Literature DB >> 9649561

Immortalization of osteoclast precursors by targeting Bcl -XL and Simian virus 40 large T antigen to the osteoclast lineage in transgenic mice.

T A Hentunen1, S V Reddy, B F Boyce, R Devlin, H R Park, H Chung, K S Selander, M Dallas, N Kurihara, D L Galson, S R Goldring, B A Koop, J J Windle, G D Roodman.   

Abstract

Cellular and molecular characterization of osteoclasts (OCL) has been extremely difficult since OCL are rare cells, and are difficult to isolate in large numbers. We used the tartrate-resistant acid phosphatase promoter to target the bcl-XL and/or Simian Virus 40 large T antigen (Tag) genes to cells in the OCL lineage in transgenic mice as a means of immortalizing OCL precursors. Immunocytochemical studies confirmed that we had targeted Bcl-XL and/or Tag to OCL, and transformed and mitotic OCL were readily apparent in bones from both Tag and bcl-XL/Tag mice. OCL formation in primary bone marrow cultures from bcl-XL, Tag, or bcl-XL/Tag mice was twofold greater compared with that of nontransgenic littermates. Bone marrow cells from bcl-XL/Tag mice, but not from singly transgenic bcl-XL or Tag mice, have survived in continuous culture for more than a year. These cells form high numbers of bone-resorbing OCL when cultured using standard conditions for inducing OCL formation, with approximately 50% of the mononuclear cells incorporated into OCL. The OCL that form express calcitonin receptors and contract in response to calcitonin. Studies examining the proliferative capacity and the resistance of OCL precursors from these transgenic mice to apoptosis demonstrated that the increased numbers of OCL precursors in marrow from bcl-XL/Tag mice was due to their increased survival rather than an increased proliferative capacity compared with Tag, bcl-XL, or normal mice. Histomorphometric studies of bones from bcl-XL/Tag mice also confirmed that there were increased numbers of OCL precursors (TRAP + mononuclear cells) present in vivo. These data demonstrate that by targeting both bcl-XL and Tag to cells in the OCL lineage, we have immortalized OCL precursors that form bone-resorbing OCL with an efficiency that is 300-500 times greater than that of normal marrow.

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Year:  1998        PMID: 9649561      PMCID: PMC509069          DOI: 10.1172/JCI2004

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  30 in total

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Review 4.  Hybridization of nucleic acids immobilized on solid supports.

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5.  The bone marrow-derived stromal cell lines MC3T3-G2/PA6 and ST2 support osteoclast-like cell differentiation in cocultures with mouse spleen cells.

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6.  DNA polymerase, thymidine kinase and DNA synthesis in erythropoietic mouse spleen cells separated on bovine serum albumin gradients.

Authors:  G D Roodman; J J Hutton; F J Bollum
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7.  Human giant cell tumors of bone identification and characterization of cell types.

Authors:  S R Goldring; M S Roelke; K K Petrison; A K Bhan
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Authors:  S Efrat; S Linde; H Kofod; D Spector; M Delannoy; S Grant; D Hanahan; S Baekkeskov
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9.  The rise and fall of apoptosis during multistage tumorigenesis: down-modulation contributes to tumor progression from angiogenic progenitors.

Authors:  P Naik; J Karrim; D Hanahan
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10.  Generation of osteoclasts from hemopoietic cells and a multipotential cell line in vitro.

Authors:  G Hattersley; T J Chambers
Journal:  J Cell Physiol       Date:  1989-09       Impact factor: 6.384

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Journal:  EMBO J       Date:  2003-12-15       Impact factor: 11.598

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9.  ADAM8 enhances osteoclast precursor fusion and osteoclast formation in vitro and in vivo.

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Review 10.  Positive and negative regulators of osteoclast apoptosis.

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  10 in total

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