Sage Journals: Discover world-class research

Abstract

Background/Aims

The quality of the evidence used to evaluate a drug’s safety and efficacy depends, in part, on how well participants adhere to the prescribed drug-taking regime. There are multiple approaches to measure adherence in clinical trials, varying in their cost and accuracy. We demonstrate a method for evaluating the cost-effectiveness of common adherence monitoring methods, considering the costs and data quality for drugs that differ in how forgiving they are of nonadherence.

Methods

We propose a simulation approach to estimate the value of evidence about adherence, considering both costs of collection and potential errors in interpreting clinical trial results. We demonstrate the approach with a simulated clinical trial of nitrendipine, a common calcium channel blocker. We consider two trial designs, one using pretrial adherence to “enrich” the trial sample and one without an enrichment strategy. We use scenarios combining high and low values of two key properties of a clinical trial: participant adherence and drug forgiveness.

Results

Under the conditions of these simulations, the most cost-effective adherence monitoring approach depends on both trial participant adherence and drug forgiveness. For example, the enrichment strategy is not cost-effective for the base scenario (high forgiveness and high adherence), but is for other scenarios. We also estimate the effects of evaluable patient analysis, a controversial procedure that excludes nonadherent participants from the analyses, after a trial is completed.

Conclusions

Our proposed approach can guide drug regulators and developers in designing efficient clinical trials and assessing the impact of nonadherence on trial results. It can identify cost-effective adherence-monitoring methods, given available knowledge about the methods, drug, and patients’ expected adherence.

Keywords

Adherence monitoring simulation trial enrichment clinical trial design cost-effectiveness digital medicine FDA

Get full access to this article

View all access options for this article.

References

Blaschke

Osterberg

Vrijens

, et al. Adherence to medications: insights arising from studies on the unreliable link between prescribed and actual drug dosing histories. Annu Rev Pharmacol Toxicol 2012; 52: 275–301.

Checchi

Huybrechts

Avorn

, et al. Electronic medication packaging devices and medication adherence: a systematic review. JAMA 2014; 312(12): 1237–1247.

FDA. Center for drug evaluation and research application number: 021752Orig1s030. Medical review(S), 2012, https://www.accessdata.fda.Gov/drugsatfda_docs/nda/2012/021752Orig1s030MedR.pdf (accessed 12 June 2019).

Vrijens

Gross

Urquhart

. The odds that clinically unrecognized poor or partial adherence confuses population pharmacokinetic/pharmacodynamic analyses. Basic Clin Pharmacol Toxicol 2005; 96(3): 225–227.

FDA and CDER. Enrichment strategies for clinical trials to support determination of effectiveness of human drugs and biological products guidance for industry, 2019, https://www.fda.gov/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/default.htm; and/or https://www.fda.gov/BiologicsBloodVaccines/GuidanceComplianceRegulatoryInformation/Guidances/default.htm (acces-sed 11 June 2019).

Fralick

Avorn

Franklin

, et al. Application and impact of run-in studies. J Gen Intern Med 2018; 33(5): 759–763.

Laursen

DRT

Paludan-Müller

Hróbjartsson

. Randomized clinical trials with run-in periods: frequency, characteristics and reporting. Clin Epidemiol 2019; 11: 169–184.

Sommer

Zeger

. On estimating efficacy from clinical trials. Stat Med 1991; 10(1): 45–52.

Dodd

White

Williamson

. Nonadherence to treatment protocol in published randomised controlled trials: a review. Trials 2012; 13(1): 84.

10.

Rehal

Morris

Fielding

, et al. Non-inferiority trials: are they inferior? A systematic review of reporting in major medical journals. BMJ Open 2016; 6(10): e012594.

11.

FDA. Good review practice: clinical review of investigational new drug applications, 2013, https://www.fda.gov/media/87621/download (accessed 30 September 2019).

12.

Farmer

. Methods for measuring and monitoring medication regimen adherence in clinical trials and clinical practice. Clin Ther 1999; 21(6): 1074–1090; discussion 1073.

13.

Hamilton

. Measuring adherence in a hypertension clinical trial. Eur J Cardiovasc Nurs 2003; 2: 219–228.

14.

Vrijens

Urquhart

. Methods for measuring, enhancing, and accounting for medication adherence in clinical trials. Clin Pharmacol Ther 2014; 95(6): 617–626.

15.

Sherbourne

Hays

Ordway

, et al. Antecedents of adherence to medical recommendations: results from the medical outcomes study. J Behav Med 1992; 15(5): 447–468.

16.

El Alili

Vrijens

Demonceau

, et al. A scoping review of studies comparing the medication event monitoring system (MEMS) with alternative methods for measuring medication adherence. Br J Clin Pharmacol 2016; 82(1): 268–279.

17.

FDA. K183052 510(k) summary, 2019, https://www.accessdata.fda.gov/cdrh_docs/pdf18/K183052.pdf

18.

FDA. Evaluation of automatic class III designation (DE NOVO) for proteus personal monitor including ingestion event marker: K113070, 2012, https://www.accessdata.fda.gov/cdrh_docs/reviews/K113070.pdf

19.

Nitrendipine—DrugBank, https://www.drugbank.ca/drugs/DB01054 (accessed 19 December 2019).

20.

Fellows

Stoneking

Ramanathan

. Bayesian population modeling of drug dosing adherence. J Pharmacokinet Pharmacodyn 2015; 42(5): 515–525.

21.

Mathes

Jaschinski

Pieper

. Adherence influencing factors—a systematic review of systematic reviews. Arch Public Health 2014; 72(1): 37.

22.

Ota

Ishii

Tsuda

, et al. A model-based comparative meta-analysis of the efficacy of dolutegravir-based and efavirenz-based regimens in HIV-infected patients. J Infect Chemother 2019; 25(9): 687–694.

23.

De Geest

Zullig

Dunbar-Jacob

, et al. ESPACOMP medication adherence reporting guideline (EMERGE). Ann Intern Med 2018; 169(1): 30–35.

24.

Vrijens

De Geest

Hughes

, et al. A new taxonomy for describing and defining adherence to medications. Br J Clin Pharmacol 2012; 73(5): 691–705.

25.

Locatelli

Grabnar

Belič

, et al. Pharmacokinetic-pharmacodynamic modelling of side effects of nitrendipine, 2002, https://pdfs.semanticscholar.org/8f7c/8b2147342832c4c9a30a9b5715e77b68250a.pdf (accessed 18 September 2019).

26.

Shimada

Nakajima

Yamamoto

, et al. Comparative pharmacodynamics of eight calcium channel blocking agents in Japanese essential hypertensive patients. Biol Pharm Bull 1996; 19(3): 430–437.

27.

Cramer

Mattson

Prevey

, et al. How often is medication taken as prescribed?: A novel assessment technique. JAMA 1989; 261(22): 3273–3277.

28.

Browne

Umlauf

Tucker

, et al. Wirelessly observed therapy compared to directly observed therapy to confirm and support tuberculosis treatment adherence: a randomized controlled trial. PLoS Med 2019; 16(10): e1002891.

29.

Home—ClinicalTrials.gov, https://clinicaltrials.gov/ (accessed 17 December 2019).

30.

Patel

Hayward

Ozdemir

, et al. Magnitude of blood pressure reduction in the placebo arms of modern hypertension trials: implications for trials of renal denervation. Hypertension 2015; 65(2): 401–406.

31.

Battelle Technology Partnership Practice, Pharmaceutical Research Manufacturers of America (PhRMA). Biopharmaceutical industry-sponsored clinical trials: impact on state economies, 2015, www.battelle.org (accessed 6 December 2019).

32.

CPI Inflation Calculator, https://data.bls.gov/cgi-bin/cpicalc.pl (accessed 20 December 2019).

33.

US Food Drug Administration. IRB waiver or alteration of informed consent for clinical investigations involving no more than minimal risk to human subjects: guidance for sponsors, investigators, and institutional review boards, 2017, https://www.fda.gov/regulatory-information/search-fda-guidance-documents/irb-waiver-or-alteration-informed-consent-clinical-investigations-involving-no-more-minimal-risk

34.

Senn

. Are placebo run ins justified? BMJ Br Med J 1997; 314(7088): 1191–1193.

35.

Mann

. Deception in the single-blind run-in phase of clinical trials. IRB 2007; 29(2): 14–17.

36.

Merrill

McClure

. Dichotomizing partial compliance and increased participant burden in factorial designs: the performance of four noncompliance methods. Trials 2015; 16: 523.

37.

Little

Long

Lin

. A comparison of methods for estimating the causal effect of a treatment in randomized clinical trials subject to noncompliance. Biometrics 2009; 65(2): 640–649.

38.

Davis

Applegate

Gordon

, et al. An empirical evaluation of the Placebo Run-in. Control Clin Trial 1995; 16(1): 41–50.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.10 MB

The value of adherence information during clinical pharmaceutical trials

Abstract

Background/Aims

Methods

Results

Conclusions

Keywords

Get full access to this article

References

Supplementary Material