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Combinatorial and computational approaches to identify interactions of macrophage colony stimulating factor (M-CSF) and its receptor c-fms.

J Biol Chem.. 2015-10;  290(43):26180-93
Rosenfeld L, Shirian J, Zur Y, Levaot N, Shifman JM, Papo N. Ben-Gurion University of the Negev, Israel.
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摘要

The molecular interactions between macrophage colony-stimulating factor (M-CSF) and the tyrosine kinase receptor c-FMS play a key role in the immune response, bone metabolism, and the development of some cancers. Because no x-ray structure is available for the human M-CSF•c-FMS complex, the binding epitope for this complex is largely unknown. Our goal was to identify the residues that are essential for binding of the human M-CSF to c-FMS. For this purpose, we used a yeast surface display (YSD) approach. We expressed a combinatorial library of monomeric M-CSF (M-CSFM) single mutants and screened this library to isolate variants with reduced affinity for c-FMS using FACS. Sequencing yielded a number of singl... More

关键词

computer modeling; directed evolution; epitope mapping; ligand-binding protein; receptor tyrosine kinase