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General Strategy For The Generation Of Human Antibody Variable Domains With Increased Aggregation Resistance.

Proc Natl Acad Sci U S A.. 2012-07;  109(27):10879 - 10884
Kip Dudgeon, Romain Rouet, Iris Kokmeijer, Peter Schofield, Jessica Stolp, David Langley, Daniela Stock, and Daniel Christ. Garvan Institute of Medical Research, 384 Victoria Street, Darlinghurst, Sydney, New South Wales 2010, Australia.
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摘要

The availability of stable human antibody reagents would be of considerable advantage for research, diagnostic, and therapeutic applications. Unfortunately, antibody variable heavy and light domains (V(H) and V(L)) that mediate the interaction with antigen have the propensity to aggregate. Increasing their aggregation resistance in a general manner has proven to be a difficult and persistent problem, due to the high level of sequence diversity observed in human variable domains and the requirement to maintain antigen binding. Here we outline such an approach. By using phage display we identified specific positions that clustered in the antigen binding site (28, 30-33, 35 in V(H) and 24, 49-53, 56 in V(L)). Intr... More

关键词

biotechnology; monoclonal antibodies; protein aggregation; protein engineering; antibody therapeutics