Rationale for Therapeutic Drug Monitoring of Biopharmaceuticals in Inflammatory Diseases.

Ther Drug Monit

*Université François-Rabelais de Tours, CNRS UMR 7292, Tours, France; †Unit of Pharmacology-Toxicology, University Hospital, Tours, France; ‡Neurologia 2, Centro Riferimento Regionale Sclerosi Multipla (CReSM), Orbassano, Turin, Italy; §Neuroscience Institute Cavalieri Ottolenghi (NICO), San Luigi Hospital, Orbassano, Turin, Italy; ¶Department of Clinical Pharmacology, Tours University Hospital, Tours, France; ∥Unit of Immunology, La Paz University Hospital, Madrid, Spain; and ††Department of Rheumatology, Tours University Hospital, Tours, France.

Published: August 2017

Biopharmaceuticals bring together a number of specific characteristics as compared with other drugs. However, as it is done for most drugs, an individual adjustment of their dose may be necessary. Similar to "chemical" drugs, biopharmaceuticals used in immunoinflammatory diseases have a rather narrow therapeutic range, lack good early clinical or biological marker of response, have variable pharmacokinetics, and their serum concentrations are most often related with response. Monoclonal antibodies have additional specific sources of pharmacokinetic variability. Low concentrations may increase the risks of immunization, plasmapheresis may increase their elimination, and subcutaneous formulations may be associated with decreased adherence. For all these reasons, pharmacokinetic therapeutic drug monitoring may be useful. However, few randomized controlled therapeutic drug monitoring studies have been published. For monoclonal antibodies, a precise definition of the therapeutic concentrations is challenging because of the interindividual variability in their concentration-effect relationship.

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Source
http://dx.doi.org/10.1097/FTD.0000000000000410DOI Listing

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