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Targeting the Tie2-αvβ3 integrin axis with bi-specific reagents for the inhibition of angiogenesis.

BMC Biol. 2018; 
Shlamkovich T, Aharon L, Koslawsky D, Einav Y, Papo N.
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Custom Vector Construction The loop library was constructed with an RGD sequence flanked by three ran- dom residues on each side of the RGD motif (GenScript) and homologous recombination into Saccharomyces cerevisiae EBY100 cells , as previously described [55]. Get A Quote

摘要

Increased activity of the receptor tyrosine kinase Tie2 has been implicated in the promotion of pathological angiogenesis. This activity is mainly mediated through angiopoietin (Ang)1- and Ang2-dependent activation of integrins by Tie2, rendering the Ang/Tie2/integrin axis an attractive putative target for cancer therapeutics.,To target this axis, we developed single domain, non-immunoglobulin high-affinity bi-specific protein inhibitors against both Tie2 and αvβ3 integrin. We have previously engineered the Ang2-binding domain of Tie2 (Ang2-BD) as a Tie2 inhibitor. Here, we engineered an exposed loop in Ang2-BD to generate variants that include an integrin-binding Arg-Gly-Asp (RGD) motif and used flow cytomet... More

关键词

Angiogenesis; Bi-specific proteins; Directed evolution; Integrins; Protein engineering; Receptor tyrosine kinases