Expression of CD34 and CD7 on human T-cell acute lymphoblastic leukemia discriminates functionally heterogeneous cell populations

B Gerby, E Clappier, F Armstrong, C Deswarte, J Calvo… - Leukemia, 2011 - nature.com
B Gerby, E Clappier, F Armstrong, C Deswarte, J Calvo, S Poglio, J Soulier, N Boissel
Leukemia, 2011nature.com
Leukemia-initiating/repopulating cells (LICs), also named leukemic stem cells, are
responsible for propagating human acute leukemia. Although they have been characterized
in various leukemias, their role in T-cell acute lymphoblastic leukemia (T-ALL) is unclear. To
identify and characterize LICs in T-ALL (T-LIC), we fractionated peripheral blood cell
populations from patient samples by flow cytometry into three cell fractions by using two
markers: CD34 (a marker of immature cells and LICs) and CD7 (a marker of early T-cell …
Abstract
Leukemia-initiating/repopulating cells (LICs), also named leukemic stem cells, are responsible for propagating human acute leukemia. Although they have been characterized in various leukemias, their role in T-cell acute lymphoblastic leukemia (T-ALL) is unclear. To identify and characterize LICs in T-ALL (T-LIC), we fractionated peripheral blood cell populations from patient samples by flow cytometry into three cell fractions by using two markers: CD34 (a marker of immature cells and LICs) and CD7 (a marker of early T-cell differentiation). We tested these populations in both in vitro culture assays and in vivo for growth and leukemia development in immune-deficient mice. We found LIC activity in CD7+ cells only as CD34+ CD7− cells contained normal human progenitors and hematopoietic stem cells that differentiated into T, B lymphoid and myeloid cells. In contrast, CD34+ CD7+ cells were enriched in LICs, when compared with CD34− CD7+ cells. These CD34+ CD7+ cells also proliferated more upon NOTCH activation than CD34− CD7+ cells and were sensitive to dexamethasone and NOTCH inhibitors. These data show that CD34 and CD7 expression in human T-ALL samples help in discriminating heterogeneous cell populations endowed with different LIC activity, proliferation capacity and responses to drugs.
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