For decades, chronic lymphocytic leukemia (CLL) has been regarded as homogeneous entity caused by the accumulation of monoclonal and immunoincompetent B cells with dysfunctional apoptotic pathways. Recently, many of these certainties have been questioned by evidence that demonstrate that CLL cells have been previously challenged by antigens, and therefore are immunocompetent cells. Moreover, in proliferative compartments, like the mantle zone of lymphoid organs or pseudo-follicles in the bone marrow, defects in proliferation seems to be as important as apoptosis impairment in the pathogenesis of the disorder. Two distinct subgroups of CLL can be segregated based on immunobiologic characteristics, clinical course and outcomes. The two subgroups can be identified by the presence of somatic mutations in the variable region of the heavy chain gene. The unmutated group presents a better outcome and is probably composed of anergized B cells previously exposed to an antigen which frequently affects a common segment of the variable region. The mutated group courses with a poorer prognosis and commonly presents an abnormal expression of ZAP70, a typical T-cell tyrosine kinase. The cell which originates CLL is a very early lymphocyte that still bears some T-cell characteristics, such as CD5 and ZAP70 expressions, but with the transcriptional machinery committed to the B-lineage. The original genetic lesion in this CLL primary cell is unknown. Cytogenetic abnormalities are frequently seen in the circulating lymphocytes and are probably late events in the pathogenesis of CLL.
Chronic lymphocytic leukemia; immunoglobulin gene; pathogenesis; review