Central control of dynamic gene circuits governs T cell rest and activation

Maya M. Arce; Jennifer M. Umhoefer; Nadia Arang; Sivakanthan Kasinathan; Jacob W. Freimer; Zachary Steinhart; Haolin Shen; Minh T.N. Pham; Mineto Ota; Anika Wadhera; Rama Dajani; Dmytro Dorovskyi; Yan Yi Chen; Qi Liu; Yuan Zhou; Danielle L. Swaney; Kirsten Obernier; Brian R. Shy; Julia Carnevale; Ansuman T. Satpathy; Nevan J. Krogan; Jonathan K. Pritchard; Alexander Marson

doi:10.1038/s41586-024-08314-y

Central control of dynamic gene circuits governs T cell rest and activation

Maya M. Arce, Jennifer M. Umhoefer, Nadia Arang, Sivakanthan Kasinathan, Jacob W. Freimer, Zachary Steinhart, Haolin Shen, Minh T.N. Pham, Mineto Ota, Anika Wadhera, Rama Dajani, Dmytro Dorovskyi, Yan Yi Chen, Qi Liu, Yuan Zhou, Danielle L. Swaney, Kirsten Obernier, Brian R. Shy, Julia Carnevale, Ansuman T. SatpathyNevan J. Krogan, Jonathan K. Pritchard, Alexander Marson

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

8 Scopus citations

Abstract

The ability of cells to maintain distinct identities and respond to transient environmental signals requires tightly controlled regulation of gene networks^{1, 2–3}. These dynamic regulatory circuits that respond to extracellular cues in primary human cells remain poorly defined. The need for context-dependent regulation is prominent in T cells, where distinct lineages must respond to diverse signals to mount effective immune responses and maintain homeostasis^{4, 5, 6, 7–8}. Here we performed CRISPR screens in multiple primary human CD4⁺ T cell contexts to identify regulators that control expression of IL-2Rα, a canonical marker of T cell activation transiently expressed by pro-inflammatory effector T cells and constitutively expressed by anti-inflammatory regulatory T cells where it is required for fitness^{9, 10–11}. Approximately 90% of identified regulators of IL-2Rα had effects that varied across cell types and/or stimulation states, including a subset that even had opposite effects across conditions. Using single-cell transcriptomics after pooled perturbation of context-specific screen hits, we characterized specific factors as regulators of overall rest or activation and constructed state-specific regulatory networks. MED12 — a component of the Mediator complex — serves as a dynamic orchestrator of key regulators, controlling expression of distinct sets of regulators in different T cell contexts. Immunoprecipitation–mass spectrometry revealed that MED12 interacts with the histone methylating COMPASS complex. MED12 was required for histone methylation and expression of genes encoding key context-specific regulators, including the rest maintenance factor KLF2 and the versatile regulator MYC. CRISPR ablation of MED12 blunted the cell-state transitions between rest and activation and protected from activation-induced cell death. Overall, this work leverages CRISPR screens performed across conditions to define dynamic gene circuits required to establish resting and activated T cell states.

Original language	English
Article number	554
Pages (from-to)	930-939
Number of pages	10
Journal	Nature
Volume	637
Issue number	8047
DOIs	https://doi.org/10.1038/s41586-024-08314-y
State	Published - 23 Jan 2025
Externally published	Yes

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Arce, M. M., Umhoefer, J. M., Arang, N., Kasinathan, S., Freimer, J. W., Steinhart, Z., Shen, H., Pham, M. T. N., Ota, M., Wadhera, A., Dajani, R., Dorovskyi, D., Chen, Y. Y., Liu, Q., Zhou, Y., Swaney, D. L., Obernier, K., Shy, B. R., Carnevale, J., ... Marson, A. (2025). Central control of dynamic gene circuits governs T cell rest and activation. Nature, 637(8047), 930-939. Article 554. https://doi.org/10.1038/s41586-024-08314-y

@article{af48f006ffdc4f4093da8e3b567a0631,

title = "Central control of dynamic gene circuits governs T cell rest and activation",

abstract = "The ability of cells to maintain distinct identities and respond to transient environmental signals requires tightly controlled regulation of gene networks1, 2–3. These dynamic regulatory circuits that respond to extracellular cues in primary human cells remain poorly defined. The need for context-dependent regulation is prominent in T cells, where distinct lineages must respond to diverse signals to mount effective immune responses and maintain homeostasis4, 5, 6, 7–8. Here we performed CRISPR screens in multiple primary human CD4+ T cell contexts to identify regulators that control expression of IL-2Rα, a canonical marker of T cell activation transiently expressed by pro-inflammatory effector T cells and constitutively expressed by anti-inflammatory regulatory T cells where it is required for fitness9, 10–11. Approximately 90\% of identified regulators of IL-2Rα had effects that varied across cell types and/or stimulation states, including a subset that even had opposite effects across conditions. Using single-cell transcriptomics after pooled perturbation of context-specific screen hits, we characterized specific factors as regulators of overall rest or activation and constructed state-specific regulatory networks. MED12 — a component of the Mediator complex — serves as a dynamic orchestrator of key regulators, controlling expression of distinct sets of regulators in different T cell contexts. Immunoprecipitation–mass spectrometry revealed that MED12 interacts with the histone methylating COMPASS complex. MED12 was required for histone methylation and expression of genes encoding key context-specific regulators, including the rest maintenance factor KLF2 and the versatile regulator MYC. CRISPR ablation of MED12 blunted the cell-state transitions between rest and activation and protected from activation-induced cell death. Overall, this work leverages CRISPR screens performed across conditions to define dynamic gene circuits required to establish resting and activated T cell states.",

author = "Arce, \{Maya M.\} and Umhoefer, \{Jennifer M.\} and Nadia Arang and Sivakanthan Kasinathan and Freimer, \{Jacob W.\} and Zachary Steinhart and Haolin Shen and Pham, \{Minh T.N.\} and Mineto Ota and Anika Wadhera and Rama Dajani and Dmytro Dorovskyi and Chen, \{Yan Yi\} and Qi Liu and Yuan Zhou and Swaney, \{Danielle L.\} and Kirsten Obernier and Shy, \{Brian R.\} and Julia Carnevale and Satpathy, \{Ansuman T.\} and Krogan, \{Nevan J.\} and Pritchard, \{Jonathan K.\} and Alexander Marson",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2025",

month = jan,

day = "23",

doi = "10.1038/s41586-024-08314-y",

language = "English",

volume = "637",

pages = "930--939",

journal = "Nature",

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Arce, MM, Umhoefer, JM, Arang, N, Kasinathan, S, Freimer, JW, Steinhart, Z, Shen, H, Pham, MTN, Ota, M, Wadhera, A, Dajani, R, Dorovskyi, D, Chen, YY, Liu, Q, Zhou, Y, Swaney, DL, Obernier, K, Shy, BR, Carnevale, J, Satpathy, AT, Krogan, NJ, Pritchard, JK & Marson, A 2025, 'Central control of dynamic gene circuits governs T cell rest and activation', Nature, vol. 637, no. 8047, 554, pp. 930-939. https://doi.org/10.1038/s41586-024-08314-y

TY - JOUR

T1 - Central control of dynamic gene circuits governs T cell rest and activation

AU - Arce, Maya M.

AU - Umhoefer, Jennifer M.

AU - Arang, Nadia

AU - Kasinathan, Sivakanthan

AU - Freimer, Jacob W.

AU - Steinhart, Zachary

AU - Shen, Haolin

AU - Pham, Minh T.N.

AU - Ota, Mineto

AU - Wadhera, Anika

AU - Dajani, Rama

AU - Dorovskyi, Dmytro

AU - Chen, Yan Yi

AU - Liu, Qi

AU - Zhou, Yuan

AU - Swaney, Danielle L.

AU - Obernier, Kirsten

AU - Shy, Brian R.

AU - Carnevale, Julia

AU - Satpathy, Ansuman T.

AU - Krogan, Nevan J.

AU - Pritchard, Jonathan K.

AU - Marson, Alexander

PY - 2025/1/23

Y1 - 2025/1/23

N2 - The ability of cells to maintain distinct identities and respond to transient environmental signals requires tightly controlled regulation of gene networks1, 2–3. These dynamic regulatory circuits that respond to extracellular cues in primary human cells remain poorly defined. The need for context-dependent regulation is prominent in T cells, where distinct lineages must respond to diverse signals to mount effective immune responses and maintain homeostasis4, 5, 6, 7–8. Here we performed CRISPR screens in multiple primary human CD4+ T cell contexts to identify regulators that control expression of IL-2Rα, a canonical marker of T cell activation transiently expressed by pro-inflammatory effector T cells and constitutively expressed by anti-inflammatory regulatory T cells where it is required for fitness9, 10–11. Approximately 90% of identified regulators of IL-2Rα had effects that varied across cell types and/or stimulation states, including a subset that even had opposite effects across conditions. Using single-cell transcriptomics after pooled perturbation of context-specific screen hits, we characterized specific factors as regulators of overall rest or activation and constructed state-specific regulatory networks. MED12 — a component of the Mediator complex — serves as a dynamic orchestrator of key regulators, controlling expression of distinct sets of regulators in different T cell contexts. Immunoprecipitation–mass spectrometry revealed that MED12 interacts with the histone methylating COMPASS complex. MED12 was required for histone methylation and expression of genes encoding key context-specific regulators, including the rest maintenance factor KLF2 and the versatile regulator MYC. CRISPR ablation of MED12 blunted the cell-state transitions between rest and activation and protected from activation-induced cell death. Overall, this work leverages CRISPR screens performed across conditions to define dynamic gene circuits required to establish resting and activated T cell states.

AB - The ability of cells to maintain distinct identities and respond to transient environmental signals requires tightly controlled regulation of gene networks1, 2–3. These dynamic regulatory circuits that respond to extracellular cues in primary human cells remain poorly defined. The need for context-dependent regulation is prominent in T cells, where distinct lineages must respond to diverse signals to mount effective immune responses and maintain homeostasis4, 5, 6, 7–8. Here we performed CRISPR screens in multiple primary human CD4+ T cell contexts to identify regulators that control expression of IL-2Rα, a canonical marker of T cell activation transiently expressed by pro-inflammatory effector T cells and constitutively expressed by anti-inflammatory regulatory T cells where it is required for fitness9, 10–11. Approximately 90% of identified regulators of IL-2Rα had effects that varied across cell types and/or stimulation states, including a subset that even had opposite effects across conditions. Using single-cell transcriptomics after pooled perturbation of context-specific screen hits, we characterized specific factors as regulators of overall rest or activation and constructed state-specific regulatory networks. MED12 — a component of the Mediator complex — serves as a dynamic orchestrator of key regulators, controlling expression of distinct sets of regulators in different T cell contexts. Immunoprecipitation–mass spectrometry revealed that MED12 interacts with the histone methylating COMPASS complex. MED12 was required for histone methylation and expression of genes encoding key context-specific regulators, including the rest maintenance factor KLF2 and the versatile regulator MYC. CRISPR ablation of MED12 blunted the cell-state transitions between rest and activation and protected from activation-induced cell death. Overall, this work leverages CRISPR screens performed across conditions to define dynamic gene circuits required to establish resting and activated T cell states.

UR - https://www.scopus.com/pages/publications/85211790127

U2 - 10.1038/s41586-024-08314-y

DO - 10.1038/s41586-024-08314-y

M3 - Article

AN - SCOPUS:85211790127

SN - 0028-0836

VL - 637

SP - 930

EP - 939

JO - Nature

JF - Nature

IS - 8047

M1 - 554

ER -

Central control of dynamic gene circuits governs T cell rest and activation

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