BOSC23

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BOSC 23 is a human kidney cell line developed by Warren Pear in David Baltimore's lab [1] that was derived from the 293T cell line. [2] [3] The main use of BOSC 23 is the production of recombinant retroviruses; it stably expresses Moloney murine leukemia virus proteins and when transiently transfected with recombinant retroviral vector DNA, produces high titers of infectious retroviral particles. The cell line does not produce detectable replication-competent virus, an important safety feature.[ citation needed ]

BOSC 23 carries neomycin/G418 resistance derived from its parental line 293T, and also hygromycin and mycophenolic acid (gpt) resistance. It should be maintained under gpt selection.[ citation needed ]

This cell line is a model for cancer research, with emphasis on the lack of activated Src protein. [4]

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Human embryonic kidney 293 cells, also often referred to as HEK 293, HEK-293, 293 cells, or less precisely as HEK cells, are a specific immortalised cell line derived from a spontaneously miscarried or aborted fetus or human embryonic kidney cells grown in tissue culture taken from a female fetus in 1973.

<span class="mw-page-title-main">Recombinant DNA</span> DNA molecules formed by human agency at a molecular level generating novel DNA sequences

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<span class="mw-page-title-main">Endogenous retrovirus</span> Inherited retrovirus encoded in an organisms genome

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Transient expression, more frequently referred to "transient gene expression", is the temporary expression of genes that are expressed for a short time after nucleic acid, most frequently plasmid DNA encoding an expression cassette, has been introduced into eukaryotic cells with a chemical delivery agent like calcium phosphate (CaPi) or polyethyleneimine (PEI). However, unlike "stable expression," the foreign DNA does not fuse with the host cell DNA, resulting in the inevitable loss of the vector after several cell replication cycles. The majority of transient gene expressions are done with cultivated animal cells. The technique is also used in plant cells; however, the transfer of nucleic acids into these cells requires different methods than those with animal cells. In both plants and animals, transient expression should result in a time-limited use of transferred nucleic acids, since any long-term expression would be called "stable expression."

Garry P. Nolan is an American immunologist, academic, inventor, and business executive. He holds the Rachford and Carlota A. Harris Professor Endowed Chair in the Department of Pathology at Stanford University School of Medicine. Nolan founded biotechnology companies, wrote numerous medical research papers, and has been active in ufology.

References

  1. "BOSC 23 cell line".
  2. Pear WS, Nolan GP, Scott ML, Baltimore D (15 Sep 1993). "Production of high-titer helper-free retroviruses by transient transfection". Proc. Natl. Acad. Sci. USA. 90 (18): 8392–8396. Bibcode:1993PNAS...90.8392P. doi: 10.1073/pnas.90.18.8392 . PMC   47362 . PMID   7690960.
  3. Baker, Andrew H. (1 February 2008). Vascular Disease: Molecular Biology and Gene Transfer Protocols. Springer Science & Business Media. ISBN   978-1-59259-247-0.
  4. Goh YM, Cinghu S, Hong ETH et al. Src kinase phosphorylates RUNX3 at tyrosine residues and localizes the protein in the cytoplasm. The Journal of Biochemistry vol.285, no.13, pp.10122-10129, March 2010
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