RT Journal Article
SR Electronic
T1 Cutting Edge: Multiple Autoimmune Pathways in <em>kd/kd</em> Mice
JF The Journal of Immunology
JO J. Immunol.
FD American Association of Immunologists
SP 2778
OP 2781
DO 10.4049/jimmunol.171.6.2778
VO 171
IS 6
A1 Hancock, Wayne W.
A1 Tsai, Tsai-Lung
A1 Madaio, Michael P.
A1 Gasser, David L.
YR 2003
UL http://www.jimmunol.org/content/171/6/2778.abstract
AB The kidney disease (kd) mutation was transferred to a C57BL/6 (B6) background by selection for closely linked microsatellite markers. The resulting congenic strain, B6.kd, was mated with partners homozygous for targeted mutations of CD4, CD8, CD28, IL-2, recombinase-activating gene-1 (Rag-1), ICAM-1, or β2-microglobulin. In most of the resulting double mutants, kidney disease occurred as readily and as severely as in the B6.kd controls, although disease occurred somewhat less frequently in age-matched CD28−/− kd/kd mice. Immunohistology demonstrated a predominance of macrophages in the lesions of B6.kd and most of the double mutants, with the remaining cells consisting of T cells and variable numbers of NK cells. In Rag-1−/− kd/kd, ∼50% of infiltrating cells were macrophages, and ∼50% were NK cells. These results suggest that the initial lesion caused by the mutant gene is intrinsic to the kidney and that the immune response that subsequently occurs can involve any one of several different cellular compositions.