2005
DOI: 10.1007/s11095-005-2495-9
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Method Validation and Measurement of Biomarkers in Nonclinical and Clinical Samples in Drug Development: A Conference Report

Abstract: Biomarkers are increasingly used in drug development to aid scientific and clinical decisions regarding the progress of candidate and marketed therapeutics. Biomarkers can improve the understanding of diseases as well as therapeutic and off-target effects of drugs. Early implementation of biomarker strategies thus promises to reduce costs and time-to-market as drugs proceed through increasingly costly and complex clinical development programs. The 2003 American Association of Pharmaceutical Sciences/Clinical L… Show more

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Cited by 179 publications
(165 citation statements)
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“…A biomarker is defined as a characteristic that can be objectively measured and evaluated as an indicator of normal biological processes, pathogenic processes or pharmacological responses to a therapeutic intervention 1, 2. Clinical biomarkers are thought to reflect disease activity and pathophysiology 3, 4. A useful biomarker in any class has to comply with the following general criteria: (i) there must be a consistent response of the biomarker across studies (preferably from different research groups) and drugs from the same mechanistic class; (ii) the biomarker must respond clearly to therapeutic (not supratherapeutic) doses; (iii) there must be a clear dose‐ or concentration‐response relationship; and (iv) there must a plausible relationship between the biomarker, pharmacology of the drug class and disease pathophysiology 4.…”
Section: Introductionmentioning
confidence: 99%
“…A biomarker is defined as a characteristic that can be objectively measured and evaluated as an indicator of normal biological processes, pathogenic processes or pharmacological responses to a therapeutic intervention 1, 2. Clinical biomarkers are thought to reflect disease activity and pathophysiology 3, 4. A useful biomarker in any class has to comply with the following general criteria: (i) there must be a consistent response of the biomarker across studies (preferably from different research groups) and drugs from the same mechanistic class; (ii) the biomarker must respond clearly to therapeutic (not supratherapeutic) doses; (iii) there must be a clear dose‐ or concentration‐response relationship; and (iv) there must a plausible relationship between the biomarker, pharmacology of the drug class and disease pathophysiology 4.…”
Section: Introductionmentioning
confidence: 99%
“…For within-day, the percentage differences measured (5.0% average for M30 and 4.1% average for M65) were within, or at least close to, the normal levels of variability associated with the methods indicating a comparatively small contribution from the biomarker itself. These data are in contrast to many typical plasma PD assays which are often associated with 30% or greater imprecision (Miller et al, 2001;Lee et al, 2005).…”
Section: Within-day and Between-day Variability In Baseline Values Ofmentioning
confidence: 59%
“…During that study method validation was conducted in accordance with available internationally recognised bioanalytical guidelines established by the pharmaceutical industry, but primarily utilised in drug and safety monitoring (Shah et al, 2000;Miller et al, 2001). There is a growing acknowledgement that these guidelines are not sufficiently flexible to accommodate the many different categories of PD assays that are employed during anticancer drug development of molecularly targeted agents (Lee et al, 2005). It is now also evident that qualification of a biomarker is a multistage process requiring a concerted team effort often paralleling the drug development cycle (Colburn, 2003;Benowitz, 2004;Ransohoff, 2004;Ludwig and Weinstein, 2005).…”
mentioning
confidence: 99%
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“…(Fig. 6) The fit‐for‐purpose, iterative approach was applied to the validation strategy in that, as the intended use of the data and the associated regulatory requirements changed, the assay was re‐optimized and re‐validated appropriately 24, 25, 26. The prototype assay was developed during the drug discovery phase and initially used to detect binding of anti‐SEMA4D candidates to cellular SEMA4D.…”
Section: Discussionmentioning
confidence: 99%