Costimulation through the inducible costimulator ligand is essential for both T helper and B cell functions in T cell–dependent B cell responses

被引:0
作者
Tak W Mak
Arda Shahinian
Steve K Yoshinaga
Andrew Wakeham
Louis-Martin Boucher
Melania Pintilie
Gordon Duncan
Beata U Gajewska
Matthew Gronski
Urs Eriksson
Bernhard Odermatt
Alexandra Ho
Denis Bouchard
John S Whorisky
Manel Jordana
Pamela S Ohashi
Tony Pawson
Friedhelm Bladt
Anna Tafuri
机构
[1] Advanced Medical Discovery Institute,Ontario Cancer Institute, and Departments of Medical Biophysics and Immunology
[2] University of Toronto,Division of Respiratory Disease and Allergy
[3] Amgen,Department of Pathology
[4] Centre for Gene Therapeutics,undefined
[5] McMaster University,undefined
[6] University Hospital Zurich,undefined
[7] Mount Sinai Hospital,undefined
[8] Samuel Lunenfeld Research Institute,undefined
[9] Hôpital Necker,undefined
[10] INSERM U-580,undefined
来源
Nature Immunology | 2003年 / 4卷
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摘要
Costimulation through the inducible costimulator (ICOS) and its ligand (ICOSL) is essential for T cell–dependent B cell responses, but the cellular and temporal dynamics underlying its in vivo effects are poorly defined. Here we have shown that Icosl−/− and Icos−/− mice had similar phenotypes and that ICOS-ICOSL costimulation modulated the early but not late phases of IgG1 affinity maturation. Exploiting the adoptive transfer of T or B cells from primed Icosl−/− mice, we provided genetic evidence that costimulation through ICOSL was essential for primary but not secondary helper T cell responses and for the control of both T and B cell activities, resulting in T cell–dependent IgG1 production.
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页码:765 / 772
页数:7
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