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A Strategy for Direct Chemical Activation of the Retinoblastoma Protein.

ACS Chem Biol.. 2016-05; 
Pye CR, Bray WM, Brown ER, Burke JR, Lokey RS, Rubin SM.
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Peptide Synthesis ... Figure 4). Synthetic E7 LxCxE (DLYCYEQLN), LIN52 (TDLEASLLSFEKLDRAphosSPDLWPE), Cyclin D (MEHQLLCCEVETIRRAY), and TMR-E2F2TD (QDDYLWGLEAGEGISDLFD) peptides were ordered from Genscript, LLC. Page 10 of 15 ACS Paragon Plus Environment ... Get A Quote

摘要

The retinoblastoma (Rb) tumor suppressor protein negatively regulates cell proliferation by binding and inhibiting E2F transcription factors. Rb inactivation occurs in cancer cells upon cyclin-dependent kinase (Cdk) phosphorylation, which induces E2F release and activation of cell cycle genes. We present a strategy for activating phosphorylated Rb with molecules that bind Rb directly and enhance affinity for E2F. We developed a fluorescence polarization assay that can detect the effect of exogenous compounds on modulating affinity of Rb for the E2F transactivation domain. We found that a peptide capable of disrupting the compact inactive Rb conformation increases affinity of the repressive Rb-E2F complex. Our r... More

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