ab versus gd fate choice: counting the T-cell lineages at the branch point
Both ab and gd T cells develop in the thymus from a common progenitor. Historically distinguished by their T-cell receptor (TCR), these lineages are now defined on the basis of distinct molecular programs. Intriguingly, in many transgenic and knockout systems these programs are mismatched with the T...
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| Published in | Immunological reviews Vol. 238; no. 1; pp. 169 - 181 |
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| Main Authors | , , , |
| Format | Journal Article |
| Language | English |
| Published |
01.11.2010
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| Subjects | |
| Online Access | Get full text |
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| Abstract | Both ab and gd T cells develop in the thymus from a common progenitor. Historically distinguished by their T-cell receptor (TCR), these lineages are now defined on the basis of distinct molecular programs. Intriguingly, in many transgenic and knockout systems these programs are mismatched with the TCR type, leading to the development of gd lineage cells driven by abTCR and vice versa. These puzzling observations were recently explained by the demonstration that TCR signal strength, rather than TCR type per se, instructs lineage fate, with stronger TCR signal favoring gd and weaker signal favoring ab lineage fates. These studies also highlighted the ERK (extracellular signal regulated kinase)-Egr (early growth response)-Id3 (inhibitor of differentiation 3) axis as a potential molecular switch downstream of TCR that determines lineage choice. Indeed, removal of Id3 was sufficient to redirect TCRgd transgenic cells to the ab lineage, even in the presence of strong TCR signal. However, in TCR non-transgenic Id3 knockout mice the overall number of gd lineage cells was increased due to an outgrowth of a Vg1Vd6.3 subset, suggesting that not all gd T cells depend on this molecular switch for lineage commitment. Thus, the gd lineage may in fact be a collection of two or more lineages not sharing a common molecular program and thus equipollent to the ab lineage. TCR signaling is not the only factor that is required for development of ab and gd lineage cells; other pathways, such as signaling from Notch and CXCR4 receptors, cooperate with the TCR in this process. |
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| AbstractList | Both ab and gd T cells develop in the thymus from a common progenitor. Historically distinguished by their T-cell receptor (TCR), these lineages are now defined on the basis of distinct molecular programs. Intriguingly, in many transgenic and knockout systems these programs are mismatched with the TCR type, leading to the development of gd lineage cells driven by abTCR and vice versa. These puzzling observations were recently explained by the demonstration that TCR signal strength, rather than TCR type per se, instructs lineage fate, with stronger TCR signal favoring gd and weaker signal favoring ab lineage fates. These studies also highlighted the ERK (extracellular signal regulated kinase)-Egr (early growth response)-Id3 (inhibitor of differentiation 3) axis as a potential molecular switch downstream of TCR that determines lineage choice. Indeed, removal of Id3 was sufficient to redirect TCRgd transgenic cells to the ab lineage, even in the presence of strong TCR signal. However, in TCR non-transgenic Id3 knockout mice the overall number of gd lineage cells was increased due to an outgrowth of a Vg1Vd6.3 subset, suggesting that not all gd T cells depend on this molecular switch for lineage commitment. Thus, the gd lineage may in fact be a collection of two or more lineages not sharing a common molecular program and thus equipollent to the ab lineage. TCR signaling is not the only factor that is required for development of ab and gd lineage cells; other pathways, such as signaling from Notch and CXCR4 receptors, cooperate with the TCR in this process. |
| Author | von Boehmer, Harald Kreslavsky, Taras Garbe, Annette I Gleimer, Michael |
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| DOI | 10.1111/j.1600-065X.2010.00947.x |
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| Snippet | Both ab and gd T cells develop in the thymus from a common progenitor. Historically distinguished by their T-cell receptor (TCR), these lineages are now... |
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| SubjectTerms | Antibodies CXCR4 protein Differentiation double prime T-cell receptor Enumeration Extracellular signal-regulated kinase Lymphocytes T Notch protein Signal transduction Stem cells Thymus |
| Title | ab versus gd fate choice: counting the T-cell lineages at the branch point |
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