Lauren I. Richie scite author profile

The thymus has been regarded as the major site of T cell differentiation. We find that in addition to αβ and γδ T cells, a significant number (∼3 × 104 per day) of B220+IgM+ mature B cells are exported from the thymus of C57BL/6 mice. Of these emigrating B cells, we estimate that at least ∼2 × 104 per day are cells which developed intrathymically, whereas a maximum of ∼0.8 × 104 per day are cells which circulated through the thymus from the periphery. The thymus possesses a significant number of pro-B and pre-B cells that express CD19, VpreB, λ5, and pax-5. These B cell progenitors were found in the thymic cortex, whereas increasingly mature B cells were found in the corticomedullar and medullary regions. Other lymphoid cells, including NK cells and lymphoid dendritic cells, are not exported from the thymus at detectable levels. Thus, the thymus contributes to the formation of peripheral pools of B cells as well as of αβ and γδ T cells.

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Conservation of T Cell Receptor Conformation in Epidermal γδ Cells with Disrupted Primary V _γ Gene Usage

Mallick-Wood

Lewis

Richie

et al. 1998

Science

115

101

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A feature that distinguishes gammadelta T cell subsets from most alphabeta T cells and B cells is the association of expression of single T cell receptor (TCR) gamma and delta variable (V) region gene segments with specific anatomic sites. Mice lacking the TCR Vgamma5 chain normally expressed by most dendritic epidermal T cells were shown to retain a conformational determinant (idiotype) ordinarily expressed exclusively by such Vgamma5+ cells. Conservation by shuffled gammadelta TCR chains of an idiotype associated with a specific anatomic site indicates that for TCRgammadelta, as for immunoglobulin, conformation is associated to a greater extent with the function or development of lymphocyte repertoires than is the use of particular gene segments.

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Imaging Synapse Formation during Thymocyte Selection

et al. 2002

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TCR signaling can result in cell fates ranging from activation to tolerance to apoptosis. Organization of molecules in an "immunological synapse" between mature T cells and APCs correlates with the strength of TCR signaling. To investigate synapse formation during thymic selection, we have established a reaggregate system in which molecular recruitment of GFP fusion proteins to thymocyte:stromal cell interfaces can be visualized in real time. We demonstrate that negative selection is associated with efficient conjugate formation and rapid recruitment of p56(lck) and CD3zeta to an immunological synapse. Interestingly, CD3zeta-GFP does not accumulate at the center of the synapse, as in mature T cells, but at the periphery across a wide range of ligand densities. This implicates differences in synapse geometry in initiation of alternate signals downstream of the TCR.

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Social process in grizzly bear management: lessons for collaborative governance and natural resource policy

2012

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Lauren I. Richie

B Lymphopoiesis in the Thymus

Conservation of T Cell Receptor Conformation in Epidermal γδ Cells with Disrupted Primary V _γ Gene Usage

Imaging Synapse Formation during Thymocyte Selection

Social process in grizzly bear management: lessons for collaborative governance and natural resource policy

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Lauren I. Richie

B Lymphopoiesis in the Thymus

Conservation of T Cell Receptor Conformation in Epidermal γδ Cells with Disrupted Primary V γ Gene Usage

Imaging Synapse Formation during Thymocyte Selection

Social process in grizzly bear management: lessons for collaborative governance and natural resource policy

Contact Info

Product

Resources

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Conservation of T Cell Receptor Conformation in Epidermal γδ Cells with Disrupted Primary V _γ Gene Usage