ABSTRACT: Obtaining a complete picture of 3D-genome organization in tissues and disease states is often blocked by limiting amounts of tissue samples such that multiple types of genome-wide analyses cannot be performed on the same sample. Here, we found that starting with a pure population of memory CD4+ T-cells (mCD4-cells) we could get reproducible Hi-C data with just 50,000 cells. This population is only ~18.75% of the whole T-cell population, but presumably its uniformity enabled high reproducibility with low cell numbers so that Hi-C, RNA-Seq and potentially other analyses could be performed with repeats from the same donor. Moreover, there was strong correspondence between data from 3 different donors, suggesting that variability between individuals observed in other reports may reflect more the dynamic variability in the status of the immune system between individuals rather than variability in genome organization between individuals for a given cell type. We further observed uniform changes between samples and blood donors occurring during activation of the memory mCD4+ T cell population. While some genome organization changes occurred concomitant with changes in gene expression, there were at least as many changes that occurred without corresponding changes in expression. Counter to the hypothesis that TADs are largely invariant structures providing a scaffold for dynamic looping contacts between enhancers and promotors, we found that there were at least as many dynamic TAD changes as loops in this highly differentiated cell type. Stimulation with IL-2 alone triggered many changes in genome organization and many of these changes were strengthened by additional TCR and CD28 co-receptor stimulation. This suggests a stepwise process whereby mCD4+ T cells undergo sequential genome organization changes induced by distinct or combined stimuli likely to "prime" or “de-prime” them for expression responses to subsequent TCR-antigen ligation or additional cytokine stimulation