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1 1st Leningrad Medical Institute, USSR Petrov
Research Institute of Oncology, Leningrad, USSR.
Introduction
Multiple myeloma (MM) is a malignant clonal B-lymphoproliferative
disease with typical immunodefficient, osteolytic, renal, amyloid
syndromes. Disturbance in the immunologic system appears early and
influences the outcome of MM [1 ]. Light chain isotype suppression
(LCIS) [2] and imbalance in T -cells [3] are the factors determining
the immunodefficiency syndrome. There are no convincing data about
changes in natural killer (NK) activity in MM [4, 5]. Osteolysis
is the second most frequently observed syndrome, and interleukin-1
ß (IL-1 ß), plays the main role in its development [6, 7]. IL-1
ß probably is also responsible for chronic renal insufficiency (CRI)
[7, 8], which is of great prognostic value im MM [9]. Amyloidosis
rarely appears in MM patients (6% 15% ) [10]. The aims of this study
were to clarify the role of LCIS, to determine NK activity of peripheral
blood mononuclear cells (PBMC) and bone marrow mononuclear cells
(BMMC) and IL-1 production by peripheral blood monocytes (PBM) in
MM, and to assess any possible correlation between these data and
the course of MM.
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