfassung:To create immortal mesenchymal cell lines, we transduced primary human bone marrow mesenchymal cells with telomerase reverse transcriptase (TERT). TERT+ mesenchymal cells continued to grow for > 2 years; parallel TERT– cultures underwent senescence after 15 weeks. TERT+ mesenchymal cells did not form foci in soft agar, had a normal karyotype and could differentiate into osteoblasts and chondrocytes. Their capacity to support leukaemic lymphoblasts and normal CD34+ haematopoietic cells was equal to or greater than that of primary cells; 42 TERT+ mesenchymal cell clones varied in their supporting capacity. Immortalized mesenchymal cells offer a promising tool for identifying molecules that regulate human haematopoiesis.
ISSN:0007-1048
1365-2141
DOI:10.1046/j.1365-2141.2003.04217.x