4.1 Article

Impact of Transporter Polymorphisms on Drug Development: Is It Clinically Significant?

期刊

JOURNAL OF CLINICAL PHARMACOLOGY
卷 56, 期 -, 页码 S40-S58

出版社

WILEY
DOI: 10.1002/jcph.691

关键词

drug transporters; pharmacogenomics; drug development

资金

  1. Wolfe Medical Research Chair in Pharmacogenomics
  2. Canadian Institutes of Health Research [MOP-89753]
  3. Drug Safety and Effectiveness Network (DSEN-PREVENT) [FRN-117588]
  4. Academic Medical Organization of Southwestern Ontario Alternate Funding Plan Innovation Fund
  5. Cancer Care Ontario (CCO) Research Chair Award (Tier-1) in Experimental Therapeutics
  6. Ontario Institute for Cancer Research (OICR) Translational Research Team grant
  7. Canadian Institutes of Health Research
  8. Clinician-Investigator Program at Schulich School of Medicine & Dentistry at Western
  9. Canadian Institutes of Health Research/Crohn's Colitis Canada/Canadian Association of Gastroenterology Joint Research Fellowship (inflammatory bowel disease priority area) [201411IBD]
  10. joint inflammatory bowel disease/clinical pharmacology research grant from Janssen Incorporated

向作者/读者索取更多资源

Drug transporters are becoming increasingly recognized as relevant to the drug development process. This may be a reflection of increasing target complexity and the need for high-affinity interaction with drug targets that minimize off-target side effects. Moreover, as new molecular entities (NMEs) become larger in size and amphipathic in nature, interaction with drug transporters, both uptake as well as efflux, becomes increasingly likely. In some cases transporters may limit the absorption or organ-specific entry of NMEs, whereas in other cases transporters may enhance their absorption or tissue accumulation. Indeed, in some cases, transporters may prove to be a therapeutic target. Accordingly, a better understanding of potentially clinically relevant drug transporter polymorphisms earlier in the drug development process is highly desirable. In this review we examine key transporters that are important to the absorption, distribution, and excretion of a large number of drugs in clinical use. Importantly, we provide our assessment of the potential impact of known polymorphisms in such transporters and discuss whether there is sufficient evidence to incorporate these polymorphisms in the drug development process.

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