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Design and analysis of EphA2-SAM peptide ligands: A multi-disciplinary screening approach

Academic Article
Publication Date:
2019
abstract:
EphA2 receptor plays a critical and debatable function in cancer and is considered a target in drug discovery. Lately, there has been a growing interest in its cytosolic C-terminal SAM domain (EphA2-SAM) as it engages protein modulators of receptor endocytosis and stability. Interestingly, EphA2-SAM binds the SAM domain from the lipid phosphatase Ship2 (Ship2-SAM) mainly producing pro-oncogenic outcomes. In an attempt to discover novel inhibitors of the EphA2-SAM/Ship2-SAM complex with possible anticancer properties, we focused on the central region of Ship2-SAM (known as Mid-Loop interface) responsible for its binding to EphA2-SAM. Starting from the amino acid sequence of the Mid-Loop interface virtual peptide libraries were built through ad hoc inserted mutations with either L- or D- amino acids and screened against EphA2-SAM by docking techniques. A few virtual hits were synthesized and experimentally tested by a variety of direct and competition-type interaction assays relying on NMR (Nuclear Magnetic Resonance), SPR (Surface Plasmon Resonance), MST (Microscale Thermophoresis) techniques. These studies guided the discovery of an original EphA2-SAM ligand antagonist of its interaction with Ship2-SAM.
Iris type:
01.01 Articolo in rivista
Keywords:
SAM domains; Virtual screening; NMR; SPR; MST; EphA2; Ship2; Cancer
List of contributors:
Leone, Marilisa; Pedone, EMILIA MARIA; DE LUCA, Stefania; Pirone, Luciano
Authors of the University:
DE LUCA STEFANIA
LEONE MARILISA
PEDONE EMILIA MARIA
PIRONE LUCIANO
Handle:
https://iris.cnr.it/handle/20.500.14243/392000
Published in:
BIOORGANIC CHEMISTRY (PRINT)
Journal
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