VASCULAR CELL-ADHESION MOLECULE-1 AND ALPHA-4-INTEGRIN AND BETA-1-INTEGRIN IN LYMPHOCYTE AGGREGATES IN SJOGRENS-SYNDROME AND RHEUMATOID-ARTHRITIS

Objectives-Interactions between vascular cell adhesion molecule 1 (VCA M-1) and its ligand, the alpha4/beta1 integrin, have been shown to be important in a number of cellular events in vitro. To assess the impor tance of such interactions in the development of lymphocytic infiltrat ion in diseased tissue the distribution of the two ligands has been st udied immunohistochemically. Methods-Cryostat sections of labial tissu e from patients with Sjogren's syndrome, normal labial tissues, rheuma toid synovia, and normal tonsils were stained using antibodies to VCAM -1, alpha4 and beta1 integrin chains, and markers for T cells, B cells , macrophages, and follicular dendritic reticulum cells (FDRCs), visua lised using alkaline phosphatase and fast red. Results-Staining patter ns for VCAM-1 and integrin chains in lymphocyte aggregates in synovial and labial tissues were similar. VCAM-1 staining was found on both va scular and ramifying dendritic cells at the centre of large T cel aggr egates and in all aggregates where there was a central clustering of B cells. VCAM-1 colocalised with, but also extended beyond, staining fo r the FDRC marker R4/23. Staining for the alpha4 and beta1 integrin ch ains was more widespread than staining for VCAM-1, with no significant increase in staining at sites of maximum VCAM-1 staining. In tonsils VCAM-1 and R4/23 codistributed in germinal centres, but staining for t he alpha4 and beta1 integrin chains was chiefly seen in T lymphocyte a reas. Conclusions-VCAM-1 may be more important in determining the dist ribution of B than T lymphocytes in lymphocytic infiltration of non-ly mphoid tissue. Unlike the follicles of lymphoid tissue, ectopic follic le-like structures in non-lymphoid tissues may form by immigration of B cells via VCAM-1+ vessels at the centre of T cell aggregates.