Maria Karvelas scite author profile

Oct-2, a POU homeo domain transcription factor, is believed to stimulate B-cell-restricted expression of immunoglobulin genes through binding sites in immunoglobulin gene promoters and enhancers. To determine whether Oct-2 is required for B-cell development or function, or has other developmental roles, the gene was disrupted by homologous recombination. Oct-2 -/-mice develop normally but die within hours of birth for undetermined reasons. Mutants contain normal numbers of B-cell precursors but are somewhat deficient in IgM + B cells. These B cells have a marked defect in their capacity to secrete immunoglobulin upon mitogenic stimulation in vitro. Thus, Oct-2 is not required for the generation of immunoglobulin-bearing B cells but is crucial for their maturation to immunoglobulin-secreting cells and for another undetermined organismal function.

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Modelling the hepatitis C virus epidemic in Australia

Razali¹,

Thein²,

Bell³

et al. 2007

Drug and Alcohol Dependence

121

110

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Oct-2 is required early in T cell-independent B cell activation for G1 progression and for proliferation

1994

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Soluble antigen profoundly reduces memory B-cell numbers even when given after challenge immunization.

Nossal

Karvelas

Pulendran

1993

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

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The splenic B-cell repertoire of unimmunized C57BL/6 mice can be examined for anti-(4-hydroxy-3-nitrophenyl)acetyl (NP) B cells of relatively high affinity by using a dual strategy. (14,15) and showed that it could prevent the generation of anti-HSA memory B cells in a dose-dependent manner. Adoptive transfer studies showed that the toleragen affected donor T and B cells, the former effect being more profound. Another way of studying the relative contributions of Tand B-lymphocyte populations to an antibody response is to make use of various hapten-carrier combinations (16-18). T-dependent anti-hapten antibody formation requires that anti-hapten B cells be "helped" by carrier-specific T cells. The anti-(4-hydroxy-3-nitrophenyl)acetyl (NP) response of C57BL/6 mice has been extensively investigated (19-21) because of the preferential appearance of B-cell clones utilizing the VH 186.2 V gene and the Al light chain gene, facilitating the study of V gene hypermutation. It is also a system in which clones making relatively high-versus relatively low-affinity antibody can be discriminated by the use of, respectively, relatively lowly versus relatively highly haptenated protein conjugates in an ELISA (22,23). In the present study, we immunized mice with highly haptenated NP-HSA, and attempted tolerance induction with lowly haptenated, freshly deaggregated, NP-HSA, with HSA carrier alone, or with NP attached to irrelevant carriers. The key findings were that NP-HSA .Jways worked better than carrier alone or NP attached i other carriers in preventing memory cell appearance and that tolerance could still be induced after immunogenic challenge, up to the time of the first appearance of V gene mutations. Apparently, the functional silencing of T and B cells is necessary for the full tolerance effect, and T-ceil help is still required for continued B-memory cell generation after the germinal center reaction is well under way.

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Maria Karvelas

Oct-2, although not required for early B-cell development, is critical for later B-cell maturation and for postnatal survival.

Modelling the hepatitis C virus epidemic in Australia

Oct-2 is required early in T cell-independent B cell activation for G1 progression and for proliferation

Soluble antigen profoundly reduces memory B-cell numbers even when given after challenge immunization.

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