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Intestinal Disease Research Program and Departments of Pathology and Molecular Medicine, McMaster University, Hamilton, Ontario, Canada
Little is understood about the earliest cytokine responses and the
role(s) of donor CD4 T cells in the intestine during the induced
graft-vs-host reaction (GVHR). We investigated the activation and
mucosal homing phenotype of the donor CD4 cells and the kinetics of
cytokine responses within the intestine and associated lymphoid tissues
during early GVHR. Significant frequencies of donor CD4 cells
accumulated within recipient Peyers patches (PP), mesenteric lymph
nodes (MLN), lamina propria (LP), and spleen (SP), during the first 9
days of GVHR. Many donor CD4 cells in SP, MLN, and LP expressed CD44
and also expressed de novo the mucosal homing integrin
4
7 (LPAM-1). A large IFN-
response
occurred by day 3 in cells from PP and MLN, but much later (day 9) in
SP and LP cells. IL-10 production by SP and MLN cells was elevated
initially but declined substantially by day 9. IL-4 production by SP,
MLN, and PP cells was low on day 3 and showed gradual decline in LP by
day 9. IL-5 production by LP cells gradually increased in direct
contrast to IL-5 production by MLN cells. The MLN CD4 cells showed the
most dynamic changes, with high numbers of activated/effector donor CD4
cells and altered cytokine production consistent with a developing Th1
response. The IFN-
responses in PP and MLN preceded that of the SP,
suggesting an intestinal origin for some Th1 effector cells in GVHR.
Donor CD4 T cells apparently acquire the ability to home to the LP
during early GVHR.
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