Stereotyped patterns of somatic hypermutation in subsets of patients with chronic lymphocytic leukemia: implications for the role of antigen selection in leukemogenesis

Murray, Fiona; Darzentas, Nikos; Hadzidimitriou, Anastasia; Tobin, Gerard; Boudjogra, Myriarn; Scielzo, Cristina; Laoutaris, Nikolaos; Karlsson, Karin; Baran-Marzsak, Fanny; Tsaftaris, Athanasios; Moreno, Carol; Anagnostopoulos, Achilles; Caligaris-Cappio, Federico; Vaur, Dominique; Ouzounis, Christos A.; Belessi, Chrysoula; Ghia, Paolo; Davi, F; Rosenquist, Richard; Stamatopoulos, Kostas

doi:10.1182/blood-2007-07-099564

Cited by 295 publications

(528 citation statements)

References 86 publications

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“…37,38 However, no such bias is evident in other B-cell lymphomas, for example, CLL or MCL, where among the rearrangements using the IGHV1-2 gene, alleles *02 and *04 are detected at roughly similar frequencies. 8,24 This restricted usage of allele *04 in SMZL is noteworthy, given that it differs from allele *02 by a single amino acid, and can be considered as a molecular argument for selection.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, interpretation of results for all cases was performed de novo in the context of this study, following the approaches reported in our recent publications. 8,24,28 Molecular modeling In order to explore the possible modifications in the antibody structure caused by a single amino-acid replacement---namely, the arginine (R)-totryptophan (W) substitution at position VH FR3-75 to obtain an IGHV1-2*04-rearranging antibody---we performed a molecular dynamics study of the human anti-polyhydroxybutyrate antibody F v : IGHV1-2*02 IGKV1-39*01/1D-39*01 (Protein Data Bank code 2D7T). Replacement of the VH FR3-75 R (germline for IGHV1-2*02) by the W residue (germline for IGHV1-2*04) was executed by the COOT algorithm.…”

Section: Pcr Amplification Of Ighv --Ighd --Ighj Rearrangementsmentioning

confidence: 99%

“…Additionally, many lymphoma subtypes are characterized by somatic hypermutation (SHM) in IGHV genes, suggestive of antigen-driven affinity maturation. 7,8 Previous studies by us and others have shown that SMZL shows a biased IG gene repertoire and is characterized by heterogeneity with regard to the mutational status of the IG receptors. 4,9 --23 Individual studies have highlighted different IG sequence features, including repertoire differences between SMZL, SDRL and hairy cell leukemia-variant; 4,15 intraclonal diversification of IG genes through ongoing SHM; 12,17,18,23 potential analogies between SMZL and hairy cell leukemia-variant; 15 and, very recently, the existence of cases sharing quasi-identical antigen-binding sites (stereotyped B-cell receptors).…”

Section: Introductionmentioning

confidence: 99%

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Over 30% of patients with splenic marginal zone lymphoma express the same immunoglobulin heavy variable gene: ontogenetic implications

et al. 2012

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We performed an immunogenetic analysis of 345 IGHV --IGHD --IGHJ rearrangements from 337 cases with primary splenic small B-cell lymphomas of marginal-zone origin. Three immunoglobulin (IG) heavy variable (IGHV) genes accounted for 45.8% of the cases (IGHV1-2, 24.9%; 12.8%; 8.1%). Particularly for the IGHV1-2 gene, strong biases were evident regarding utilization of different alleles, with 79/86 rearrangements (92%) using allele *04. Among cases more stringently classified as splenic marginal-zone lymphoma (SMZL) thanks to the availability of splenic histopathological specimens, the frequency of IGHV1-2*04 peaked at 31%. The IGHV1-2*04 rearrangements carried significantly longer complementaritydetermining region-3 (CDR3) than all other cases and showed biased IGHD gene usage, leading to CDR3s with common motifs. The great majority of analyzed rearrangements (299/345, 86.7%) carried IGHV genes with some impact of somatic hypermutation, from minimal to pronounced. Noticeably, 75/79 (95%) IGHV1-2*04 rearrangements were mutated; however, they mostly (56/75 cases; 74.6%) carried few mutations (97 --99.9% germline identity) of conservative nature and restricted distribution. These distinctive features of the IG receptors indicate selection by (super)antigenic element(s) in the pathogenesis of SMZL. Furthermore, they raise the possibility that certain SMZL subtypes could derive from progenitor populations adapted to particular antigenic challenges through selection of VH domain specificities, in particular the IGHV1-2*04 allele.

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Section: Discussionmentioning

confidence: 99%

Section: Pcr Amplification Of Ighv --Ighd --Ighj Rearrangementsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Over 30% of patients with splenic marginal zone lymphoma express the same immunoglobulin heavy variable gene: ontogenetic implications

et al. 2012

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“…From a biological standpoint, there are data to suggest that low mutational load in CLL productive rearrangements (leading to a germline identity of X98% but o100%) may have been functionally selected, perhaps providing the clone with certain antigenic reactivities. [15][16][17] The unproductive rearrangement would have been similarly targeted by the SHM process but remained free of any functional constraints and thus left to acquire significantly more mutations of a random nature. Whatever the underlying explanation for this phenomenon, at present, a prognostically relevant interpretation is lacking.…”

Section: Discussionmentioning

confidence: 99%

Immunoglobulin sequence analysis and prognostication in CLL: guidelines from the ERIC review board for reliable interpretation of problematic cases

et al. 2011

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Immunoglobulin gene sequence analysis is widely utilized for prognostication in chronic lymphocytic leukemia (CLL) and the definition of standardized procedures has allowed reliable and reproducible results. Occasionally, a straightforward interpretation of the sequences is not possible because of the so-called 'problematic sequences' that do not fit the 'classic' interpretation and pose scientific questions at the cross-road between hematology and immunology. Thanks to a dedicated effort within the European Research Initiative on CLL (ERIC), we have now the possibility to present such cases, offer a scientific explanation and propose recommendations in terms of prognostication.

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“…All patients were diagnosed according to recently revised criteria and displayed the typical CLL immunophenotype (CD5 1 /CD19 1 /CD23 1 ) [21]. Subsets were defined according to previously described criteria [3,22] (Supporting Information Table 8S). All samples were collected at follow-up (median 82 and range 6-167 months after diagnosis) and contained 90% (average 93%) tumor cells.…”

Section: Methodsmentioning

confidence: 99%

Next generation RNA‐sequencing in prognostic subsets of chronic lymphocytic leukemia

et al. 2012

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Advances in next-generation RNA-sequencing have revealed the complexity of transcriptomes by allowing both coding and noncoding (nc)RNAs to be analyzed. However, limited data exist regarding the whole transcriptional landscape of chronic lymphocytic leukemia (CLL). In this pilot-study, we evaluated RNA-sequencing in CLL by comparing two subsets which carry almost identical or ''stereotyped'' B-cell receptors with distinct clinical outcome, that is the poor-prognostic subset #1 (n 5 4) and the more favorable-prognostic subset #4 (n 5 4). Our analysis revealed that 156 genes (e.g. LPL, WNT9A) and 76 ncRNAs, (e.g. SNORD48, SNORD115) were differentially expressed between the subsets. This technology also enabled us to identify numerous subset-specific splice variants (n 5 406), which were predominantly expressed in subset #1, including a splice-isoform of MSI2 with a novel start exon. A further important application of RNA-sequencing was for mutation detection and revealed 16-30 missense mutations per sample; notably many of these changes were found in genes with a strong potential for involvement in CLL pathogenesis, e.g., ATM and NOTCH2. This study not only demonstrates the effectiveness of RNA-sequencing for identifying mutations, quantifying gene expression and detecting splicing events, but also highlights the potential such global approaches have to significantly advance our understanding of the molecular mechanisms behind CLL development.Chronic lymphocytic leukemia (CLL) is a clinically and biologically heterogeneous disease, with many patients following an indolent disease course, whilst others develop a more aggressive disease. The mutation status of the immunoglobulin heavy variable (IGHV) genes divides CLL into two clinically relevant subgroups, where unmutated IGHV genes ( 40% of patients) are associated with a considerably worse prognosis compared to mutated IGHV genes [1,2]. Moreover, CLL is characterized by multiple subsets carrying quasi-identical or ''stereotyped'' B-cell receptors which imply a role for antigen selection in leukemogenesis [3]. Recently, certain subsets have also been shown to share clinico-biological features [3,4]; for instance, subset #1 patients, which uniformly express unmutated IGHV1/5/7 together with IGKV1(D)-39 genes and a stereotyped heavy complementarity determining region 3 (VH CDR3) of 13-14 amino acids, have a significantly inferior outcome compared to patients expressing the same IGHV genes but without stereotypy [3,5]. In contrast, subset #4 patients (IGHV4-34/IGKV2-30 usage and VH CDR3 of 20 amino acids), have a low median age at diagnosis, express surface IgG and have an indolent disease [3]. Furthermore, we have previously shown that stereotyped subsets can carry a different spectrum of genomic alterations as well as diverse gene expression profiles [6,7]. In the present pilot-study, we applied next-generation RNA-sequencing to compare poor-prognostic subset #1 (n 5 4) with the more favorable prognostic subset #4 (n 5 4, Table I), in order to explore the potential...

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Stereotyped patterns of somatic hypermutation in subsets of patients with chronic lymphocytic leukemia: implications for the role of antigen selection in leukemogenesis

Cited by 295 publications

References 86 publications

Over 30% of patients with splenic marginal zone lymphoma express the same immunoglobulin heavy variable gene: ontogenetic implications

Over 30% of patients with splenic marginal zone lymphoma express the same immunoglobulin heavy variable gene: ontogenetic implications

Immunoglobulin sequence analysis and prognostication in CLL: guidelines from the ERIC review board for reliable interpretation of problematic cases

Next generation RNA‐sequencing in prognostic subsets of chronic lymphocytic leukemia

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