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Impact of Survivin Acetylation on its Biological Function [Paperback]

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  • Category: Books (Medical)
  • Author:  Dannheisig, David
  • Author:  Dannheisig, David
  • ISBN-10:  3658186224
  • ISBN-10:  3658186224
  • ISBN-13:  9783658186227
  • ISBN-13:  9783658186227
  • Publisher:  Springer Spektrum
  • Publisher:  Springer Spektrum
  • Binding:  Paperback
  • Binding:  Paperback
  • Pub Date:  01-Apr-2017
  • Pub Date:  01-Apr-2017
  • SKU:  3658186224-11-SPRI
  • SKU:  3658186224-11-SPRI
  • Item ID: 100970793
  • List Price: $54.99
  • Seller: ShopSpell
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  • Delivery by: Jan 21 to Jan 23
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In his research, David Dannheisig investigates the influence of lysine129 acetylation on the biological function of survivin including alteration of nucleocytoplasmic shuttling as well as dimerization behavior. Since survivin participates in two major hallmarks of oncogenesis, namely cell death inhibition and chromosomal segregation during the cell cycle, it reflects a valuable target in cancer therapy and research. The author establishes proximity-dependent, fluorescence-microscopic methods to quantify the interaction of survivin with the export receptor Crm1 as well as the homodimerization itself. In the future, those systems can be used to examine the feasible effect of chemical modulators which are targeting these interactions in a cellular background. The outcome achieved is an essential step towards the enhancement of potential cancer therapies.

Apoptosis  The Programmed Suicide.- Cancer  The Enemy Inside.- Nucleocytoplasmic Transport Cellular Navigation.- Biological Function of Survivin.- Protein modification  Make-Up for Proteins.- Cell cycle  Virchows Heritage.

David Dannheisig currently is a student of the International Graduate School in Molecular Medicine (IGradU) pursuing his PhD (Dr. rer. nat) degree at the Institute of Biochemistry and Molecular Biology (iBMB) at Ulm University, Germany.

In his research, David Dannheisig investigates the influence of lysine129 acetylation on the biological function of survivin including alteration of nucleocytoplasmic shuttling as well as dimerization behavior. Since survivin participates in two major hallmarks of oncogenesis, namely cell death inhibition and chromosomal segregation during the cell cycle, it reflects a valuable target in cancer therapy and research. The author establishes proximity-dependent, fluorescence-microscopic methods to quantify the interaction of survivin with the export receptor Crm1 as well as the homodimerizatioló
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