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The bcr‐c‐abl tyrosine kinase activity is extinguished by TPA in K562 leukemia cells
[摘要]

Tyrosine kinase activity is associated with the transforming potential of several oncogenes. Human chronic myeloid leukemia (CML) cells and cell lines have been shown to contain an active bcr-c-abl p210 tyrosine kinase as a consequence of the Philadelphia chromosomal translocation. In the present work the activity of the c-abl and c-src oncogene-encoded tyrosine kinases was investigated during phorbol diester (TPA) induced differentiation of the K562 CML cells. The high tyrosine kinase activity of p210 bcr -c- abl is strongly reduced during the initial 24 h of TPA treatment. In contrast, the activity of the c-src tyrosine kinase is not changed. No change occurs in the expression of the c-abl-specific RNAs during this period. Following the reduction of bcr-c-abl kinase activity, cell proliferation is arrested and megakaryoblastic antigens appear on the cells. Sodium butyrate caused a slight decrease in growth rate and of bcr-c-abl kinase activity during erythroid differentiation whereas no changes in c-src or c-abl tyrosine kinase activities were seen in DMSO-treated control cells.

[发布日期]  [发布机构] 
[效力级别]  [学科分类] 生物化学/生物物理
[关键词] Chronic myeloid leukemia;Oncoprotein;Philadelphia chromosome;Phosphotyrosine;Tyrosine kinase;CML;chronic myeloid leukemia;DMSO;dimethyl sulfoxide;TBRS;tumor-bearing rabbit serum;TPA;12-O-tetradecanoyl phorbol-13-acetate [时效性] 
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