Integrins of the 7 subfamily, ␣47 and ␣E7, contribute to lymphocyte homing and to the development of protective or autoreactive immune responses at mucosal sites. The  subunits of integrins are considered important for regulation of stimulated cell adhesion and adhesion-dependent signal transduction. Using a yeast interaction trap screen, a human WD repeat protein, termed WAIT-1, was isolated that interacts with the integrin 7 cytoplasmic tail and is homologous to mouse EED and Drosophila ESC proteins. WAIT-1 also binds to the cytoplasmic domains of ␣4 and ␣E but not to those of integrin 1, 2, and ␣L subunits. Association of WAIT-1 and 7-integrin was confirmed by coprecipitation from transiently transfected 293 cells. The binding site for WAIT-1 was mapped to a short membrane-proximal region of the 7 cytoplasmic tail with Tyr-735 being of critical importance. Northern blot analysis revealed multiple WAIT-1-related transcripts with differential expression in circulating leukocytes, tissue-resident cells of diverse origin, and lymphoid malignancies. These results suggest that WAIT-1, together with the recently identified RACK1, may define a novel subfamily of WD repeat proteins that interact with distinct subsets of integrin cytoplasmic tails and may act as specific regulators of integrin function.Expression of 7-integrins, ␣47 and ␣E7, is largely confined to leukocytes. Although ␣47-integrin is homogeneously expressed on natural killer cells, eosinophils, and naive T and B cells, its distribution on effector/memory T and B cells is restricted to a subset of gut-homing lymphocytes (1-6). Peripheral blood monocytes do not express 7-integrins, but ␣47 and ␣E7 are up-regulated upon stimulation of macrophage differentiation with phorbol ester or interferon-␥ (7). Recent studies have indicated that, in addition, ␣47-integrin is induced on endothelial cells after treatment with proinflammatory mediators such as tumor necrosis factor (8). In contrast to ␣47, expression of the ␣E7-integrin is confined to a subset of gutassociated T lymphocytes and dendritic cells (4,6,9).7-Integrins are considered important for the development and function of gut-associated lymphoid tissues. Interaction of ␣47 with MAdCAM-1 allows for tissue-specific migration of circulating lymphocytes into the lamina propria and Peyer's patches of the gut (10, 11), whereas ␣E7 may retain intraepithelial lymphocytes within the gut epithelium through binding of E-cadherin on epithelial cells (12,13). Lack of 7-integrins severely impairs the development of the gut immune system, as Peyer's patches are absent or hypoplastic, and fewer intraepithelial lymphocytes are detected in 7-integrin-deficient mice (14). Moreover, gut-homing ␣47 ϩ CD4 T cells specifically harbor cellular memory for intestinal antigens, suggesting that ␣47 helps to target and segregate intestinal versus systemic immune responses (15).Integrins of the 7 family are involved in the development and/or progression of diseases such as colitis (16,17), diabetic insul...
