The Power of Phase I Studies to Detect Clinical Relevant QTc Prolongation: A Resampling Simulation Study

Concentration-effect (CE) models applied to early clinical QT data from healthy subjects are described in the latest E14 Q&A document as promising analysis to characterise QTc prolongation. The challenges faced if one attempts to replace a TQT study by thorough ECG assessments in Phase I based on CE models are the assurance to obtain sufficient power and the establishment of a substitute for the positive control to show assay sensitivity providing protection against false negatives. To demonstrate that CE models in small studies can reliably predict the absence of an effect on QTc, we investigated the role of some key design features in the power of the analysis. Specifically, the form of the CE model, inclusion of subjects on placebo, and sparse sampling on the performance and power of this analysis were investigated. In this study, the simulations conducted by subsampling subjects from 3 different TQT studies showed that CE model with a treatment effect can be used to exclude small QTc effects. The number of placebo subjects was also shown to increase the power to detect an inactive drug preventing false positives while an effect can be underestimated if time points aroundtmaxare missed.

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The Role of Socioeconomic Conditions and Psychological Factors in the Willingness to Volunteer for Phase I Studies

Pharmaceutical Medicine ◽

10.1007/bf03256734 ◽

2008 ◽

Vol 22 (6) ◽

pp. 367-374 ◽

Cited By ~ 2

Author(s):

Luis Almeida ◽

Amílcar Falcão ◽

Rui Coelho ◽

António Albino-Teixeira ◽

Patrício Soares-da-Silva

Keyword(s):

Phase I ◽

Psychological Factors ◽

Socioeconomic Conditions ◽

Phase I Studies

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Role of pharmacogenetic studies in early clinical development: Phase I studies with lapatinib

Journal of Clinical Oncology ◽

10.1200/jco.2006.24.18_suppl.3029 ◽

2006 ◽

Vol 24 (18_suppl) ◽

pp. 3029-3029 ◽

Cited By ~ 9

Author(s):

T. Z. Zaks ◽

A. Akkari ◽

L. Briley ◽

M. Mosteler ◽

A. G. Stead ◽

...

Keyword(s):

Phase I ◽

Healthy Volunteers ◽

Kinase Inhibitor ◽

Clinical Development ◽

Pharmacokinetic Data ◽

Nucleotide Polymorphisms ◽

Single Nucleotide ◽

Phase I Studies ◽

Clinical Drug Development

3029 Background: Rash and diarrhea are a class effect of ERBB1 inhibitors. These events are relatively mild with Lapatinib (a dual ERBB1/ERBB2 kinase inhibitor). Finding a genetic basis for patients who may be predisposed to these adverse events, from the outset of clinical development, may improve the understanding of the mechanisms of these side effects and may have implications for use and dosing. Methods: DNA was isolated from peripheral blood of 107 Caucasian subjects from eight monotherapy phase I studies including 73 healthy volunteers and 34 cancer patients, 100 of whom had associated pharmacokinetic data. 284 single nucleotide polymorphisms (SNPs) from five candidate genes of transporters (ABCB1, ABCG2) and enzymes (CYP 3A4 and 3A5, and 2C19) for which lapatinib is a substrate were genotyped and examined for associations with pharmacokinetic variables (dose-normalized AUC, Cmax, and Tmax) as well as rash (15 cases) and diarrhea (18 cases). Results: Skin rash and diarrhea in this phase I cohort were only mild, (i.e. grade I or II). Statistically significant associations were observed between 34 SNPs in CYP2C19, rash (22 SNPs) and diarrhea (6 SNPs), and between 15 SNPs in ABCB1 and Tmax. Notably, 3/3 subjects (2 healthy volunteers, one patient) homozygous for the CYP2C19*2 allele experienced both mild rash and diarrhea. Extensive linkage disequilibrium was observed among these associated SNPs. Conclusions: Our results suggest that it is possible to determine pharmacogenetic associations with side effect phenotypes during the earliest phase of clinical drug development. These results are currently being validated on a larger cohort of patients from phase II lapatinib clinical trials. [Table: see text]

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