Royal College of Surgeons in Ireland
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Advances in the design and development of PROTAC-mediated HDAC degradation.

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journal contribution
posted on 2024-01-22, 14:09 authored by Daniel Alencar RodriguesDaniel Alencar Rodrigues, Andrew RoeAndrew Roe, Darren GriffithDarren Griffith, Triona Ni ChonghaileTriona Ni Chonghaile
Due to developments in modern chemistry, previously undruggable targets are becoming druggable thanks to selective degradation using the ubiquitin-proteasomal degradation system. PROteolysis TArgeting Chimeras (PROTACs) are heterobifunctional molecules designed specifically to degrade target proteins (protein of interest, POI). They are of significant interest to industry and academia as they are highly specific and can target previously undruggable target proteins from transcription factors to enzymes. More than 15 degraders are expected to be evaluated in clinical trials by the end of 2021. Herein, we describe recent advances in the design and development of PROTAC-mediated degradation of histone deacetylases (HDACs). PROTAC-mediated degradation of HDACs can offer some significant advantages over direct inhibition, such as the use of substoichiometric doses and the potential to disrupt enzyme-independent HDAC function. Herein, we discuss the potential implications of the degradation of HDACs with HDAC knockout studies and the selection of HDAC inhibitors and E3 ligase ligands for the design of the PROTACs. The potential utility of HDAC PROTACs in various disease pathologies from cancer to inflammation to neurodegeneration is driving the interest in this field.

Funding

Science Foundation Ireland Frontiers for the Future (19/FFP/6461)

History

Comments

The published manuscript is available at EurekaSelect via https://www.eurekaselect.com/openurl/content.php?genre=article&doi=10.2174/1568026621666211015092047

Published Citation

Rodrigues DA, Roe A, Griffith D, Chonghaile TN. Advances in the design and development of PROTAC-mediated HDAC degradation. Curr Top Med Chem. 2022;22(5):408-424.

Publication Date

29 November 2021

PubMed ID

34649488

Department/Unit

  • Chemistry
  • Physiology and Medical Physics

Research Area

  • Cancer
  • Chemistry and Pharmaceutical Sciences

Publisher

Bentham Science Publishers Ltd.

Version

  • Accepted Version (Postprint)