| Literature DB >> 25921529 |
Onofrio Zirafi1, Kyeong-Ae Kim1, Ludger Ständker2, Katharina B Mohr1, Daniel Sauter1, Anke Heigele1, Silvia F Kluge1, Eliza Wiercinska3, Doreen Chudziak3, Rudolf Richter4, Barbara Moepps5, Peter Gierschik5, Virag Vas6, Hartmut Geiger6, Markus Lamla7, Tanja Weil7, Timo Burster8, Andreas Zgraja9, Francois Daubeuf10, Nelly Frossard10, Muriel Hachet-Haas11, Fabian Heunisch12, Christoph Reichetzeder12, Jean-Luc Galzi11, Javier Pérez-Castells13, Angeles Canales-Mayordomo14, Jesus Jiménez-Barbero14, Guillermo Giménez-Gallego14, Marion Schneider15, James Shorter16, Amalio Telenti17, Berthold Hocher12, Wolf-Georg Forssmann18, Halvard Bonig3, Frank Kirchhoff19, Jan Münch20.
Abstract
CXCL12-CXCR4 signaling controls multiple physiological processes and its dysregulation is associated with cancers and inflammatory diseases. To discover as-yet-unknown endogenous ligands of CXCR4, we screened a blood-derived peptide library for inhibitors of CXCR4-tropic HIV-1 strains. This approach identified a 16 amino acid fragment of serum albumin as an effective and highly specific CXCR4 antagonist. The endogenous peptide, termed EPI-X4, is evolutionarily conserved and generated from the highly abundant albumin precursor by pH-regulated proteases. EPI-X4 forms an unusual lasso-like structure and antagonizes CXCL12-induced tumor cell migration, mobilizes stem cells, and suppresses inflammatory responses in mice. Furthermore, the peptide is abundant in the urine of patients with inflammatory kidney diseases and may serve as a biomarker. Our results identify EPI-X4 as a key regulator of CXCR4 signaling and introduce proteolysis of an abundant precursor protein as an alternative concept for chemokine receptor regulation.Entities:
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Year: 2015 PMID: 25921529 DOI: 10.1016/j.celrep.2015.03.061
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423