Focused On-demand Library for Crossover junction endonuclease EME1

Details

Focused On-demand Libraries - Receptor.AI Collaboration


Explore the Potential with AI-Driven Innovation

This comprehensive focused library is produced on demand with state-of-the-art virtual screening and parameter assessment technology driven by Receptor.AI drug discovery platform. This approach outperforms traditional methods and provides higher-quality compounds with superior activity, selectivity and safety.


We pick out particular compounds from an extensive virtual database of more than 60 billion molecules. The preparation and shipment of these compounds are facilitated by Reaxense.


In the library, a selection of top modulators is provided, each marked with 38 ADME-Tox and 32 parameters related to physicochemical properties and drug-likeness. Also, every compound comes with its best docking poses, affinity scores, and activity scores, providing a comprehensive overview.


We utilise our cutting-edge, exclusive workflow to develop focused libraries for enzymes.


 

Fig. 1. The screening workflow of Receptor.AI

The procedure entails thorough molecular simulations of the catalytic and allosteric binding pockets, accompanied by ensemble virtual screening that factors in their conformational flexibility. When developing modulators, the structural modifications brought about by reaction intermediates are factored in to optimize activity and selectivity.


Our library stands out due to several important features:


  • The Receptor.AI platform compiles comprehensive data on the target protein, encompassing previous experiments, literature, known ligands, structural details, and more, leading to a higher chance of selecting the most relevant compounds.

  • Advanced molecular simulations on the platform help pinpoint potential binding sites, making the compounds in our focused library ideal for finding allosteric inhibitors and targeting cryptic pockets.

  • Receptor.AI boasts over 50 tailor-made AI models, rigorously tested and proven in various drug discovery projects and research initiatives. They are crafted for efficacy, dependability, and precision, all of which are key in creating our focused libraries.

  • Beyond creating focused libraries, Receptor.AI offers comprehensive services and complete solutions throughout the preclinical drug discovery phase. Our success-based pricing model minimises risk and maximises the mutual benefits of the project's success.

PARTNER
Receptor.AI
 
UPACC
Q96AY2

UPID:
EME1_HUMAN

ALTERNATIVE NAMES:
MMS4 homolog

ALTERNATIVE UPACC:
Q96AY2; Q96N62

BACKGROUND:
The protein Crossover junction endonuclease EME1, alternatively named MMS4 homolog, is integral to DNA repair. By partnering with MUS81, it forms an endonuclease that targets branched DNA structures, including 3'-flap structures, replication forks, and nicked Holliday junctions. This specificity is vital for the resolution of DNA replication issues and the maintenance of genomic integrity during cell division.

THERAPEUTIC SIGNIFICANCE:
Understanding the role of Crossover junction endonuclease EME1 could open doors to potential therapeutic strategies. Given its essential role in the DNA damage repair pathway, targeting EME1 could lead to innovative treatments for conditions marked by DNA repair defects.

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