Technologies

time icon March 14, 2017

Ligands for Improved Angiogenesis and Endothelialization of Blood Contacting Devices

Technology description

Thrombus formation is a common cause of failure for blood-contacting medical devices. In most cases, RGD-based short peptide ligands have been used to reduce protein adhesion and enhance endothelial cell (EC) and endothelial progenitor (EPC) recruitment. These ligands, however, are non-specific and strongly bind platelets. Therefore there is a need for alternative ligands that can specifically target and promote endothelial function while resisting thrombosis and blood coagulation.

Researchers at the University of California, Davis have discovered novel endothelial targeting ligands that can specifically bind and capture ECs and EPCs for improved endothelialization and angiogenesis of medical devices and scaffolds. These ligands bind specifically to ECs and EPCs derived from native blood vessels and circulation. They are structurally stable and easy to chemically modify without compromising binding affinity to targeted cell surface molecules. These ligands offer novel therapeutic potential for vascular, intravascular, blood contacting and tissue engineering applications.

Researchers at the University of California, Davis have discovered novel targeting ligands that can specifically bind and capture endothelial cells and endothelial progenitors for improved endothelialization and angiogenesis of medical devices and scaffolds.



Related Cases

2016-375-0

Application area

  • EC/EPC related biomedical applications
  • Cell delivery
  • Cell culture
  • Blood-contacting medical devices
  • Scaffolds used in tissue engineering

Advantages

  • EC and EPC binding specificity
  • Does not bind monocytes or platelets
  • Structural stability
  • Easily used for chemical modification without compromising binding affinity to targeted cell surface molecules

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More information

Categories
  • Cardiology
  • Information technology
Keywords:

reduce protein adhesion

compromising binding affinity

tissue engineering applications

enhance endothelial cell

promote endothelial function

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