TGF‐β: a mobile purveyor of immune privilege

SM Wahl, J Wen, N Moutsopoulos - Immunological reviews, 2006 - Wiley Online Library
SM Wahl, J Wen, N Moutsopoulos
Immunological reviews, 2006Wiley Online Library
Functionally barricaded immune responses or sites of immune privilege are no longer
considered dependent on specific anatomical considerations, but rather, they can develop in
any location where immunoregulatory cells congregate and express or release products
capable of deviating the host response to foreign antigens. Among the pivotal molecules
involved in orchestrating these ectopic sites of immune suppression is transforming growth
factor‐β (TGF‐β), a secreted and cell‐associated polypeptide with a multiplicity of actions in …
Summary
Functionally barricaded immune responses or sites of immune privilege are no longer considered dependent on specific anatomical considerations, but rather, they can develop in any location where immunoregulatory cells congregate and express or release products capable of deviating the host response to foreign antigens. Among the pivotal molecules involved in orchestrating these ectopic sites of immune suppression is transforming growth factor‐β (TGF‐β), a secreted and cell‐associated polypeptide with a multiplicity of actions in innate and adaptive immunity. While beneficial in initiating and controlling immune responses and maintaining immune homeostasis, immunosuppressive pathways mediated by TGF‐β may obscure immune surveillance mechanisms, resulting in failure to recognize or respond adequately to self, foreign, or tumor‐associated antigens. CD4+CD25+Foxp3+ regulatory T cells represent a dominant purveyor of TGF‐β‐mediated suppression and are found in infiltrating tumors and other sites of immune privilege, where they influence CD8+ T cells; CD4+ T‐helper (Th)1, Th2, and Th17 cells; natural killer cells; and cells of myeloid lineage to choreograph and/or muck up host defense. Defining the cellular sources, mechanisms of action, and networking that distinguish the dynamic establishment of localized immune privilege is vital for developing strategic approaches to diminish or to embellish these tolerogenic events for therapeutic benefit.
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