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DILIsymSoftware for Predicting Drug-Induced Liver Injury

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DILIsym is a sophisticated quantitative systems toxicology (QST) software designed to predict and elucidate drug-induced liver injury (DILI). This tool utilizes a middle-out, multi-scale modeling approach to simulate the complex biochemical and physiological interactions leading to liver toxicity. DILIsym integrates compound exposure with mechanisms of drug toxicity and inter-individual variability, offering insights into hepatotoxicity prediction for multiple species, including mice, rats, dogs, and humans. Its comprehensive sub-models cover key liver cell populations, intracellular biochemical processes, and immune response simulations. DILIsym supports drug development by enabling the assessment of potential DILI risks and mechanistic analysis of observed liver injury signals. It features a graphical user interface for simulating experimental parameters and provides a command-line option for streamlined workflow integration. The software can be extended with a high-performance grid license for large-scale simulations, making it a valuable tool for pharmaceutical companies and researchers involved in hepatic safety evaluations.
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DILIsym is Quantitative Systems Toxicology (QST) software capable of predicting and explaining Drug-Induced Liver Injury (DILI).

DILIsym is a “middle-out”, multi‑scale representation of drug-induced liver injury. Includes multiple sub-models which are solved in an integrated fashion to generate simulation results.

 

DILIsym is Quantitative Systems Toxicology (QST) software designed to be used during drug development to provide an indication of the potential drug-induced liver injury (DILI) hazard posed by individual molecules and/or to provide deeper insight into the mechanisms responsible for observed DILI responses at various stages of the development process.

DILIsym is Quantitative Systems Toxicology (QST) software designed to be used during drug development to provide an indication of the potential drug-induced liver injury (DILI) hazard posed by individual molecules and/or to provide deeper insight into the mechanisms responsible for observed DILI responses at various stages of the development process.