CDK2 Phosphorylation on Threonine39 by AKT and Its Implication on Cyclin Binding, Cellular Localization, and Cell Cycle Progression

Abstract

One of the hallmarks of cancer is the deregulation of the cell proliferation. This deregulation promotes genetic errors that contribute to genomic instability. Our hypothesis is that Cdk2 exists in two freely exchangeable conformations: that seen in the active, cyclin bound crystal and that of the inactive monomeric Cdk2, with the latter predominating in the absence of cyclin. We propose that phosphorylation of Cdk2T39 shifts the equilibrium in the direction of the active conformation that best fits cyclin and therefore facilitating cyclin binding, G1 progression and initiation of DNA synthesis. We will test this hypothesis by treating recombinant cdk2 with AKT and sending it for mass spectroscopy so we can determine if Cdk2 is indeed phosphorylated by AKT. We will also determine the effect of AKT phosphorylation on Cdk2 by constructing a phosphomimetic mutant of Cdk2 and determining if this has an effect on cyclin binding and G1 progression. Ultimately, this research may elucidate a novel method of cell cycle control through which mitogenic signals may influence the cell cycle.

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Document Details

Document Type
Technical Report
Publication Date
Oct 01, 2007
Accession Number
ADA490431

Entities

People

  • Thiago Da Silva

Organizations

  • University of Miami

Tags

DTIC Thesaurus Topics

  • Biomedical Research
  • Blood Coagulation Factors
  • Cancer
  • Cell Division
  • Cell Line
  • Cell Physiological Processes
  • Cells
  • Department Of Defense
  • Electronic Mail
  • Fungi
  • Information Operations
  • Kinases
  • Mass Spectroscopy
  • Phosphorylation
  • Proteins
  • Recombinant Proteins
  • Tumor Cell Line

Fields of Study

  • Biology

Readers

  • Breast cancer cell signaling and growth regulation.
  • Molecular Biology and Genetics

Technology Areas

  • Biotechnology