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Cell-type-restricted anti-cytokine therapy: TNF inhibition from one pathogenic source.

Proc. Natl. Acad. Sci. U.S.A.. 2016-09; 
EfimovGrigory A,KruglovAndrei A,KhlopchatnikovaZoya V,RozovFedor N,MokhonovVladislav V,Rose-JohnStefan,SchellerJürgen,GordonSiamon,StaceyMartin,DrutskayaMarina S,TillibSergei V,NedospasovSerg
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Mammalian Expression System Sequence coding for the extracellular part of F4/80 flanked at both N and C termini with affinity tags was codon-optimized for mammalian expression, synthesized by GenScript, and subcloned into pOptiVec vector (Invitrogen). Get A Quote

摘要

Overexpression of TNF contributes to pathogenesis of multiple autoimmune diseases, accounting for a remarkable success of anti-TNF therapy. TNF is produced by a variety of cell types, and it can play either a beneficial or a deleterious role. In particular, in autoimmunity pathogenic TNF may be derived from restricted cellular sources. In this study we evaluated the feasibility of cell-type-restricted TNF inhibition in vivo. To this end, we engineered MYSTI (Myeloid-Specific TNF Inhibitor)--a recombinant bispecific antibody that binds to the F4/80 surface molecule on myeloid cells and to human TNF (hTNF). In macrophage cultures derived from TNF humanized mice MYSTI could capture the secreted hTNF, lim... More

关键词

TNF,anti-cytokine therapy,autoimmunity,bispecific antibody,humanized