Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 E proteins orchestrate dynamic transcriptional cascades implicated in the suppression of the differentiation of group 2 innate lymphoid cells.

Literature DB >> 32817168

E proteins orchestrate dynamic transcriptional cascades implicated in the suppression of the differentiation of group 2 innate lymphoid cells.

Vincent Peng¹, Constantin Georgescu², Anna Bakowska³, Aneta Pankow³, Liangyue Qian³, Jonathan D Wren², Xiao-Hong Sun⁴.

Abstract

Group 2 innate lymphoid cells (ILC2s) represent a subset of newly discovered immune cells that are involved in immune reactions against microbial pathogens, host allergic reactions, as well as tissue repair. The basic helix-loop-helix transcription factors collectively called E proteins powerfully suppress the differentiation of ILC2s from bone marrow and thymic progenitors while promoting the development of B and T lymphocytes. How E proteins exert the suppression is not well understood. Here we investigated the underlying molecular mechanisms using inducible gain and loss of function approaches in ILC2s and their precursors, respectively. Cross-examination of RNA-seq and ATAC sequencing data obtained at different time points reveals a set of genes that are likely direct targets of E proteins. Consequently, a widespread down-regulation of chromatin accessibility occurs at a later time point, possibly due to the activation of transcriptional repressor genes such as Cbfa2t3 and Jdp2 The large number of genes repressed by gain of E protein function leads to the down-regulation of a transcriptional network important for ILC2 differentiation.

Entities: Disease Gene

Keywords: E2A; HEB; ILC2; MTG16; basic helix-loop-helix transcription factor (bHLH); innate immunity; innate lymphoid cells; lymphocyte; repressor protein; transcription factor

Year: 2020 PMID： 32817168 PMCID： PMC7606671 DOI： 10.1074/jbc.RA120.013806

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

45 in total

Review 1. Helix-loop-helix proteins and lymphocyte development.

Authors: Cornelis Murre
Journal: Nat Immunol Date: 2005-11 Impact factor: 25.606

Review 2. Wnt signaling in normal and malignant hematopoiesis.

Authors: William Lento; Kendra Congdon; Carlijn Voermans; Marcie Kritzik; Tannishtha Reya
Journal: Cold Spring Harb Perspect Biol Date: 2013-02-01 Impact factor: 10.005

3. Differentiation of type 1 ILCs from a common progenitor to all helper-like innate lymphoid cell lineages.

Authors: Christoph S N Klose; Melanie Flach; Luisa Möhle; Leif Rogell; Thomas Hoyler; Karolina Ebert; Carola Fabiunke; Dietmar Pfeifer; Veronika Sexl; Diogo Fonseca-Pereira; Rita G Domingues; Henrique Veiga-Fernandes; Sebastian J Arnold; Meinrad Busslinger; Ildiko R Dunay; Yakup Tanriver; Andreas Diefenbach
Journal: Cell Date: 2014-04-10 Impact factor: 41.582

4. Tissue-Resident Group 2 Innate Lymphoid Cells Differentiate by Layered Ontogeny and In Situ Perinatal Priming.

Authors: Christoph Schneider; Jinwoo Lee; Satoshi Koga; Roberto R Ricardo-Gonzalez; Jesse C Nussbaum; Lucas K Smith; Saul A Villeda; Hong-Erh Liang; Richard M Locksley
Journal: Immunity Date: 2019-05-22 Impact factor: 31.745

5. c-JUN Dimerization Protein 2 (JDP2) Is a Transcriptional Repressor of Follicle-stimulating Hormone β (FSHβ) and Is Required for Preventing Premature Reproductive Senescence in Female Mice.

Authors: Carrie R Jonak; Nancy M Lainez; Lacey L Roybal; Alexa D Williamson; Djurdjica Coss
Journal: J Biol Chem Date: 2016-12-22 Impact factor: 5.157

6. HTSeq--a Python framework to work with high-throughput sequencing data.

Authors: Simon Anders; Paul Theodor Pyl; Wolfgang Huber
Journal: Bioinformatics Date: 2014-09-25 Impact factor: 6.937

7. Suppression of ILC2 differentiation from committed T cell precursors by E protein transcription factors.

Authors: Liangyue Qian; Sandra Bajana; Constantin Georgescu; Vincent Peng; Hong-Cheng Wang; Indra Adrianto; Marco Colonna; Jose Alberola-Ila; Jonathan D Wren; Xiao-Hong Sun
Journal: J Exp Med Date: 2019-03-21 Impact factor: 14.307

8. The transcription factor TCF-1 enforces commitment to the innate lymphoid cell lineage.

Authors: Christelle Harly; Devin Kenney; Gang Ren; Binbin Lai; Tobias Raabe; Qi Yang; Margaret C Cam; Hai-Hui Xue; Keji Zhao; Avinash Bhandoola
Journal: Nat Immunol Date: 2019-07-29 Impact factor: 25.606

9. Id1 induces apoptosis through inhibition of RORgammat expression.

Authors: Yuanzheng Yang; Hong-Cheng Wang; Xiao-Hong Sun
Journal: BMC Immunol Date: 2008-05-19 Impact factor: 3.615

10. Tissue signals imprint ILC2 identity with anticipatory function.

Authors: Roberto R Ricardo-Gonzalez; Steven J Van Dyken; Christoph Schneider; Jinwoo Lee; Jesse C Nussbaum; Hong-Erh Liang; Dedeepya Vaka; Walter L Eckalbar; Ari B Molofsky; David J Erle; Richard M Locksley
Journal: Nat Immunol Date: 2018-09-10 Impact factor: 25.606

7 in total

1. ILC Differentiation in the Thymus.

Authors: Xiao-Hong Sun; Sandra Bajana
Journal: Adv Exp Med Biol Date: 2022 Impact factor: 2.622

2. E-Protein Inhibition in ILC2 Development Shapes the Function of Mature ILC2s during Allergic Airway Inflammation.

Authors: Gilad Barshad; Lauren M Webb; Hung-An Ting; Oyebola O Oyesola; Oluomachi G Onyekwere; James J Lewis; Edward J Rice; Macy K Matheson; Xiao-Hong Sun; Jakob von Moltke; Charles G Danko; Elia D Tait Wojno
Journal: J Immunol Date: 2022-02-18 Impact factor: 5.426

Review 3. Crosstalk between ILC2s and Th2 CD4⁺ T Cells in Lung Disease.

Authors: Lan-Lan Mi; Wei-Wei Guo
Journal: J Immunol Res Date: 2022-05-10 Impact factor: 4.493

4. MTG16 regulates colonic epithelial differentiation, colitis, and tumorigenesis by repressing E protein transcription factors.

Authors: Rachel E Brown; Justin Jacobse; Shruti A Anant; Koral M Blunt; Bob Chen; Paige N Vega; Chase T Jones; Jennifer M Pilat; Frank Revetta; Aidan H Gorby; Kristy R Stengel; Yash A Choksi; Kimmo Palin; M Blanca Piazuelo; Mary Kay Washington; Ken S Lau; Jeremy A Goettel; Scott W Hiebert; Sarah P Short; Christopher S Williams
Journal: JCI Insight Date: 2022-05-23

E proteins orchestrate dynamic transcriptional cascades implicated in the suppression of the differentiation of group 2 innate lymphoid cells.

Review 1. Helix-loop-helix proteins and lymphocyte development.

Review 2. Wnt signaling in normal and malignant hematopoiesis.

3. Differentiation of type 1 ILCs from a common progenitor to all helper-like innate lymphoid cell lineages.

4. Tissue-Resident Group 2 Innate Lymphoid Cells Differentiate by Layered Ontogeny and In Situ Perinatal Priming.

5. c-JUN Dimerization Protein 2 (JDP2) Is a Transcriptional Repressor of Follicle-stimulating Hormone β (FSHβ) and Is Required for Preventing Premature Reproductive Senescence in Female Mice.

6. HTSeq--a Python framework to work with high-throughput sequencing data.

7. Suppression of ILC2 differentiation from committed T cell precursors by E protein transcription factors.

8. The transcription factor TCF-1 enforces commitment to the innate lymphoid cell lineage.

9. Id1 induces apoptosis through inhibition of RORgammat expression.

10. Tissue signals imprint ILC2 identity with anticipatory function.

1. ILC Differentiation in the Thymus.

2. E-Protein Inhibition in ILC2 Development Shapes the Function of Mature ILC2s during Allergic Airway Inflammation.

Review 3. Crosstalk between ILC2s and Th2 CD4⁺ T Cells in Lung Disease.

4. MTG16 regulates colonic epithelial differentiation, colitis, and tumorigenesis by repressing E protein transcription factors.

5. Augmenting E Protein Activity Impairs cDC2 Differentiation at the Pre-cDC Stage.

Review 6. The divergence between T cell and innate lymphoid cell fates controlled by E and Id proteins.

7. Correlation between circulating innate lymphoid cell precursors and thymic function.

Review 1. Helix-loop-helix proteins and lymphocyte development.

Review 2. Wnt signaling in normal and malignant hematopoiesis.

Review 3. Crosstalk between ILC2s and Th2 CD4+ T Cells in Lung Disease.

Review 6. The divergence between T cell and innate lymphoid cell fates controlled by E and Id proteins.

Review 3. Crosstalk between ILC2s and Th2 CD4⁺ T Cells in Lung Disease.