AI-ACCELERATED DRUG DISCOVERY

Charged multivesicular body protein 4b

Explore its Potential with AI-Driven Innovation
Predicted by Alphafold

Charged multivesicular body protein 4b - Focused Library Design

Available from Reaxense

This protein is integrated into the Receptor.AI ecosystem as a prospective target with high therapeutic potential. We performed a comprehensive characterization of Charged multivesicular body protein 4b including:

1. LLM-powered literature research

Our custom-tailored LLM extracted and formalized all relevant information about the protein from a large set of structured and unstructured data sources and stored it in the form of a Knowledge Graph. This comprehensive analysis allowed us to gain insight into Charged multivesicular body protein 4b therapeutic significance, existing small molecule ligands, relevant off-targets, and protein-protein interactions.

 Fig. 1. Preliminary target research workflow

2. AI-Driven Conformational Ensemble Generation

Starting from the initial protein structure, we employed advanced AI algorithms to predict alternative functional states of Charged multivesicular body protein 4b, including large-scale conformational changes along "soft" collective coordinates. Through molecular simulations with AI-enhanced sampling and trajectory clustering, we explored the broad conformational space of the protein and identified its representative structures. Utilizing diffusion-based AI models and active learning AutoML, we generated a statistically robust ensemble of equilibrium protein conformations that capture the receptor's full dynamic behavior, providing a robust foundation for accurate structure-based drug design.

 Fig. 2. AI-powered molecular dynamics simulations workflow

3. Binding pockets identification and characterization

We employed the AI-based pocket prediction module to discover orthosteric, allosteric, hidden, and cryptic binding pockets on the protein’s surface. Our technique integrates the LLM-driven literature search and structure-aware ensemble-based pocket detection algorithm that utilizes previously established protein dynamics. Tentative pockets are then subject to AI scoring and ranking with simultaneous detection of false positives. In the final step, the AI model assesses the druggability of each pocket enabling a comprehensive selection of the most promising pockets for further targeting.

 Fig. 3. AI-based binding pocket detection workflow

4. AI-Powered Virtual Screening

Our ecosystem is equipped to perform AI-driven virtual screening on Charged multivesicular body protein 4b. With access to a vast chemical space and cutting-edge AI docking algorithms, we can rapidly and reliably predict the most promising, novel, diverse, potent, and safe small molecule ligands of Charged multivesicular body protein 4b. This approach allows us to achieve an excellent hit rate and to identify compounds ready for advanced lead discovery and optimization.

 Fig. 4. The screening workflow of Receptor.AI

Receptor.AI, in partnership with Reaxense, developed a next-generation technology for on-demand focused library design to enable extensive target exploration.

The focused library for Charged multivesicular body protein 4b includes a list of the most effective modulators, each annotated with 38 ADME-Tox and 32 physicochemical and drug-likeness parameters. Furthermore, each compound is shown with its optimal docking poses, affinity scores, and activity scores, offering a detailed summary.

Charged multivesicular body protein 4b

partner:

Reaxense

upacc:

Q9H444

UPID:

CHM4B_HUMAN

Alternative names:

Chromatin-modifying protein 4b; SNF7 homolog associated with Alix 1; SNF7-2; Vacuolar protein sorting-associated protein 32-2

Alternative UPACC:

Q9H444; E1P5N4; Q53ZD6

Background:

Charged multivesicular body protein 4b (CHMP4B), also known as Chromatin-modifying protein 4b, plays a pivotal role in the endosomal sorting required for transport complex III (ESCRT-III). This complex is crucial for multivesicular bodies (MVBs) formation, sorting of endosomal cargo proteins into MVBs, and the degradation of membrane proteins. CHMP4B's involvement extends to cytokinesis and nuclear envelope sealing during late anaphase.

Therapeutic significance:

CHMP4B's mutation is linked to Cataract 31, multiple types, highlighting its significance in ocular health. Understanding the role of CHMP4B could open doors to potential therapeutic strategies for cataract treatment and prevention.

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