| Literature DB >> 27856797 |
Daniel F Ortiz1, Jonathan C Lansing1, Laura Rutitzky1, Elma Kurtagic1, Thomas Prod'homme1, Amit Choudhury1, Nathaniel Washburn1, Naveen Bhatnagar1, Christopher Beneduce1, Kimberly Holte1, Robert Prenovitz1, Matthew Child1, Jason Killough1, Steven Tyler1, Julia Brown1, Stephanie Nguyen1, Inessa Schwab2, Maurice Hains1, Robin Meccariello1, Lynn Markowitz1, Jing Wang1, Radouane Zouaoui1, Allison Simpson1, Birgit Schultes1, Ishan Capila1, Leona Ling1, Falk Nimmerjahn2, Anthony M Manning1, Carlos J Bosques3.
Abstract
Autoantibody immune complex (IC) activation of Fcγ receptors (FcγRs) is a common pathogenic hallmark of multiple autoimmune diseases. Given that the IC structural features that elicit FcγR activation are poorly understood and the FcγR system is highly complex, few therapeutics can directly block these processes without inadvertently activating the FcγR system. To address these issues, the structure activity relationships of an engineered panel of multivalent Fc constructs were evaluated using sensitive FcγR binding and signaling cellular assays. These studies identified an Fc valency with avid binding to FcγRs but without activation of immune cell effector functions. These observations directed the design of a potent trivalent immunoglobulin G-Fc molecule that broadly inhibited IC-driven processes in a variety of immune cells expressing FcγRs. The Fc trimer, Fc3Y, was highly efficacious in three different animal models of autoimmune diseases. This recombinant molecule may represent an effective therapeutic candidate for FcγR-mediated autoimmune diseases.Entities:
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Year: 2016 PMID: 27856797 DOI: 10.1126/scitranslmed.aaf9418
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956