Drug Transporter

Understanding the implication of transporters in DILI

Discovery
Drug Development
Product Development & CMC
Clinical Services
Central Laboratories

Drug Transporter Services

At Frontage, we have extensive experience in drug transporter research. We offer comprehensive transporter services to support projects from discovery to development including screening, and full characterization of both uptake and efflux transporters.

We Provide Innovative Solutions to Better Understand the Implication of Transporters in Drug-Induced Liver Injury (DILI)

Hepatic transporters help facilitate bile production by exporting bile salts and phosphatidylcholine (PC) from hepatocytes. In humans, inhibition of bile salt export protein (BSEP, ABCB11) and/or multidrug resistance protein 3 (MDR3, ABCB4) transporters can lead to potentially serious DILI.

Drug candidates can be screened for inhibition of BSEP and/or MDR3 to assess DILI risk. BSEPcyte® and MDR3cyte® assays detect the potential of drug candidates to inhibit BSEP and MDR3, respectively. Both approaches utilize a hepatocyte suspension platform, which offers several advantages over other in vitro techniques:

  • Hepatocytes are more physiologically relevant compared to vesicles and transfected cell lines
  • In situ metabolism capability is present in hepatocytes
  • Suspension studies save cell culturing time and allow quicker data generation
  • The assay is accurate, robust, reproducible, and customizable
  • The assay allows for cross-species comparison
  • Specific LC-MS/MS determination of exported bile salts

BSEPcyte®

BSEP is responsible for the biliary secretion of bile salts, which is the primary driving force for enterohepatic recirculation of bile salts and maintaining bile flow. Inhibition of BSEP by a diverse range of drugs or therapeutic agents is associated with DILI. At Frontage, we have developed a novel assay, BSEPcyte®, that accurately measures BSEP inhibition.

BSEPcyte 300x235 - Drug Transporter Services

BSEPcyte® is protected by patent US 9,772,325

MDR3cyte®

MDR3 is primarily expressed in the canalicular membrane of hepatocytes and is responsible for the biliary secretion of PC. PC combined with bile salts forms mixed micelles in bile that solubilize cholesterol and prevent highly concentrated bile salts from damaging biliary canaliculi epithelial cells. Mutations in the human MDR3 gene are associated with progressive familial intrahepatic cholestasis, primary biliary cirrhosis, cholangiocarcinoma, and DILI. The novel MDR3cyte® assay platform at Frontage can provide an accurate assessment of MDR3 inhibition by drug candidates and new chemical entities.

MDR3cyte - Drug Transporter Services

MDR3cyte® is protected by patent US 10,280,401

 

Also check out our Drug Permeability services

Resources to Consider

webinar
BSEPcyte® and MDR3cyte®: Innovative Solutions for Investigating Drug-Induced Liver Injury

BSEPcyte® and MDR3cyte®: Innovative Solutions for Investigating Drug-Induced Liver Injury

Drug-induced liver injury (DILI) accounts for >50% acute liver failures, and is the leading cause of drug development failure, boxed warning and market withdrawal of approved drugs. Inhibition of BSEP and MDR3 is one of the underlying mechanisms for DILI. BSEP and MDR3 are the primary hepatic transporters responsible for exporting bile salts and phosphatidylcholine, respectively. In humans, inhibition of BSEP and/or MDR3 can result in serious liver injury. This presentation will discuss our patented platforms BSEPcyte® and MDR3cyte® using primary hepatocytes in suspension for higher throughput assessment of DILI potentials. In addition, a brief review of the critical transporter studies to inform DDI potentials will also be discussed. This presentation will benefit scientists wanting to learn more about DILI and/or those needing guidance on crucial transporter studies for better assessment of DDI potentials that is aligned with regulatory guidance.

Download Resource