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Increased yields and biological potency of knob-into-hole-based soluble MHC class II molecules

Nat Commun.. 2019; 
Serra P1, Garabatos N2, Singha S3, Fandos C2, Garnica J2, Solé P2, Parras D2, Yamanouchi J3, Blanco J2,4, Tort M2, Ortega M2, Yang Y3,5, Ellestad KK3, Santamaria P6,7.
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Peptide Synthesis The biotinylated molecules were then loaded with peptide by incubation with a 10-fold molar excess of PDC-E2122–135 (Tebu-bio), PDC-E2249–262 (Tebu-bio), and IGRP13–25 (Genscript) in 100 mM NaPO4 pH 6.0, 0.2% n-octyl-d-glucopyranoside (Sigma-Aldrich) and 1 mg/ml Pefabloc® (Sigma-Aldrich) for 72 h at 37 °C. Get A Quote

摘要

Assembly of soluble peptide-major histocompatibility complex class II (pMHCII) monomers into multimeric structures enables the detection of antigen-specific CD4+ T cells in biological samples and, in some configurations, their reprogramming in vivo. Unfortunately, current MHCII-αβ chain heterodimerization strategies are typically associated with low production yields and require the use of foreign affinity tags for purification, precluding therapeutic applications in humans. Here, we show that fusion of peptide-tethered or empty MHCII-αβ chains to the IgG1-Fc mutated to form knob-into-hole structures results in the assembly of highly stable pMHCII monomers. This design enables the expression and rapid purif... More

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