Drug-Induced Liver Injury (DILI) Compound Library | MedChemExpress (MCE)

Drug-Induced Liver Injury (DILI) Compound Library | MedChemExpress (MCE)

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Drug-Induced Liver Injury (DILI) Compound Library

MCE 国际站:Drug-Induced Liver Injury (DILI) Compound Library

Drug-induced liver injury (DILI; also known as drug-induced hepatotoxicity) is caused by medications (prescription or OTC), herbal and dietary supplements (HDS), or other xenobiotics that result in abnormalities in liver tests or in hepatic dysfunction that cannot be explained by other causes. Drugs are an important cause of liver injury. Drug-induced hepatic injury is the most common reason cited for withdrawal of an approved drug.DILI is thought to occur via several different mechanisms. Among these are direct impairment of the structural (e.g., mitochondrial dysfunction) and functional integrity of the liver; production of a metabolite that alters hepatocellular structure and function; production of a reactive drug metabolite that binds to hepatic proteins to produce new antigenic drug-protein adducts, which are targeted by hosts’ defenses (the hapten hypothesis); and initiation of a systemic hypersensitivity response (i.e., drug allergy) that damages the liver.MCE Drug-induced Liver Injury (DILI) Compound Library contains a unique collection of 1346 hepatotoxicity causing compounds and is a powerful tool to research DILI and other drug toxicities. This library can be used to understand the mechanisms of DILI, identify biomarkers for early DILI prediction, and allow timely recognition during drug development, thus finally achieving successful DILI prevention and assessment in the pre-marketing phase.

Description & Advantages:

•   A unique collection of 1346 hepatotoxicity causing compounds for high throughput screening (HTS) and high content screening (HCS).

•   Including antibiotics, anti-cancer drugs, cardiac medications and anti-inflammatory agent, etc.

•   A useful tool for researching drug toxicity and mechanisms of DILI.

•   Including several different toxicities: steatosis, mitochondrial toxicity, cholestasis, drug allergy (hypersensitivity), etc.;

•   Structurally diverse, bioactive, and cell permeable.

•   More detailed compound information with structure, IC50, and brief introduction.

•   NMR and HPLC validated ensure high purity.

•   All compounds are in stock and continuously updated.

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