Bone marrow stroma inhibits proliferation and apoptosis in leukemic cells through gap junction-mediated cell communication
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Abstract
Normal and leukemic blood cell progenitors depend upon the
bone marrow (BM) stroma with which they communicate
through soluble and membrane-anchored mediators, adhe sive interactions and gap junctions (GJ). Regarding hemato poiesis, it is believed that it can be influenced by connexin
expression, but the exact role of GJ in cell death and
proliferation is not clear. Using flow cytometry, we monitored
the division rate of leukemic cell lines, communicating and
not communicating with stromal cell line through GJ. We
found that GJ-coupled cells (i) did not proliferate; (ii) were
kept in G0; and (iii) were protected from drug-induced
apoptosis when compared to either total or uncoupled cell
population. We conclude that GJ coupling between stroma
and leukemic lymphoblasts prevents proliferation, keeping
cells in a quiescent state, thus increasing their resistance to
antimitotic drugs. Since GJ are particularly abundant in the
sub-endosteal environment, which harbors blood stem cells,
we also asked which cells within the normal human BM
communicate with the stroma. Using a primary BM stroma cell
culture, our results show that 80% of CD34 þ progenitors
communicate through GJ. We propose that blood cell
progenitors might be retained in the low-cycling state by
GJ-mediated communication with the hematopoietic stroma.