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Structure and ligand of a histone acetyltransferase bromodomain

Author

Listed:
  • Christophe Dhalluin

    (Structural Biology Program, Mount Sinai School of Medicine)

  • Justin E. Carlson

    (Structural Biology Program, Mount Sinai School of Medicine)

  • Lei Zeng

    (Structural Biology Program, Mount Sinai School of Medicine)

  • Cheng He

    (Structural Biology Program, Mount Sinai School of Medicine)

  • Aneel K. Aggarwal

    (Structural Biology Program, Mount Sinai School of Medicine)

  • Ming-Ming Zhou

    (Structural Biology Program, Mount Sinai School of Medicine)

  • Ming-Ming Zhou

    (Structural Biology Program, Mount Sinai School of Medicine)

Abstract

Histone acetylation is important in chromatin remodelling and gene activation1,2,3,4. Nearly all known histone-acetyltransferase (HAT)-associated transcriptional co-activators contain bromodomains, which are ∼110-amino-acid modules found in many chromatin-associated proteins5,6,7,8,9. Despite the wide occurrence of these bromodomains, their three-dimensional structure and binding partners remain unknown. Here we report the solution structure of the bromodomain of the HAT co-activator P/CAF (p300/CBP-associated factor)10,11. The structure reveals an unusual left-handed up-and-down four-helix bundle. In addition, we showby a combination of structural and site-directed mutagenesis studies that bromodomains can interact specifically with acetylated lysine, making them the first known protein modules to do so. The nature of the recognition of acetyl-lysine by the P/CAF bromodomain is similar to that of acetyl-CoA by histone acetyltransferase. Thus, the bromodomain is functionally linked to the HAT activity of co-activators in the regulation of gene transcription.

Suggested Citation

  • Christophe Dhalluin & Justin E. Carlson & Lei Zeng & Cheng He & Aneel K. Aggarwal & Ming-Ming Zhou & Ming-Ming Zhou, 1999. "Structure and ligand of a histone acetyltransferase bromodomain," Nature, Nature, vol. 399(6735), pages 491-496, June.
  • Handle: RePEc:nat:nature:v:399:y:1999:i:6735:d:10.1038_20974
    DOI: 10.1038/20974
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    Cited by:

    1. Ziad Ibrahim & Tao Wang & Olivier Destaing & Nicola Salvi & Naghmeh Hoghoughi & Clovis Chabert & Alexandra Rusu & Jinjun Gao & Leonardo Feletto & Nicolas Reynoird & Thomas Schalch & Yingming Zhao & Ma, 2022. "Structural insights into p300 regulation and acetylation-dependent genome organisation," Nature Communications, Nature, vol. 13(1), pages 1-23, December.
    2. Michael F. Emmons & Richard L. Bennett & Alberto Riva & Kanchan Gupta & Larissa Anastasio Da Costa Carvalho & Chao Zhang & Robert Macaulay & Daphne Dupéré-Richér & Bin Fang & Edward Seto & John M. Koo, 2023. "HDAC8-mediated inhibition of EP300 drives a transcriptional state that increases melanoma brain metastasis," Nature Communications, Nature, vol. 14(1), pages 1-18, December.
    3. Ying Liang & Haiyue Xu & Tao Cheng & Yujuan Fu & Hanwei Huang & Wenchang Qian & Junyan Wang & Yuenan Zhou & Pengxu Qian & Yafei Yin & Pengfei Xu & Wei Zou & Baohui Chen, 2022. "Gene activation guided by nascent RNA-bound transcription factors," Nature Communications, Nature, vol. 13(1), pages 1-16, December.
    4. Bhardwaj, Vijay Kumar & Das, Pralay & Purohit, Rituraj, 2023. "Integrating microsecond timescale classical and biased molecular dynamics simulations to screen potential molecules for BRD4-BD1," Chaos, Solitons & Fractals, Elsevier, vol. 167(C).
    5. Masaki Kikuchi & Satoshi Morita & Masatoshi Wakamori & Shin Sato & Tomomi Uchikubo-Kamo & Takehiro Suzuki & Naoshi Dohmae & Mikako Shirouzu & Takashi Umehara, 2023. "Epigenetic mechanisms to propagate histone acetylation by p300/CBP," Nature Communications, Nature, vol. 14(1), pages 1-16, December.

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