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Journal of Clinical Immunology

Published in:

01-01-2009

Engineered Alt a 13 Fragment of Alternaria alternata Abrogated IgE Binding without Affecting T-cell Stimulation

Authors: Jay Shankar, Bhanu P. Singh, Shailendra N. Gaur, Naveen Arora

Published in: Journal of Clinical Immunology | Issue 1/2009

Abstract

Rationale

Epitopes were delineated for allergenic proteins, but studies are required to identify residues mediating IgE binding. In the present study, the in silico approach was used to identify IgE-binding residues of Alt a 13^1–50 fragment and confirmed by experimental approach.

Method and Results

IgE-binding epitopes of Alt a 13 mapped computationally were cloned, expressed, purified, and characterized using various immunochemical and biophysical methods. Among four fragments of Alt a 13, Alt a 13^1–50 demonstrated maximum IgE binding with two immunodominant regions and was mutated at these regions. The mutation in first region, Alt a 13^1–50-K4A_S6F, did not show any change in immunological and biophysical properties of protein. However, mutations in the second region, Alt a 13^1–50-T21F_N27I, caused reduced IgE binding, histamine release, and low IL-4 release on stimulation of Alternaria alternata positive patients peripheral blood mononuclear cells in vitro.

Conclusion

This suggests that residues T21 and N27 are important for the secondary structure. In conclusion, Alt a 13^1–50-T21F_N27I with reduced Th 2 response and intact T-cell proliferation capacity has potential for clinical use.

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Title: Engineered Alt a 13 Fragment of Alternaria alternata Abrogated IgE Binding without Affecting T-cell Stimulation
Authors: Jay Shankar
Bhanu P. Singh
Shailendra N. Gaur
Naveen Arora
Publication date: 01-01-2009
Publisher: Springer US
Published in: Journal of Clinical Immunology / Issue 1/2009
Print ISSN: 0271-9142
Electronic ISSN: 1573-2592
DOI: https://doi.org/10.1007/s10875-008-9224-1

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Abstract

Rationale

Method and Results

Conclusion

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