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Pharmacogenomics of Pain Management: The Impact of Specific Biological Polymorphisms on Drugs and Metabolism

Authors :
Alan D. Kaye
Narjeet Khurmi
Elyse M. Cornett
G Jason Huang
Michelle A. Carroll Turpin
Allison M. Pinner
Tamizh Selvan Gnana Sekaran
Harish Siddaiah
Richard D. Urman
Pankaj Thakur
Jasmine Rivas
Cain W. Stark
Anitha Senthil
Anna Yates
Jenna L Miller
Source :
Current Oncology Reports. 22
Publication Year :
2020
Publisher :
Springer Science and Business Media LLC, 2020.

Abstract

Pain is multifactorial and complex, often with a genetic component. Pharmacogenomics is a relative new field, which allows for the development of a truly unique and personalized therapeutic approach in the treatment of pain. Until recently, drug mechanisms in humans were determined by testing that drug in a population and calculating response averages. However, some patients will inevitably fall outside of those averages, and it is nearly impossible to predict who those outliers might be. Pharmacogenetics considers a patient’s unique genetic information and allows for anticipation of that individual’s response to medication. Pharmacogenomic testing is steadily making progress in the management of pain by being able to identify individual differences in the perception of pain and susceptibility and sensitivity to drugs based on genetic markers. This has a huge potential to increase efficacy and reduce the incidence of iatrogenic drug dependence and addiction. The streamlining of relevant polymorphisms of genes encoding receptors, transporters, and drug-metabolizing enzymes influencing the pain phenotype can be an important guide to develop safe new strategies and approaches to personalized pain management. Additionally, some challenges still prevail and preclude adoption of pharmacogenomic testing universally. These include lack of knowledge about pharmacogenomic testing, inadequate standardization of the process of data handling, questionable benefits about the clinical and financial aspects of pharmacogenomic testing-guided therapy, discrepancies in clinical evidence supporting these tests, and doubtful reimbursement of the tests by health insurance agencies.

Details

ISSN :
15346269 and 15233790
Volume :
22
Database :
OpenAIRE
Journal :
Current Oncology Reports
Accession number :
edsair.doi.dedup.....4443f1343ba11c057860e19ed6ab33a9
Full Text :
https://doi.org/10.1007/s11912-020-0865-4