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Blood.
2006 Aug 15;108(4):1135-44. Epub 2006 Apr 18.
In-tandem insight from basic
science combined with clinical research: CD38 as
both marker and key component of the pathogenetic
network underlying chronic lymphocytic leukemia.
Deaglio S,
Vaisitti T, Aydin S, Ferrero E, Malavasi F.
Laboratory of Immunogenetics, Department of
Genetics, Biology and Biochemistry, University of
Torino, Italy.
The absence of mutations in the
IgV genes, together with the presence of ZAP-70 and
CD38, are the most reliable negative prognostic
markers for chronic lymphocytic leukemia (CLL)
patients. Several lines of evidence indicate that
CD38 may be not only a diagnostic marker but also a
key element in the pathogenetic network in CLL.
First, CD38 is a receptor that induces proliferation
and increases survival of CLL cells. Second, CD38
signals start upon interaction with the CD31 ligand
expressed by stromal and nurse-like cells. Third,
CD38/CD31 contacts up-regulate CD100, a semaphorin
involved in sustaining CLL growth. Fourth, evidence
that nurselike cells express high levels of CD31 and
plexin-B1, the high-affinity ligand for CD100,
offers indirect confirmation for this model of
receptor cross-talk. Elements of variation in the
clinical course of CD38(+) CLL patients include (1)
potential intersection with ZAP-70, a kinase
involved in the CD38 signaling pathway in T and
natural killer (NK) cells, and (2) the effects of
genetic polymorphisms of the receptors involved, at
least of CD38 and CD31. Consequently, CD38 together
with ZAP-70 appear to be the key elements of a
coreceptor pathway that may sustain the signals
mediated by the B-cell receptor and potentially by
chemokines and their receptors. This would result in
acquisition of increased survival potential,
providing clues to the poorer prognosis of CD38(+)
patients.
PMID: 16621959 [PubMed - indexed for
MEDLINE]