Ectopic T cell receptor expression causes B cell immunodeficiency in transgenic mice

Lobito, Adrian A.; Lopes, Marcela F.; Lenardo, Michael J.

doi:10.1002/eji.200324675

Cited by 4 publications

(9 citation statements)

References 32 publications

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“…Transgenes under the control of TCRα gene regulatory elements have previously been reported to be ectopically expressed in B cells [2], [3]. Based on the results of our dual-reporter transgene described above, we hypothesized that the Dad1 gene normally present 3′ of the TCRα LCR in the genome might serve to suppress such ectopic B cell expression.…”

Section: Resultsmentioning

confidence: 87%

“…The second is a TCRα/Dad1 bacterial artificial chromosome (BAC) construction in which separate Vα and Dad1 promoter driven reporter genes flank the LCR DNA in its natural context of DNA sequence spanning from the Cα exons through the entire Dad1 genomic locus. Among the significant findings we report here is that neither of the 5′-flanking genes in these “two-gene” reporter systems displayed the ectopic B cell expression that was observed from “single-gene” Vα promoter-driven [2], [3] and heterologous promoter driven [4] reporter constructs studied previously. These data are consistent with a model in which flanking the TCRα LCR with two distinct, active genes results in a T cell restriction to its activity on the upstream-linked gene.…”

Section: Introductionmentioning

confidence: 67%

“…Similar results were obtained from simultaneous analyses of endogenous TCRα mRNA. Thus, unlike the Vα promoter-driven (single transcription unit) transgenes studied previously [2], [3], the Vα promoter-driven hCD2 reporter gene in the dual-reporter TCRα/Dad1 BAC does not display ectopic expression in B cells. Figure 9B shows RT-PCR data confirming that, as expected, the Dad1 promoter driven rCD2 reporter gene is active in B cells of the BAC transgenic mice.…”

Section: Resultsmentioning

confidence: 92%

“…Therefore, despite these important advances, a clear explanation for the restriction of TCRα gene expression to T cells has remained elusive. Nevertheless, this existing information may explain why TCRα transgenes removed from their natural genomic context [3] as well as other transcription units under the control of TCRα gene regulatory elements, such as the TCRα LCR, become expressed in both T and B cells. The latter is true whether or not transcription from the transgene construct is driven by a natural Vα promoter [2] or a heterologous promoter [4].…”

Section: Discussionmentioning

confidence: 99%

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Ectopic T Cell Receptor-α Locus Control Region Activity in B Cells Is Suppressed by Direct Linkage to Two Flanking Genes at Once

et al. 2010

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The molecular mechanisms regulating the activity of the TCRα gene are required for the production of the circulating T cell repertoire. Elements of the mouse TCRα locus control region (LCR) play a role in these processes. We previously reported that TCRα LCR DNA supports a gene expression pattern that mimics proper thymus-stage, TCRα gene-like developmental regulation. It also produces transcription of linked reporter genes in peripheral T cells. However, TCRα LCR-driven transgenes display ectopic transcription in B cells in multiple reporter gene systems. The reasons for this important deviation from the normal TCRα gene regulation pattern are unclear. In its natural locus, two genes flank the TCRα LCR, TCRα (upstream) and Dad1 (downstream). We investigated the significance of this gene arrangement to TCRα LCR activity by examining transgenic mice bearing a construct where the LCR was flanked by two separate reporter genes. Surprisingly, the presence of a second, distinct, reporter gene downstream of the LCR virtually eliminated the ectopic B cell expression of the upstream reporter observed in earlier studies. Downstream reporter gene activity was unaffected by the presence of a second gene upstream of the LCR. Our findings indicate that a gene arrangement in which the TCRα LCR is flanked by two distinct transcription units helps to restrict its activity, selectively, on its 5′-flanking gene, the natural TCRα gene position with respect to the LCR. Consistent with these findings, a TCRα/Dad1 locus bacterial artificial chromosome dual-reporter construct did not display the ectopic upstream (TCRα) reporter expression in B cells previously reported for single TCRα transgenes.

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Section: Resultsmentioning

confidence: 87%

Section: Introductionmentioning

confidence: 67%

Section: Resultsmentioning

confidence: 92%

Section: Discussionmentioning

confidence: 99%

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Ectopic T Cell Receptor-α Locus Control Region Activity in B Cells Is Suppressed by Direct Linkage to Two Flanking Genes at Once

et al. 2010

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“…Subsequent transgenic studies have detected B cell expression in transgene configurations involving TCR␣ LCR elements. However, these studies used either indirectly linked, cointegrated TCR␣ LCR (45) or incomplete TCR␣ LCR cointegrated with a TCR␤ transgene (46). We directly addressed this question at single-cell resolution in a directly linked, complete LCR-driven reporter transgene system free of integration site-dependent position effects.…”

Section: Discussionmentioning

confidence: 99%

The TCRα Locus Control Region Specifies Thymic, But Not Peripheral, Patterns of TCRα Gene Expression

Harrow

Ortiz

2005

The Journal of Immunology

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The molecular mechanisms ensuring the ordered expression of TCR genes are critical for proper T cell development. The mouse TCR α-chain gene locus contains a cis-acting locus control region (LCR) that has been shown to direct integration site-independent, lymphoid organ-specific expression of transgenes in vivo. However, the fine cell type specificity and developmental timing of TCRα LCR activity are both still unknown. To address these questions, we established a transgenic reporter model of TCRα LCR function that allows for analysis of LCR activity in individual cells by the use of flow cytometry. In this study we report the activation of TCRα LCR activity at the CD4−CD8−CD25−CD44− stage of thymocyte development that coincides with the onset of endogenous TCRα gene rearrangement and expression. Surprisingly, TCRα LCR activity appears to decrease in peripheral T cells where TCRα mRNA is normally up-regulated. Furthermore, LCR-linked transgene activity is evident in γδ T cells and B cells. These data show that the LCR has all the elements required to reliably reproduce a developmentally correct TCRα-like expression pattern during thymic development and unexpectedly indicate that separate gene regulatory mechanisms are acting on the TCRα gene in peripheral T cells to ensure its high level and fine cell type-specific expression.

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B lymphocyte deficiency in IgH‐transgenic rabbits

et al. 2007

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We developed IgH-transgenic rabbits carrying a productive VDJ-Cl Tg and found the rabbits were B cell-deficient, with a 50-100% reduction in serum IgM and IgG levels. The bone marrow of newborn Tg rabbits contained severely reduced levels of preB cells and almost no B cells. The few preB cells present in the bone marrow were large, cycling cells that expressed the VDJ-Cl Tg, indicating that the block in B cell development likely occurred at or before the transition from large (early) preB to small (late) preB cells. By immunoprecipitation, the Tg l-chain paired with VpreB and k5, suggesting that the B cell deficiency is not due to an inability to form a preB cell receptor. Despite the block in B cell development, a few B cells, expressing predominantly endogenous l-chains, began the second stage of development in GALT. B cells were localized in and beneath the follicle-associated epithelium of GALT prior to B cell follicle formation, suggesting to us that B cell follicle formation is initiated near the follicle-associated epithelium, possibly through contact with intestinal microbiota. These IgH-Tg rabbits should provide a useful model for studies of B cell development both in bone marrow and in GALT.

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Ectopic T cell receptor expression causes B cell immunodeficiency in transgenic mice

Cited by 4 publications

References 32 publications

Ectopic T Cell Receptor-α Locus Control Region Activity in B Cells Is Suppressed by Direct Linkage to Two Flanking Genes at Once

Ectopic T Cell Receptor-α Locus Control Region Activity in B Cells Is Suppressed by Direct Linkage to Two Flanking Genes at Once

The TCRα Locus Control Region Specifies Thymic, But Not Peripheral, Patterns of TCRα Gene Expression

B lymphocyte deficiency in IgH‐transgenic rabbits

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