Preferential utilization of specific immunoglobulin heavy chain diversity and joining segments in adult human peripheral blood B lymphocytes.

Yamada, Masao; Wasserman, Robert; Reichard, Betty Anne; Shane, Sara; Caton, Andrew J.; Rovera, Giovanni

doi:10.1084/jem.173.2.395

Cited by 345 publications

(222 citation statements)

References 19 publications

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“…In contrast, an extraordinary diversity in length and composition of the CDR3 was described for a set of RA-derived polyreactive antibodies and RF [30] and rearranged V H genes from PBL of a healthy donor [17]. For the J H segments we can confirm a predominant use of J H 4 [17,19].…”

Section: Discussionmentioning

confidence: 89%

Evidence for a selected humoral immune response encoded by VH4 family genes in the synovial membrane of a patient with rheumatoid arthritis (RA)

Voswinkel

Trümper

Carbon

et al. 1996

Clinical and Experimental Immunology

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SUMMARYThe analysis of rearranged antibody-encoding genes from B cell foci in rheumatoid synovial tissue has characterized these cells as highly mutated memory B cells with a high proportion of members of the V H 4 family. In order to characterize further the V H 4 response in one patient, B cell-rich areas from different sections of synovial membrane (SM) were identified by CD20 staining, isolated by microdissection and pooled, in order to analyse highly enriched B cells without selection by in vitro culture procedures. From DNA of about 5 2 10 3 B cells rearranged V H genes were amplified by polymerase chain reaction (PCR) and cloned. Sequencing of 11 clones containing rearranged V H 4 gene products revealed that seven were potentially functional, and all were mutated with 84-96% homology to known germ-line (gl) genes and V H 4 gl genes amplified from the patient's genomic DNA. Analysis of the complementarity determining region (CDR) 3 revealed that two products represented members of one B cell clone which differed by five nucleotide changes. Three of the five mutations encoded amino acid replacements in CDRs indicating antigen-driven expansion of one specific clone. Additional analyses of 25 members of three B cell clones from isolated aggregates showing intraclonal diversity in one of three clones provided further evidence that antigen selection takes place in the SM. Overall, the pattern of mutations and the replacement to silent (R:S) ratios were diverse, with six products indicating antigen selection by their high R:S ratios in CDRs. Although DNA analysis does not allow a characterization of antibody specificities, we can conclude from our analysis of antibody-encoding genes that selection by antigen and expansion of specific clones occur in the SM against the background of polyclonal activation.

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Section: Discussionmentioning

confidence: 89%

Evidence for a selected humoral immune response encoded by VH4 family genes in the synovial membrane of a patient with rheumatoid arthritis (RA)

Voswinkel

Trümper

Carbon

et al. 1996

Clinical and Experimental Immunology

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“…In the rearrangement of the IgH gene, the usage of J H segments revealed a developmental stage-specific trend. [7][8][9][10][11][12][13] At the earliest stage of B cell development, the initial D-J H rearrangements predominantly occur between D H Q52 and J H -1 segments which are located close to each other. 53 During B cell development, a second or a third D-J H joining might occur, then the more 5ЈD segments and more 3ЈJ H segments would join at a later stage.…”

Section: Figurementioning

confidence: 99%

“…6 Studies on IgH variable region gene sequences at various stages of development have revealed stage-specific trends in the usage of V H , D, and J H segments, the degree of N nucleotide addition, and the rate of somatic mutations. [7][8][9][10][11][12][13] However, little is known of the organization and diversification of the IgL variable region gene on -chain. On the other hand, multiple myeloma (MM) has a variety of clinical features relating to clinical stage, prognosis and complication.…”

Section: Introductionmentioning

confidence: 99%

Characterization of the immunoglobulin light chain variable region gene expressed in multiple myeloma

et al. 1998

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We studied the organization, diversification and clinical significance of the immunoglobulin light chain (IgL) variable region genes expressed in 17 -chain and 16 -chain producing multiple myeloma (MM) samples. The V genes from 31 MM samples had over 84.9% homology to the known germline V / genes, whereas one V and one V gene had only 75.5% and 65.9% homology, respectively. While all five J segments were equally used, only J -1 or J -2/3 was used among seven J segments. N nucleotide addition was found at two V -J and five V -J junctions. The -chain complementarity determining region (CDR)-3 was longer and more variable than the -chain CDR-3 mainly due to junctional flexibility of V and J segments. Somatic mutations were more frequent in the J than the J segments, and were distributed in the CDR-3 as well as the frame work region (FWR)-4. Those of the J segments, however, were limited to FWR-4. In FWR-4, replacement mutations were clustered at codon 106 of -chain and 103 of -chain. Thus nucleotide mutation or conservation was dependent on position, indicating a structural necessity of IgL for the development of myeloma cells in addition to a non-random distribution of mutations. There was no characteristic IgL sequence according to the isotype of M-protein, clinical stage or renal complication.

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“…After alkaline denaturation and UV cross-linking of the DNA, the filters were hybridized with the CDR3-specific oligonucleotide probes and a JHC probe (Figure 1). 25 Pre-hybridization was performed in 6 × SSC (20 × SSC: 3 mol/l NaCl, 0.3 mol/l Na citrate, pH 7.0), 10 × Denhardt's (0.2% w/v Ficoll, 0.2% w/v polyvinyl pyrrolidone, 0.2% w/v BSA), 1% SDS and 100 g/ l boiled herring sperm DNA at 55°C. After prehybridization the denatured 32 P-labeled olignucleotide probes were added and the filters were hybridized at 55°C overnight.…”

Section: Hybridization To Pcr-amplified Cdna Librariesmentioning

confidence: 99%

“…The JHC probe consists of a mixture of four different oligonucleotides derived from the sequences of JH2, JH3, JH4 and JH6 genes. 25 To ensure that the JH4 olignucleotide also hybridized to JH1 and JH5 gene sequences, the hybridization was performed at 35°C and the filters were washed at lower stringency, ie 1 × SSC, 1% SDS at RT.…”

Section: Hybridization To Pcr-amplified Cdna Librariesmentioning

confidence: 99%

Oligoclonal dominance of immunglobulin VH3 rearrangements following allogeneic bone marrow transplantation

Näsman-Björk

Lundkvist

1998

Bone Marrow Transplant

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Summary:Normal numbers of circulating B lymphocytes are reached during the first 6 months following allogeneic BMT, but humoral immunity remains poor. The molecular basis for this lack of function in the first appearing B lymphocytes has not been clarified. Accordingly, we have studied the reconstitution of the VH3 containing Ig repertoire in two CML patients transplanted with allogeneic BM and one healthy control. PBMCs were isolated at several time-points after BMT and mRNA was prepared. VH3 containing Ig rearrangements were amplified with RT-PCR and then cloned and analyzed with colony hybridization using complementary determining region 3 (CDR3)-specific oligonucleotide probes. Four weeks after BMT, two individual clones together represented 52% of the analyzed CDR3 regions. At 6, 8 and 12 weeks after BMT the corresponding probes hybridized with 2-6% of the colonies. A similar pattern was obtained for the other patient. In samples from the healthy control no clones were detected using CDR3-specific oligonucleotide probes from the control. We conclude that the VH3 containing Ig repertoire after BMT is oligoclonal and that specific rearrangements dominate at different time-points. This restriction of the B cell repertoire may contribute to the impaired humoral immunity observed in BMT recipients.

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Preferential utilization of specific immunoglobulin heavy chain diversity and joining segments in adult human peripheral blood B lymphocytes.

Cited by 345 publications

References 19 publications

Evidence for a selected humoral immune response encoded by VH4 family genes in the synovial membrane of a patient with rheumatoid arthritis (RA)

Evidence for a selected humoral immune response encoded by VH4 family genes in the synovial membrane of a patient with rheumatoid arthritis (RA)

Characterization of the immunoglobulin light chain variable region gene expressed in multiple myeloma

Oligoclonal dominance of immunglobulin VH3 rearrangements following allogeneic bone marrow transplantation

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