Genetic and temporal control of neonatal antibody expression.

Denis, Kathleen A.

doi:10.1084/jem.157.4.1170

Cited by 36 publications

(16 citation statements)

References 49 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Furthermore, an important observation was the major contribution of VH 36-60 expression to the DNP response . This was most pronounced in the fetal response and is consistent with our previous results indicating that predominant idiotypes 36 (52) and 460 (53)(54)(55), both associated with VH 36-60 (35,55,56), were produced in the DNP-specific fetal response (56) . In addition, the 460 idiotype is also a predominant idiotype found in the adult DNP response (53)(54)(55).…”

Section: Discussionsupporting

confidence: 79%

“…The results suggest that the anti-DNP response, in general, is very heterogeneous and that member(s) of all of the VH gene families tested can potentially code for anti-DNP antibodies in both the fetus and adult. The heterogeneous nature of the anti-DNP response and the ability of anti-DNP antibodies to be encoded by more than one VH gene family is consistent with other reports (35,(52)(53)(54)(55) .…”

Section: Discussionsupporting

confidence: 79%

See 1 more Smart Citation

Comparison of the fetal and adult functional B cell repertoires by analysis of VH gene family expression.

Jeong

Teale

1988

The Journal of Experimental Medicine

102

View full text Add to dashboard Cite

The functional B cell repertoire in BALB/c mice was assessed at various stages in ontogeny. This was done by analyzing VH gene family expression using the sensitive technique of in situ hybridization. The B cell repertoire was probed with the mitogen, LPS, and the antigen DNP. DNP was chosen because B cells responsive to this hapten appear very early in ontogeny. The APCs that developed after stimulation with LPS or DNP were analyzed for VH gene expression by in situ hybridization of individual cells using radiolabeled VH gene family probes. The results indicated that VH gene expression in fetal B cells after stimulation was distinct from adult B cells in that there was a biased expression of D proximal families. The results indicated that this bias was associated with developmental age and not a given differentiation stage in the B cell lineage. In addition, stimulation of fetal B cells with DNP resulted in a large increase in expression of member(s) of VH 36-60, suggesting that the early appearance of DNP-responsive B cells is not strictly correlated with preferential rearrangement of D proximal families, VH 7183 and VH Q52. However, the results suggested that a large proportion of pre-B cells that preferentially rearrange D proximal families early in ontogeny become part of the functional developing repertoire.

show abstract

Section: Discussionsupporting

confidence: 79%

Section: Discussionsupporting

confidence: 79%

Comparison of the fetal and adult functional B cell repertoires by analysis of VH gene family expression.

Jeong

Teale

1988

The Journal of Experimental Medicine

102

View full text Add to dashboard Cite

show abstract

“…During the first weeks after birth, this repertoire undergoes a reproducible and patterned expansion (3)(4)(5)(6)(7)(8)(9). Thus, in the first 3 days of neonatal life, all BALB/c neonates share three predominant 2,4-dinitrophenyl (DNP)-specific and three predominant 2,4,6-trinitrophenyl (TNP)-specific clonotypes (3).…”

mentioning

confidence: 99%

“…Although the adult primary B-cell repertoire ofBALB/c mice exceeds 107 conotypes (1,2), the antibody repertoire at birth is limited to 104-105 different specificities (3,4). During the first weeks after birth, this repertoire undergoes a reproducible and patterned expansion (3)(4)(5)(6)(7)(8)(9).…”

mentioning

confidence: 99%

“…In order to evaluate the contribution of such a developmentally ordered rearrangement of V segments to the repertoire of antigen-responsive B cells, we have examined the V genes utilized by three hybridomas derived by fusion of DNP-hemocyanin-stimulated neonatal spleen cells (4). The idiotypes expressed by the antibody products ofeach ofthese three hybridomas have been shown to be expressed independently on a high proportion of the anti-DNP monoclonal antibody products of BALB/c neonatal spleen cells (4).…”

mentioning

confidence: 99%

See 1 more Smart Citation

Preferential expression of variable region heavy chain gene segments by predominant 2,4-dinitrophenyl-specific BALB/c neonatal antibody clonotypes.

Riley¹,

Connors²,

Klinman³

et al. 1986

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

The B-cell repertoire in neonatal mice contains predominant clonotypes that are reproducibly expressed at particular times after birth. We have isolated and sequenced heavy and light chain cDNA clones from three 2,4-dinitrophenyl-specific neonatal hybridomas. Two of these hybridomas (TF2-36 and TF5-139) express idiotypes (Ids) that predominate during the first days after birth, and the third hybridoma (TF2-76) expresses Although the adult primary B-cell repertoire ofBALB/c mice exceeds 107 conotypes (1, 2), the antibody repertoire at birth is limited to 104-105 different specificities (3, 4). During the first weeks after birth, this repertoire undergoes a reproducible and patterned expansion (3-9). Thus, in the first 3 days of neonatal life, all BALB/c neonates share three predominant 2,4-dinitrophenyl (DNP)-specific and three predominant 2,4,6-trinitrophenyl (TNP)-specific clonotypes (3). The same mice do not express predominant clonotypes for fluorescein (3), phosphocholine (6), and either a(1-*3) or a(1--6) dextran determinants (7,8). Phosphocholine-specific clones reproducibly appear several days after DNP-or TNP-specific clones in both fetal liver (9) and neonatal spleen (6). Two weeks after birth, the antibody repertoire, which contains 106 specificities, is still more restricted than the adult repertoire (5).Recently, several investigators have attempted to correlate this patterned acquisition of the antibody repertoire with the preferential rearrangement of specific variable (V) region gene segments (10, 11). Murine germ-line heavy (H) chain V region gene segments (VH) have been grouped by sequence homologies into eight families (12, 13). VH recombinant strains have been used to obtain the order of these VH families, whose names relate to cell lines, on chromosome 12 as: 5' (VH 3609, VH 36-60, VH J606, VH X24)-VH J558-VH S107-VH Q52-VH 7183-D-JH 3' (14). The relative order ofthe set of VH gene families 5' to the J558 VH family cannot be mapped with the existing recombinant strains. The potential correlation between sequential rearrangement of V segments and sequential expression of antibody specificities is based on the observation that the rearrangement of VH families in fetal liver pre-B-cells is not random (10, 11). Cells with a rearranged member of the 7183 VH family have been the most frequently found among Abelson murine leukemia virus (Ab-MuLV)-transformed pre-B-cells and among fetal liver pre-B-cell hybridomas. This is especially striking because the 7183 VH family represents only z10% of all VH genes (13). One member of the 7183 VH family, VH 81X, rearranges at a particularly high frequency. VH 81X, one of the most JHproximal VH regions, is rearranged in almost half of AbMuLV-transformed fetal liver pre-B-cells (10).In order to evaluate the contribution of such a developmentally ordered rearrangement of V segments to the repertoire of antigen-responsive B cells, we have examined the V genes utilized by three hybridomas derived by fusion of DNP-hemocyanin-stimulated neonatal spleen cell...

show abstract

Functional Maturation of B Cell Repertoire Expression

Froscher

1987

Antibodies

View full text Add to dashboard Cite

Genetic and temporal control of neonatal antibody expression.

Cited by 36 publications

References 49 publications

Comparison of the fetal and adult functional B cell repertoires by analysis of VH gene family expression.

Comparison of the fetal and adult functional B cell repertoires by analysis of VH gene family expression.

Preferential expression of variable region heavy chain gene segments by predominant 2,4-dinitrophenyl-specific BALB/c neonatal antibody clonotypes.

Functional Maturation of B Cell Repertoire Expression

Contact Info

Product

Resources

About