2005
DOI: 10.3109/2000-1967-075
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The Immunoglobulin genes and Chronic Lymphocytic Leukemia (CLL)

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Cited by 11 publications
(14 citation statements)
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“…If the development of the malignant CLL clone occurred independently of antigenic interaction, one would expect the gene usage and CDR3 sequences (the most individual antigen-binding part of the immunoglobulin) of CLL BCRs to be randomly distributed as in normal B-cells. However, the CLL immunoglobulin gene usage is biased [22], [23], [24], [25] and a number of highly similar CDR3 regions are expressed. Indeed, more than 26% of CLL cells express BCRs belonging to one of almost 150 stereotyped subsets with virtually identical CDR3 sequences characterized so far [19], [20], [24], [26], [27], [28].…”
Section: Introductionmentioning
confidence: 99%
“…If the development of the malignant CLL clone occurred independently of antigenic interaction, one would expect the gene usage and CDR3 sequences (the most individual antigen-binding part of the immunoglobulin) of CLL BCRs to be randomly distributed as in normal B-cells. However, the CLL immunoglobulin gene usage is biased [22], [23], [24], [25] and a number of highly similar CDR3 regions are expressed. Indeed, more than 26% of CLL cells express BCRs belonging to one of almost 150 stereotyped subsets with virtually identical CDR3 sequences characterized so far [19], [20], [24], [26], [27], [28].…”
Section: Introductionmentioning
confidence: 99%
“…Tobin et al 12 initially reported that patients with CLL cells that express IGHV3-21 have relatively aggressive disease, even when the expressed IGHV3-21 had evidence for somatic mutation. 13,14 However, such mutated (M) IGHV3-21 frequently had higher percent homology to the germline IGHV3-21 (eg, Ͼ 97%) than did the M-IGHV of other CLL cases that do not use IGHV3-21, which on average have less than 94% homology to any known germline IGHV gene. 3,4,15 This led to speculation that there might be genetic polymorphism in IGHV3-21 and that use of different IGHV3-21 alleles only gave the appearance that such Ig had undergone somatic mutation.…”
mentioning
confidence: 99%
“…16 However, Tobin et al 14 analyzed the germline IGHV3-21 genes of patients with CLL cells that used M-IGHV3-21 and found that genetic polymorphism could not account for the base substitutions observed in the expressed IGHV3-21 genes, indicating that they indeed had incurred somatic mutations. 13,14 However, it still was is not resolved whether CLL cells expressing such M-IGHV3-21 were derived from B cells that had experienced maturation in the germinal center, where B cells can undergo Ig somatic hypermutation during the immune response to antigen.Furthermore, the prevalence of CLL cases that use IGHV3-21 in the United States is uncertain. Although initially reported that 31 of 265 patients in a Scandinavian study had CLL cells that used IGHV3-21 (12%), more recent studies of patients mostly from southern and central Europe found that less than 3% of all patients used this IGHV.…”
mentioning
confidence: 99%
“…Furthermore, progressive disease can be predicted using a combination of cellular markers including Zap-70 [3 -6] and CD38 expression [2,7,8] or by gene expression profiling of lipoprotein lipase (LPL) and CLLU-1 [9,10]. In addition, it is becoming increasingly clear that IgHV gene usage, associated with or independent of mutational status, may be of prognostic significance [11].…”
Section: Introductionmentioning
confidence: 99%