A3(人T淋巴細(xì)胞白血病細(xì)胞)
CBP60703
                       
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                | I. General information | |
| Synonyms: | A3 | 
| Background: | The A3 subclone was derived from a Jurkat cell line obtained from the laboratory of Gerald Crabtree at Stanford University. | 
| Species: | Homo sapiens, human | 
| Disease: | acute T cell leukemia | 
| Gender: | male | 
| Morphology: | lymphoblast | 
| Growth Mode: | suspension | 
| DNA Profile: | Amelogenin: X,Y CSF1PO: 11,12 D13S317: 8,11 D16S539: 11 D5S818: 9 D7S820: 8,10 THO1: 6,9.3 TPOX: 8,10 vWA: 17,18 Our Cell Line Authentication Service | 
| Culture Medium: | RPMI-1640 +10%FBS A3完全培養(yǎng)基,# CBP60703M | 
| Cryopreservation medium: | 90%FBS+10%DMSO | 
| Comments: | The Jurkat cells were treated with Fas Antibody and isolated by limiting dilution to obtain a cell line that had a low spontaneous rate of resistance to Fas-medicated apoptosis.The resulting wild-type A3 subclone is very sensitive to Fas-mediated apoptosis.Wild-type A3 cells were made neomycin resistant and treated with three cycles of exposure to the frameshifting mutagen ICR-191 to isolate clones harboring recessive mutations that were resistant to killing by Fas antibody. ICR-191 treated clones were serially diluted in 96-well plates in the presence of Fas Antibody for 3 to 5 weeks.Two of these ICR-191 treated clones have been deposited at the ATCC. They are I 9.2 (ATCC CRL-2571), a clone with a mutation in the cysteine protease caspase-8/FLICE and I 2.1 (ATCC CRL-2572), a clone with a mutation in the adaptor FADD. For more information, please contact us (4008-750-250). | 
 
            
 
             
             
         
             
             
             
             
             
             
            