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Structural characterization of anti-CCL5 activity of the tick salivary protein Evasin-4

JBC. 2020-08; 
Stepan S. Denisov, Mercedes Ramírez-Escudero, Alexandra C.A. Heinzmann, Johannes H. Ippel3, Philip E Dawson, Rory R. Koenen, Tilman M. Hackeng, Bert J.C. Janssen6 and Ingrid Dijkgraaf
Products/Services Used Details Operation
Gene Synthesis Recombinant met-CXCL4 was obtained from Dr. R. Koenen. The met-Evasin-4 pET30a, His6-SUMO-Evasin-4 pET23a and E66S MKKKWPR-CCL5 pET24a vectors (Table S1) were purchased from GenScript, USA Get A Quote

摘要

Ticks, as blood sucking parasites, have developed a complex strategy to evade and suppress host immune responses during feeding. The crucial part of this strategy is expression of a broad family of salivary proteins, called Evasins, to neutralize chemokines responsible for cell trafficking and recruitment. However, structural information about Evasins is still scarce and little is known about the structural determinants of their binding mechanism to chemokines. Here, we studied the structurally uncharacterized Evasin-4, which neutralizes a broad range of CC-motif chemokines, including the chemokine CC-motif ligand 5 (CCL5) involved in atherogenesis. Crystal structures of Evasin-4 and E66S CCL5—an obligatory d... More

关键词

Ticks, parasite, protein structure, protein-protein interaction, immunosuppressor, chemokine X-ray, crystallography nuclear magnetic resonance (NMR)