1997
DOI: 10.1046/j.1365-2141.1997.72653.x
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Circulating plasma cells in multiple myeloma: characterization and correlation with disease stage

Abstract: Summary. The aim of this study was to develop a flow cytometric test to quantitate low levels of circulating myeloma plasma cells, and to determine the relationship of these cells with disease stage. Cells were characterized using five-parameter flow cytometric analysis with a panel of antibodies, and results were evaluated by comparison with fluorescent consensus-primer IgH-PCR.Bone marrow myeloma plasma cells, defined by high CD38 and Syndecan-1 expression, did not express CD10, 23, 30, 34 or 45RO, and demon… Show more

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Cited by 160 publications
(134 citation statements)
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“…Clearly, their CD56 − MM patients (45% of their patients) did not overlap our CD56 − population of patients. On the other hand, our data are in complete agreement with those of Rawstron et al, 12 showing a weaker expression of CD56 on circulating myeloma cells in MM lacking overt PCL. A last point deserves some comment.…”
Section: Discussionsupporting
confidence: 93%
See 1 more Smart Citation
“…Clearly, their CD56 − MM patients (45% of their patients) did not overlap our CD56 − population of patients. On the other hand, our data are in complete agreement with those of Rawstron et al, 12 showing a weaker expression of CD56 on circulating myeloma cells in MM lacking overt PCL. A last point deserves some comment.…”
Section: Discussionsupporting
confidence: 93%
“…The interest in using CD138 to define plasma cells has been validated by ourselves 8 and recently confirmed by others. 12 CD138 plasma cell identification was controlled by coexpression of CD38 and intracytoplasmic / immunofluorescence, in a three-color assay. 13 The mean fluorescence ratio (MFR) was calculated as follows: mean of specific fluorescence/mean of control fluorescence.…”
Section: Phenotypic Analysismentioning
confidence: 99%
“…Circulating aberrant PC have been detected at diagnosis in a relatively high percentage of MM cases (46-75%) (122,123) and in patients with MGUS and smoldering MM (25 and 50%, respectively) (124). However, contradictory results exist concerning the relationship between frequency of PB clonal PC and tumor burden, disease stage or cytogenetic abnormalities (39,(122)(123)(124); in addition, the clinic-biological significance of PC trafficking still remains to be clarified. Circulating aberrant PC have been found in PB-derived leukaphaeresis products after mobilization (16-41%) (72,125) and prior to ASCT (39%) (125).…”
Section: Identification and Enumeration Of Circulatingmentioning
confidence: 99%
“…5,6 Despite the different tumor mass [7][8][9][10][11][12][13][14] and clinical behavior of the disease, clonal PC from MGUS, SMM and MM patients show highly similar and largely overlapping genetic profiles. [15][16][17] In addition, no clear phenotypic differences have been reported so far among clonal PC from MGUS, SMM and MM, 18 except for a few molecules involved in the interaction between PC and their microenvironment.…”
Section: Introductionmentioning
confidence: 99%