共 35 条
Discovery of T Cell Antigens by High-Throughput Screening of Synthetic Minigene Libraries
被引:20
作者:

Hondowicz, Brian D.
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Schwedhelm, Katharine V.
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Kas, Arnold
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Tasch, Michael A.
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Rawlings, Crystal
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Ramchurren, Nirasha
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

McIntosh, Martin
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机构:
Fred Hutchinson Canc Res Ctr, Seattle, WA 98104 USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

D'Amico, Leonard A.
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Sanda, Srinath
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Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Standifer, Nathan E.
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机构:
Amgen Inc, Clin Immunol, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Shendure, Jay
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机构:
Univ Washington, Dept Genome Sci, Seattle, WA 98195 USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA

Stone, Brad
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机构:
Benaroya Res Inst, Translat Res Program, Seattle, WA USA Benaroya Res Inst, Translat Res Program, Seattle, WA USA
机构:
[1] Benaroya Res Inst, Translat Res Program, Seattle, WA USA
[2] Amgen Inc, Clin Immunol, Seattle, WA USA
[3] Univ Washington, Dept Genome Sci, Seattle, WA 98195 USA
[4] Fred Hutchinson Canc Res Ctr, Seattle, WA 98104 USA
来源:
基金:
美国国家卫生研究院;
关键词:
CLASS-I MOLECULES;
ADHESION MOLECULE;
PEPTIDE;
IDENTIFICATION;
RESPONSES;
EPITOPES;
EPCAM;
D O I:
10.1371/journal.pone.0029949
中图分类号:
O [数理科学和化学];
P [天文学、地球科学];
Q [生物科学];
N [自然科学总论];
学科分类号:
07 ;
0710 ;
09 ;
摘要:
The identification of novel T cell antigens is central to basic and translational research in autoimmunity, tumor immunology, transplant immunology, and vaccine design for infectious disease. However, current methods for T cell antigen discovery are low throughput, and fail to explore a wide range of potential antigen-receptor interactions. To overcome these limitations, we developed a method in which programmable microarrays are used to cost-effectively synthesize complex libraries of thousands of minigenes that collectively encode the content of hundreds of candidate protein targets. Minigene-derived mRNA are transfected into autologous antigen presenting cells and used to challenge complex populations of purified peripheral blood CD8+ T cells in multiplex, parallel ELISPOT assays. In this proof-of-concept study, we apply synthetic minigene screening to identify two novel pancreatic islet autoantigens targeted in a patient with Type I Diabetes. To our knowledge, this is the first successful screen of a highly complex, synthetic minigene library for identification of a T cell antigen. In principle, responses against the full protein complement of any tissue or pathogen can be assayed by this approach, suggesting that further optimization of synthetic libraries holds promise for high throughput antigen discovery.
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