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Evidence for Contribution of CD4+CD25+ Regulatory T Cells in Maintaining Immune Tolerance to Human Factor IX following Perinatal Adenovirus Vector Delivery
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نویسنده
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nivsarkar m.s. ,buckley s.m.k. ,parker a.l. ,perocheau d. ,mckay t.r. ,rahim a.a. ,howe s.j. ,waddington s.n.
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منبع
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journal of immunology research - 2015 - دوره : 2015 - شماره : 0
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چکیده
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Following fetal or neonatal gene transfer in mice and other species immune tolerance of the transgenic protein is frequently observed; however the underlying mechanisms remain largely undefined. in this study fetal and neonatal balb/c mice received adenovirus vector to deliver human factor ix (hfix) cdna. the long-term tolerance of hfix was robust in the face of immune challenge with hfix protein and adjuvant but was eliminated by simultaneous administration of anti-cd25+ antibody. naive irradiated balb/c mice which had received lymphocytes from donors immunised with hfix developed anti-hfix antibodies upon immune challenge. cotransplantation with cd4+cd25+ cells isolated from neonatally tolerized donors decreased the antibody response. in contrast,cotransplantation with cd4+cd25-cells isolated from the same donors increased the antibody response. these data provide evidence that immune tolerance following perinatal gene transfer is maintained by a cd4+cd25+ regulatory population. © 2015 megha s. nivsarkar et al.
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آدرس
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gene transfer technology group,university college london,86-96 chenies mews, United Kingdom, gene transfer technology group,university college london,86-96 chenies mews, United Kingdom, institute of cancer and genetics,cardiff university school of medicine,heath park, United Kingdom, gene transfer technology group,university college london,86-96 chenies mews, United Kingdom, stem cell group,cardiovascular and cell sciences research institute,st. george's university of london,cranmer terrace, United Kingdom, department of pharmacology,school of pharmacy,university college london,29-39 brunswick square, United Kingdom, molecular and cellular immunology,ucl institute of child health,30 guilford street, United Kingdom, gene transfer technology group,university college london,86-96 chenies mews,london,united kingdom,antiviral gene therapy research unit,faculty of health sciences,university of the witwatersrand, South Africa
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Authors
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