Loss of CD4+ T cell IL-6R expression during inflammation underlines a role for IL-6 trans signaling in the local maintenance of Th17 cells

GW Jones, RM McLoughlin, VJ Hammond… - The journal of …, 2010 - journals.aai.org
GW Jones, RM McLoughlin, VJ Hammond, CR Parker, JD Williams, R Malhotra, J Scheller…
The journal of immunology, 2010journals.aai.org
IL-6 responses are classically orchestrated via a membrane-bound IL-6R (CD126) α subunit
(classical IL-6R signaling) or through a soluble form of this cognate receptor (IL-6 trans
signaling). Appraisal of IL-6R expression on human and mouse T cells emphasized that IL-
6R expression is closely linked with that of CCR7 and CD62L. In this regard, infiltrating
effector T cells from clinical and experimental peritonitis episodes lose IL-6R expression,
and anti-CD3/CD28 Ab costimulation of peripheral T cells in vitro leads to a downregulation …
Abstract
IL-6 responses are classically orchestrated via a membrane-bound IL-6R (CD126) α subunit (classical IL-6R signaling) or through a soluble form of this cognate receptor (IL-6 trans signaling). Appraisal of IL-6R expression on human and mouse T cells emphasized that IL-6R expression is closely linked with that of CCR7 and CD62L. In this regard, infiltrating effector T cells from clinical and experimental peritonitis episodes lose IL-6R expression, and anti-CD3/CD28 Ab costimulation of peripheral T cells in vitro leads to a downregulation in IL-6R expression. Consequently, IL-6 signaling through membrane-bound IL-6R seems to be limited to naive or central memory T cell populations. Loss of IL-6R expression by activated T cells further suggests that these effector cells might still retain IL-6 responsiveness via IL-6 trans signaling. Using IL-6R–deficient mice and recombinant tools that modulate the capacity of IL-6 to signal via its soluble receptor, we report that local control of IL-6 trans signaling regulates the effector characteristics of the T cell infiltrate and promotes the maintenance of IL-17A–secreting CD4+ T cells. Therefore, we concluded that classical IL-6R signaling in naive or central memory CD4+ T cells is required to steer their effector characteristics, whereas local regulation of soluble IL-6R activity might serve to maintain the cytokine profile of the Th cell infiltrate. Therefore, the activation status of a T cell population is linked with an alteration in IL-6 responsiveness.
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