Abstract

T-cell depletion (TCD) of BM allows transplantation across HLA barriers. Although different methods are used throughout the world, the optimal application of TCD still remains unclear, partly due to the lack of thorough analyses of the cellular fractions eliminated or retained in each method, and their possible implications regarding GvHD, GvL, or engraftment. We have analyzed the phenotype of the successive fractions of 19 BM samples depleted by soybean lectin agglutination and sheep erythrocyte rosetting (elimination of T cells that form rosettes through CD2), focusing on the final fraction infused to patients. Analysis was performed using three-color flow cytometry and strategies for optimal staining and individualism of the subsets of interest. The relative composition of the lymphoid population varied significantly along the successive steps in TCD: at the agglutination step, B cells and CD4 T cells are greatly reduced, while natural killer cells (NK) and TCRgammadelta+ T are augmented. The rosetting steps imply the relative enrichment of CD2-dim T cells, together with a further rise in the proportion of NK and double-negative T cells frequently TCRgammadelta+. The presence of minor subsets of CD2- TCRgammadelta+ and CD2- TCRalphabeta T cells has already been described in the peripheral blood of normal individuals. We report that, by using this method of TCD, CD2-dim T cells, frequently TCRgammadelta+, are retained in the grafts and infused in patients, together with NK cells as the main lymphoid population. We discuss the possible implications of these populations in the biology of the graft, regarding GvHD, GvL and engraftment.

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