Circulating human B cells that express surrogate light chains and edited receptors

被引:0
|
作者
Eric Meffre
Eric Davis
Claudine Schiff
Charlotte Cunningham-Rundles
Lionel B. Ivashkiv
Louis M. Staudt
James W. Young
Michel C. Nussenzweig
机构
[1] Laboratory of Molecular Immunology,Division of Clinical Sciences
[2] The Rockefeller University,Department of Medicine and Pediatrics
[3] Howard Hughes Medical Institute,Department of Medicine
[4] National Cancer Institute Building 10,Department of Medicine
[5] Room 5A02,undefined
[6] National Institutes of Health,undefined
[7] Centre d'Immunologie de Marseille-Luminy,undefined
[8] case 906 ,undefined
[9] Mount Sinai Medical Center,undefined
[10] Hospital for Special Surgery,undefined
[11] Allogenic Bone Marrow Transplant and Clinical Immunology Services,undefined
[12] Memorial Sloan-Kettering Cancer Center Weil Medical College of Cornell University,undefined
来源
Nature Immunology | 2000年 / 1卷
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摘要
Immunoglobulin gene recombination can result in the assembly of self-reactive antibodies. Deletion, anergy or receptor editing normally silence B cells that produce these autoantibodies. Receptor editing is highly efficient in mouse B cells that carry pre-recombined autoantibody transgenes or gene “knock-ins”. However, it has been difficult to identify cells that have edited receptors in unmanipulated mice and humans. To try to identify such cells we isolated and characterized B cells that coexpress surrogate and conventional light chains (V-preB+L+) from the blood of normal human donors. V-preB+L+ B cells express RAG mRNA, display an unusual heavy and light chain antibody repertoire consistent with antiself reactivity, and show evidence of receptor editing. These cells accumulate in the joints of patients with rheumatoid arthritis, consistent with a role for V-preB+L+ B cells and receptor editing in autoimmune disease.
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页码:207 / 213
页数:6
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