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Eliminating antibody polyreactivity through addition of N-linked glycosylation
Authors:Gwo-Yu Chuang  Baoshan Zhang  Krisha McKee  Sijy O'Dell  Young Do Kwon  Tongqing Zhou  Julie Blinn  Krissey Lloyd  Robert Parks  Tarra Von Holle  Sung-Youl Ko  Wing-Pui Kong  Amarendra Pegu  Keyun Wang  Kavitha Baruah  Max Crispin  John R Mascola  M Anthony Moody  Barton F Haynes  Ivelin S Georgiev  Peter D Kwong
Affiliation:1Vaccine Research Center, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland, 20892;2Duke Human Vaccine Institute, Duke University Medical Center, Durham, North Carolina, 103020;3Oxford Glycobiology Institute, Department of Biochemistry, University of Oxford, Oxford, OX1, 3QU, United Kingdom
Abstract:Antibody polyreactivity can be an obstacle to translating a candidate antibody into a clinical product. Standard tests such as antibody binding to cardiolipin, HEp-2 cells, or nuclear antigens provide measures of polyreactivity, but its causes and the means to resolve are often unclear. Here we present a method for eliminating antibody polyreactivity through the computational design and genetic addition of N-linked glycosylation near known sites of polyreactivity. We used the HIV-1-neutralizing antibody, VRC07, as a test case, since efforts to increase VRC07 potency at three spatially distinct sites resulted in enhanced polyreactivity. The addition of N-linked glycans proximal to the polyreactivity-enhancing mutations at each of the spatially distinct sites resulted in reduced antibody polyreactivity as measured by (i) anti-cardiolipin ELISA, (ii) Luminex AtheNA Multi-Lyte ANA binding, and (iii) HEp-2 cell staining. The reduced polyreactivity trended with increased antibody concentration over time in mice, but not with improved overall protein stability as measured by differential scanning calorimetry. Moreover, glycan proximity to the site of polyreactivity appeared to be a critical factor. The results provide evidence that antibody polyreactivity can result from local, rather than global, features of an antibody and that addition of N-linked glycosylation can be an effective approach to reducing antibody polyreactivity.
Keywords:polyreactivity   antibody engineering   bioinformatics   broadly neutralizing antibody   glycan engineering
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