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2020 年度 実施状況報告書

The role of the transcription factor Tox2 in Treg and Tfh biology

研究課題

研究課題/領域番号 18K07175
研究機関大阪大学

研究代表者

ウィング ジェイムス  大阪大学, 免疫学フロンティア研究センター, 特任准教授(常勤) (00648694)

研究期間 (年度) 2018-04-01 – 2022-03-31
キーワードRegulatory T-cells / T-follicular regulatory / T-follicular helper / Mass Cytometry (CyTOF)
研究実績の概要

We have now bred the Tox2 flox mice to Foxp3-IRES-Cre mice and found some evidence of disruption of the germinal center environment and particularly IgA producing B-cells in the payer’s patch of the gut environment. This suggests that Tox2 expressing Tregs and particualrly Tfr may have their function regulated by Tox2.
Since Tox2 appears to be upregulated by TCR stimulation in vitro we have used CRISPR KO of around 50 genes in human cells to determine the effect of components of TCR signaling pathways on the expression of Tox2 in CD4 T-cells. Here we find that particularly modulation of the tumor necrosis factor alpha-induced protein 3 (TNFAIP3/A20) a negative regulator of TCR mediated Nf-KB function. The expression of Tox2 correlates with expression of it family member Tox to a certain extent but does not have an identical expression profile.

現在までの達成度 (区分)
現在までの達成度 (区分)

3: やや遅れている

理由

We did have some disruption of our plans due to the COVID-19 outbreak. In particular this affected staff recruitment due to the difficulty of international travel. As a result, we requested some carry over of funding into a fourth year.

今後の研究の推進方策

Our plan for the next year is more detailed analysis of the effect of the loss of Tox2 on murine Tregs by vaccination experiments. In these experiments we will vaccinate mice with NP-Ova allowing the detailed measurement of changes to antibody responses and germinal center formation. We will also closely monitor the formation of antigen specific plasma cells since recent accumulating evidence is that Tfr have a particularly important role in plasma cell formation.
We have also further refined our Mass cytometry technique to allow the monitoring of the immunometabolism and will use this to define any effects of Tox2 on metabolic parameter of Tregs. Tox is known to have some role in the control of the immunometabolism so we also expect some effect from Tox2.
Additionally, we will monitor the effect of Tox2 CRISPR on human cells particularly in the context of changes to the immunometabolism by mass cytometry and chromatin accessibility as measured by single-cell Assay for Transposase Accessible Chromatin by sequencing (scATAC-seq) a novel form of sequencing that we recently contributed too the invention of.

次年度使用額が生じた理由

We did have some disruption of our plans due to the COVID-19 outbreak. As a result, we requested some carry over of funding into a fourth year. The research plan is not substantially altered by this.

  • 研究成果

    (2件)

すべて 2021 2020

すべて 雑誌論文 (2件) (うち国際共著 2件、 査読あり 1件)

  • [雑誌論文] CTLA-4 expression by B-1a B cells is essential for immune tolerance2021

    • 著者名/発表者名
      Yang Y、Li X、Ma Z、Wang C、Yang Q, Byrne-Steele M、Hong R、Min Q、Zhou G、Cheng Y、Qin G、Youngyunpipatkul JV.、Wing JB.、Sakaguchi S、Toonstra C、Wang L-X、Vilches-Moure JG.、Wang D、Snyder MP.、Wang J-Y、Han J、Herzenberg LA.
    • 雑誌名

      Nature Communications

      巻: 12 ページ: 1-17

    • DOI

      10.1038/s41467-020-20874-x

    • 査読あり / 国際共著
  • [雑誌論文] Control of foreign Ag‐specific Ab responses by Treg and Tfr2020

    • 著者名/発表者名
      Wing James B.Lim Ee Lyn、Sakaguchi Shimon
    • 雑誌名

      Immunological Reviews

      巻: 296 ページ: 104~119

    • DOI

      10.1111/imr.12888

    • 国際共著

URL: 

公開日: 2021-12-27  

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