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Retinoblastoma protein co-purifies with proteasomal insulin-degrading enzyme: Implications for cell proliferation control |
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| Authors: | Razvan T Radulescu William C Duckworth Janet Fawcett |
| Institution: | a Molecular Concepts Research (MCR), Muenster, Germany b Department of Medicine, Phoenix VA Health Care System, Phoenix, AZ, USA c Research Service, Phoenix VA Health Care System, Phoenix, AZ, USA |
| Abstract: | Previous investigations on proteasomal preparations containing insulin-degrading enzyme (IDE; EC 3.4.24.56) have invariably yielded a co-purifying protein with a molecular weight of about 110 kDa. We have now found both in MCF-7 breast cancer and HepG2 hepatoma cells that this associated molecule is the retinoblastoma tumor suppressor protein (RB). Interestingly, the amount of RB in this protein complex seemed to be lower in HepG2 vs. MCF-7 cells, indicating a higher (cytoplasmic) protein turnover in the former vs. the latter cells. Moreover, immunofluorescence showed increased nuclear localization of RB in HepG2 vs. MCF-7 cells. Beyond these subtle differences between these distinct tumor cell types, our present study more generally suggests an interplay between RB and IDE within the proteasome that may have important growth-regulatory consequences. |
| Keywords: | CDKs cyclin-dependent kinases RB retinoblastoma tumor suppressor protein IDE insulin-degrading enzyme FCS fetal calf serum PBSCM PBS containing 1 mM CaCl2 and 1 mM MgCl2 |
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