Clin Lymphoma. 2005 Mar;5(4):278-81.
CD52 expression in Waldenstrom's macroglobulinemia: implications for alemtuzumab
therapy and response assessment.
Owen
RG, Hillmen
P, Rawstron
AC.
Haematological Malignancy Diagnostic Service Laboratory, The Leeds Teaching Hospitals NHS
Trust, General Infirmary at Leeds, Great George Street, Leeds LS1 3EX, UK.
rgowen@hmds.org.uk
The efficacy of monoclonal antibody therapy is determined, at least in part, by the extent
to which the target antigen is expressed. This is a complex issue in Waldenstrom's
macroglobulinemia (WM) as it is a disorder characterized by plasma cell differentiation
and therefore target antigen expression may differ between the B-cell and plasma cell
compartments of the disease. In order to assess this in the context of alemtuzumab
therapy, the authors used multiparameter flow cytometry to determine CD52 expression in
the B-cells and plasma cells of patients with WM. CD52 expression was demonstrable in the
B-cells of all cases, with a median of 99% of cells (range, 81%-100%) expressing the
antigen compared with the isotype control (n = 47). Antigen density was very similar to
that seen in chronic lymphocytic leukemia (median mean fluorescence intensity [MFI], 1249;
range, 175-3170). Antigen expression was, however, significantly lower in the plasma cells
(median MFI, 235; range, 31-1814) in all but 1 of the cases assessed (n = 21). The
clinical significance of this was assessed by examining serial bone marrow samples from
patients receiving alemtuzumab as part of an ongoing clinical trial. In 4 of 5 patients,
alemtuzumab therapy successfully eradicated clonal B-cells from the bone marrow, but
residual plasma cells remained evident in 2 of these patients. The implications of these
findings for monoclonal antibody therapy in WM are discussed.
PMID: 15794865 [PubMed - indexed for MEDLINE]