Clonal anergy: Persistence in tolerant mice of antigen-binding B lymphocytes incapable of responding to antigen or mitogen

Nossal, G. J. V.; Pike, Beverley L.

doi:10.1073/pnas.77.3.1602

Cited by 219 publications

(126 citation statements)

References 24 publications

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“…Anergy is thought to arise as the immature B cells leave the bone marrow and enter the periphery (12,42,43). If they meet Ags without the appropriate T cell help (CD40 Ligand), they are anergized or deleted.…”

Section: Discussionmentioning

confidence: 99%

B Cells from Mice Prematurely Expressing Human Complement Receptor Type 2 Are Unresponsive to T-Dependent Antigens

Birrell

Kulik

Morgan

et al. 2005

The Journal of Immunology

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Complement receptor type 2 (CR2/CD21), in association with CD19, plays an important role in enhancing mature B cell responses to opsonized Ags. We have shown that mice expressing a human CR2/CD21 (hCR2/CD21) transgene during the CD43+/CD25− late pro-B cell stage of B cell development demonstrate marked changes in subsequent B cell ontogeny. In the present study, we show that the humoral immune response to the T cell-dependent Ag, sheep RBC, is muted severely in a manner inversely proportional to B cell expression level of hCR2. Individual Ag-specific IgG isotypes vary in the degree to which they are affected but all are reduced while IgM titers are normal. A substantial reduction in germinal centers, both in size and frequency, in the spleens of immunized hCR2 transgenic mice demonstrates a failure to maintain germinal center reaction. However, both IgM expression levels and LPS-proliferative responses appear fully intact in B cells from hCR2-positive mice, suggesting that this alteration in B cell phenotype is different qualitatively from that of specific Ag-defined anergy models. These data suggest that the unresponsiveness to T-dependent Ags displayed by hCR2-positive B cells is linked to an increase in the level of stimulus required to propel the B cell into a fully activated state and thus a normal humoral immune response to Ags. We conclude that this phenotype and these mice may offer an additional means to dissect mechanisms underlying B cell tolerance and Ag responsiveness both in bone marrow and periphery.

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Section: Discussionmentioning

confidence: 99%

B Cells from Mice Prematurely Expressing Human Complement Receptor Type 2 Are Unresponsive to T-Dependent Antigens

Birrell

Kulik

Morgan

et al. 2005

The Journal of Immunology

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“…These notions, originally proposed by Nossal and Pike [3,4], were apparently supported by in vivo studies in the HEL/anti-HEL transgenic model, where high avidity BCR interactions led to the elimination of HEL-reactive cells in the bone marrow, while low avidity interactions indeed yielded self-reactive cells in the periphery [5]. However, following description of the TR compartment, Fulcher and Basten demonstrated that these 'anergic' B cells achieved entrance to the TR pools, but nonetheless died rapidly before entering mature pools [6].…”

Section: B Cells Undergo Both Negative and Positive Selection As Theymentioning

confidence: 99%

BAFF and the plasticity of peripheral B cell tolerance

Stadanlick

Cancro

2008

Current Opinion in Immunology

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BAFF and its receptors play a crucial role in peripheral B cell selection and survival, by dictating the set point for mature primary B cell numbers and adjusting thresholds for specificity-based selection during transitional differentiation. The notion that selective stringency can be varied on the basis of homeostatic demands reveals a previously unappreciated degree of plasticity in B cell tolerance, and suggests a paradigm that unites peripheral negative and positive selection with the maintenance of mature B cell numbers. Moreover, it implies a developmentally regulated coupling of BCR and BAFF receptors at the transitional stages and beyond.

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“…Co-stimulatory signals implicated in the activation of the TcR include tyrosine kinases, interleukins, the B7 family (Chen et al, 1993) (Nossal and Pike, 1980;Goodnow et al, 1991). The concept of a population of down-regulated T-and B-cell repertoires with a threshold affinity for silencing was advanced by Nossal (1983) as one of 'immune ignorance'.…”

Section: Mechanisms Of Tumour Escape From Immunological Recognitionmentioning

confidence: 99%

Biological therapy: approaches in colorectal cancer

Zbar

Lemoine²,

Wadhwa³

et al. 1998

Br J Cancer

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Clonal anergy: Persistence in tolerant mice of antigen-binding B lymphocytes incapable of responding to antigen or mitogen

Cited by 219 publications

References 24 publications

B Cells from Mice Prematurely Expressing Human Complement Receptor Type 2 Are Unresponsive to T-Dependent Antigens

B Cells from Mice Prematurely Expressing Human Complement Receptor Type 2 Are Unresponsive to T-Dependent Antigens

BAFF and the plasticity of peripheral B cell tolerance

Biological therapy: approaches in colorectal cancer

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