AI Article Synopsis
- Cancer cells often disrupt normal signaling that leads to cell death, making them more resilient due to factors like genomic instability and oncogene activation.
- The study focuses on the antiapoptotic protein BCL-2, which is commonly overexpressed in cancer cells, preventing apoptosis and allowing cancer survival.
- BH3 profiling was used to show that acute lymphoblastic leukemia (ALL) cells depend on BCL-2, suggesting that treatments targeting BCL-2, like ABT-737, could be effective for ALL patients in future clinical trials.
Article Abstract
Cancer cells acquire disruptions in normal signal transduction pathways and homeostatic mechanisms that would trigger apoptosis in normal cells. These abnormalities include genomic instability, oncogene activation, and growth factor independent proliferation. Therefore, cancer cells likely require a block in apoptosis in order to survive. Overexpression of the antiapoptotic protein BCL-2 provides a block in apoptosis that is frequently observed in cancer cells. We have developed methods for the detection and analysis of BCL-2 dependence and here apply them to acute lymphoblastic leukemia (ALL). BH3 profiling, a mitochondrial assay that classifies blocks in the intrinsic apoptotic pathway, indicated a dependence on BCL-2 of both ALL cell lines and primary samples. This dependence predicted that BCL-2 would be complexed with select pro-death BH3 family proteins, a prediction confirmed by the isolation of BCL-2 complexes with BIM. Furthermore, the BH3 profiling and protein analysis predicted that ALL cell lines and primary cells would be sensitive to ABT-737 as a single agent. Finally, BH3 profiling and protein studies accurately predicted a relative degree of sensitivity to BCL-2 antagonism in cell lines. The ALL cells studied exhibit BCL-2 dependence, supporting clinical trials of BCL-2 antagonists in ALL as single agents or combination therapies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2234061 | PMC |
| http://dx.doi.org/10.1182/blood-2007-06-098012 | DOI Listing |
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