Regulation of γδ versus αβ T lymphocyte differentiation by the transcription factor SOX13

Heather J. Melichar; Kavitha Narayan; Sandy O. Der; Yoshiki Hiraoka; Noemie Gardiol; Gregoire Jeannet; Werner Held; Cynthia A. Chambers; Joonsoo Kang

doi:10.1126/science.1135344

Regulation of γδ versus αβ T lymphocyte differentiation by the transcription factor SOX13

Heather J. Melichar, Kavitha Narayan, Sandy O. Der, Yoshiki Hiraoka, Noemie Gardiol, Gregoire Jeannet, Werner Held, Cynthia A. Chambers, Joonsoo Kang

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134 被引用数 (Scopus)

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αβ and γδ T cells originate from a common, multipotential precursor population in the thymus, but the molecular mechanisms regulating this lineage-fate decision are unknown. We have identified Sox13 as a γδ-specific gene in the immune system. Using Sox13 transgenic mice, we showed that this transcription factor promotes γδ T cell development while opposing αβ T cell differentiation. Conversely, mice deficient in Sox13 expression exhibited impaired development of γδ cells but not αβ T cells. One mechanism of SOX13 function is the inhibition of signaling by the developmentally important Wnt/T cell factor (TCF) pathway. Our data thus reveal a dominant pathway regulating the developmental fate of these two lineages of T lymphocytes.

本文言語	English
ページ（範囲）	230-233
ページ数	4
ジャーナル	Science
巻	315
号	5809
DOI	https://doi.org/10.1126/science.1135344
出版ステータス	Published - 2007 1月 12

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10.1126/science.1135344

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abstract = "αβ and γδ T cells originate from a common, multipotential precursor population in the thymus, but the molecular mechanisms regulating this lineage-fate decision are unknown. We have identified Sox13 as a γδ-specific gene in the immune system. Using Sox13 transgenic mice, we showed that this transcription factor promotes γδ T cell development while opposing αβ T cell differentiation. Conversely, mice deficient in Sox13 expression exhibited impaired development of γδ cells but not αβ T cells. One mechanism of SOX13 function is the inhibition of signaling by the developmentally important Wnt/T cell factor (TCF) pathway. Our data thus reveal a dominant pathway regulating the developmental fate of these two lineages of T lymphocytes.",

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AU - Melichar, Heather J.

AU - Narayan, Kavitha

AU - Der, Sandy O.

AU - Hiraoka, Yoshiki

AU - Gardiol, Noemie

AU - Jeannet, Gregoire

AU - Held, Werner

AU - Chambers, Cynthia A.

AU - Kang, Joonsoo

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N2 - αβ and γδ T cells originate from a common, multipotential precursor population in the thymus, but the molecular mechanisms regulating this lineage-fate decision are unknown. We have identified Sox13 as a γδ-specific gene in the immune system. Using Sox13 transgenic mice, we showed that this transcription factor promotes γδ T cell development while opposing αβ T cell differentiation. Conversely, mice deficient in Sox13 expression exhibited impaired development of γδ cells but not αβ T cells. One mechanism of SOX13 function is the inhibition of signaling by the developmentally important Wnt/T cell factor (TCF) pathway. Our data thus reveal a dominant pathway regulating the developmental fate of these two lineages of T lymphocytes.

AB - αβ and γδ T cells originate from a common, multipotential precursor population in the thymus, but the molecular mechanisms regulating this lineage-fate decision are unknown. We have identified Sox13 as a γδ-specific gene in the immune system. Using Sox13 transgenic mice, we showed that this transcription factor promotes γδ T cell development while opposing αβ T cell differentiation. Conversely, mice deficient in Sox13 expression exhibited impaired development of γδ cells but not αβ T cells. One mechanism of SOX13 function is the inhibition of signaling by the developmentally important Wnt/T cell factor (TCF) pathway. Our data thus reveal a dominant pathway regulating the developmental fate of these two lineages of T lymphocytes.

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Regulation of γδ versus αβ T lymphocyte differentiation by the transcription factor SOX13

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