Bcl11b prevents catastrophic autoimmunity by controlling multiple aspects of a regulatory T cell gene expression program

Syed Nurul Hasan; Amit Sharma; Sayantani Ghosh; Sung Wook Hong; Sinchita Roy-Chowdhuri; Sin Hyeog Im; Keunsoo Kang; Dipayan Rudra

doi:10.1126/sciadv.aaw0706

Bcl11b prevents catastrophic autoimmunity by controlling multiple aspects of a regulatory T cell gene expression program

Syed Nurul Hasan, Amit Sharma, Sayantani Ghosh, Sung Wook Hong, Sinchita Roy-Chowdhuri, Sin Hyeog Im, Keunsoo Kang, Dipayan Rudra

Pathology

Research output: Contribution to journal › Article › peer-review

14 Scopus citations

Abstract

Foxp3 and its protein partners establish a regulatory T (T_reg) cell transcription profile and promote immunological tolerance. However, molecular features contributing to a T_reg-specific gene expression program are still incompletely understood. We find that the transcription factor Bcl11b is a prominent Foxp3 cofactor with multifaceted functions in T_reg biology. Optimal genomic recruitment of Foxp3 and Bcl11b is critically interdependent. Genome-wide occupancy studies coupled with gene expression profiling reveal that Bcl11b, in association with Foxp3, is primarily responsible in establishing a T_reg-specific gene activation program. Furthermore, Bcl11b restricts misdirected recruitment of Foxp3 to sites, which would otherwise result in an altered T_reg transcriptome profile. Consequently, T_reg-specific ablation of Bcl11b results in marked breakdown of immune tolerance, leading to aggressive systemic autoimmunity. Our study provides previously underappreciated mechanistic insights into molecular events contributing to basic aspects of T_reg function. Furthermore, it establishes a therapeutic target with potential implications in autoimmunity and cancer.

Original language	English (US)
Article number	eaaw0706
Journal	Science Advances
Volume	5
Issue number	8
DOIs	https://doi.org/10.1126/sciadv.aaw0706
State	Published - Aug 7 2019

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title = "Bcl11b prevents catastrophic autoimmunity by controlling multiple aspects of a regulatory T cell gene expression program",

abstract = "Foxp3 and its protein partners establish a regulatory T (Treg) cell transcription profile and promote immunological tolerance. However, molecular features contributing to a Treg-specific gene expression program are still incompletely understood. We find that the transcription factor Bcl11b is a prominent Foxp3 cofactor with multifaceted functions in Treg biology. Optimal genomic recruitment of Foxp3 and Bcl11b is critically interdependent. Genome-wide occupancy studies coupled with gene expression profiling reveal that Bcl11b, in association with Foxp3, is primarily responsible in establishing a Treg-specific gene activation program. Furthermore, Bcl11b restricts misdirected recruitment of Foxp3 to sites, which would otherwise result in an altered Treg transcriptome profile. Consequently, Treg-specific ablation of Bcl11b results in marked breakdown of immune tolerance, leading to aggressive systemic autoimmunity. Our study provides previously underappreciated mechanistic insights into molecular events contributing to basic aspects of Treg function. Furthermore, it establishes a therapeutic target with potential implications in autoimmunity and cancer.",

author = "Hasan, {Syed Nurul} and Amit Sharma and Sayantani Ghosh and Hong, {Sung Wook} and Sinchita Roy-Chowdhuri and Im, {Sin Hyeog} and Keunsoo Kang and Dipayan Rudra",

note = "Funding Information: We thank N. Mullapudi, Scientific Officer, Hong Kong University of Science and Technology, for technical suggestions in ChIP-seq. We also thank H. Jung for technical assistance in cell sorting. Funding: This work was supported by Project IBS-R005 from the Institute for Basic Science, Korean Ministry of Science and ICT. Publisher Copyright: Copyright {\textcopyright} 2019 The Authors, some rights reserved;",

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AU - Hasan, Syed Nurul

AU - Sharma, Amit

AU - Ghosh, Sayantani

AU - Hong, Sung Wook

AU - Roy-Chowdhuri, Sinchita

AU - Im, Sin Hyeog

AU - Kang, Keunsoo

AU - Rudra, Dipayan

N1 - Funding Information: We thank N. Mullapudi, Scientific Officer, Hong Kong University of Science and Technology, for technical suggestions in ChIP-seq. We also thank H. Jung for technical assistance in cell sorting. Funding: This work was supported by Project IBS-R005 from the Institute for Basic Science, Korean Ministry of Science and ICT. Publisher Copyright: Copyright © 2019 The Authors, some rights reserved;

PY - 2019/8/7

Y1 - 2019/8/7

N2 - Foxp3 and its protein partners establish a regulatory T (Treg) cell transcription profile and promote immunological tolerance. However, molecular features contributing to a Treg-specific gene expression program are still incompletely understood. We find that the transcription factor Bcl11b is a prominent Foxp3 cofactor with multifaceted functions in Treg biology. Optimal genomic recruitment of Foxp3 and Bcl11b is critically interdependent. Genome-wide occupancy studies coupled with gene expression profiling reveal that Bcl11b, in association with Foxp3, is primarily responsible in establishing a Treg-specific gene activation program. Furthermore, Bcl11b restricts misdirected recruitment of Foxp3 to sites, which would otherwise result in an altered Treg transcriptome profile. Consequently, Treg-specific ablation of Bcl11b results in marked breakdown of immune tolerance, leading to aggressive systemic autoimmunity. Our study provides previously underappreciated mechanistic insights into molecular events contributing to basic aspects of Treg function. Furthermore, it establishes a therapeutic target with potential implications in autoimmunity and cancer.

AB - Foxp3 and its protein partners establish a regulatory T (Treg) cell transcription profile and promote immunological tolerance. However, molecular features contributing to a Treg-specific gene expression program are still incompletely understood. We find that the transcription factor Bcl11b is a prominent Foxp3 cofactor with multifaceted functions in Treg biology. Optimal genomic recruitment of Foxp3 and Bcl11b is critically interdependent. Genome-wide occupancy studies coupled with gene expression profiling reveal that Bcl11b, in association with Foxp3, is primarily responsible in establishing a Treg-specific gene activation program. Furthermore, Bcl11b restricts misdirected recruitment of Foxp3 to sites, which would otherwise result in an altered Treg transcriptome profile. Consequently, Treg-specific ablation of Bcl11b results in marked breakdown of immune tolerance, leading to aggressive systemic autoimmunity. Our study provides previously underappreciated mechanistic insights into molecular events contributing to basic aspects of Treg function. Furthermore, it establishes a therapeutic target with potential implications in autoimmunity and cancer.

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Bcl11b prevents catastrophic autoimmunity by controlling multiple aspects of a regulatory T cell gene expression program

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