Journal
IMMUNOBIOLOGY
Volume 217, Issue 2, Pages 216-224Publisher
ELSEVIER GMBH, URBAN & FISCHER VERLAG
DOI: 10.1016/j.imbio.2011.06.004
Keywords
Complement; T cell; Autoimmunity; Transplantation; C5a; C3a; CD46
Categories
Funding
- NIH [R01AI043578, R01AI071185]
- MRC [G1002165]
- Medical Research Council Centre for Transplantation, Guy's Hospital, King's College
- Department of Health, National Institute for Health Research comprehensive Biomedical Research Centre
- MRC [G1002165] Funding Source: UKRI
- Medical Research Council [G1002165] Funding Source: researchfish
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Our understanding of the complement system has markedly evolved from its early beginnings as a protein system merely detecting and tagging a pathogen for further clearance. For example, the repertoire of danger that complement recognizes covers currently a wide range of distinct self and non-self danger signals. Further, complement is now firmly established as instructor of adaptive B and T cell immunity. This review focuses on two the recent emerging paradigms in the field. Firstly, that complement is not only vitally required for the induction of Th1 immunity but also for the timely contraction of this protective response and therefore for prevention of autoimmunity and immune homeostasis. Secondly, that local rather than systemic complement is impacting on immunemodulation during a T cell response. (C) 2011 Elsevier GmbH. All rights reserved.
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