CD38 and chronic lymphocytic leukemia: a decade later

F Malavasi, S Deaglio, R Damle… - Blood, The Journal …, 2011 - ashpublications.org
F Malavasi, S Deaglio, R Damle, G Cutrona, M Ferrarini, N Chiorazzi
Blood, The Journal of the American Society of Hematology, 2011ashpublications.org
This review highlights a decade of investigations into the role of CD38 in CLL. CD38 is
accepted as a dependable marker of unfavorable prognosis and as an indicator of activation
and proliferation of cells when tested. Leukemic clones with higher numbers of CD38+ cells
are more responsive to BCR signaling and are characterized by enhanced migration. In vitro
activation through CD38 drives CLL proliferation and chemotaxis via a signaling pathway
that includes ZAP-70 and ERK1/2. Finally, CD38 is under a polymorphic transcriptional …
Abstract
This review highlights a decade of investigations into the role of CD38 in CLL. CD38 is accepted as a dependable marker of unfavorable prognosis and as an indicator of activation and proliferation of cells when tested. Leukemic clones with higher numbers of CD38+ cells are more responsive to BCR signaling and are characterized by enhanced migration. In vitro activation through CD38 drives CLL proliferation and chemotaxis via a signaling pathway that includes ZAP-70 and ERK1/2. Finally, CD38 is under a polymorphic transcriptional control after external signals. Consequently, CD38 appears to be a global molecular bridge to the environment, promoting survival/proliferation over apoptosis. Together, this evidence contributes to the current view of CLL as a chronic disease in which the host's microenvironment promotes leukemic cell growth and also controls the sequential acquisition and accumulation of genetic alterations. This view relies on the existence of a set of surface molecules, including CD38, which support proliferation and survival of B cells on their way to and after neoplastic transformation. The second decade of studies on CD38 in CLL will tell if the molecule is an effective target for antibody-mediated therapy in this currently incurable leukemia.
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