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Abstract

Rationale:

Drug-drug interactions (DDIs) with oral antineoplastics (OAs) are of increasing concern given the rapid increase in OA approvals and use in cancer patients. A small pilot study of 20 DDIs with OAs showed significant variability in commonly used DDI screening databases in sensitivity of detecting potentially clinically relevant DDIs. This study builds upon that work by expanding the number of potential DDIs analyzed and including a specificity analysis.

Methods

Newly approved OAs from 2016 to May 2019 (n = 22) were included in this analysis. Prescribing information for each drug was reviewed. A list of explicit and theoretical drug interactions was created for each OA by the two investigators. A board-certified oncology pharmacist adjudicated all DDI pairs for potential clinical significance. In total, 229 DDI pairs were used to analyze sensitivity of 5 DDI databases (Lexicomp®, Micromedex®, Medscape, Eporactes®, & Drugs.com). Additionally, 64 “dummy” or false DDI pairs were created to analyze specificity. Sensitivity and specific were analyzed using Cochran’s Qtest, while accuracy was analyzed using chi-square test.

Results

There was significant variability among the databases with regards to sensitivity (p < 0.0001), specificity (p < 0.0001), and accuracy (p < 0.0001). In terms of accuracy (max score = 400), Lexicomp®(355), Epocrates® (344), and Drugs.com (352) scored higher than MicroMedex® (270) and Medscape (280).

Conclusions

Considerable variability exists among DDI screening databases with regards to OAs and potential drug interactions. Clinicians should be vigilant in both screening for DDIs with OAs and describing DDIs encountered in clinical practice.

Keywords

Drug interaction database pharmacovigilance oral antineoplastics

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References

Center for Drug Evaluation and Research: New Drugs at FDA, www.fda.gov/drugs/development-approval-process-drugs/new-drugs-fda-cders-new-molecular-entities-and-new-therapeutic-biological-products (accessed 4 May 2020).

Streicher

Daulange

Madranges

, et al. Severe rhabdomyolysis induced by possible drug-drug interaction between ribociclib and simvastatin. J Oncol Pharm Practice. Epub ahead of print 29 July 2020. DOI: 10.1177%2F1078155220945365

Kisqali. Package insert. Basel: Novartis Pharmaceuticals Corp; 2020.

Agarwal

DiNardo

Potluri

, et al. Management of venetoclax-posaconazole interaction in acute myeloid leukemia patients: evaluation of dose adjustments. Clin Ther 2017; 39: 359–367.

Ergun

Ozdemir

Toptas

, et al. Drug-drug interactions in patients using tyrosine kinase inhibitors: a multicenter retrospective study. J Buon 2019; 24: 1719–1726.

Diaz-Carrasco

Almanchel-Rivadeneyra

TomasLuiz

, et al. Observational study of drug-drug interactions in oncological patients. Farm Hosp 2018; 42: 10–15.

Rompelman

Smit

Franssen

, et al. Drug-drug interactions of cytostatics with regular medicines in lung cancer patients. J Oncol Pharm Pract 2017; 23: 483–490.

Ramos-Esquivel

Viquez-Jaikel

Fernandez

Potential drug-drug and herb-drug interactions in patients with cancer: a prospective study of medication surveillance. J Oncol Pract 2017; 13: e613–e622.

van Leeuwen

Jansman

van den Bemt

, et al. Drug-drug interactions in patients treated for cancer: a prospective study on clinical interventions. Ann Oncol 2015; 26: 992–997.

10.

Marcath

Coe

Hoylman

, et al. Prevalence of drug-drug interactions in oncology patients enrolled on national clinical trials network oncology clinical trials. BMC Cancer 2018; 18: 1155.

11.

Keller

Franquiz

Duffy

, et al. Drug-drug interactions in patients receiving tyrosine kinase inhibitors. J Oncol Pharm Pract 2018; 24: 110–115.

12.

Bossaer

Thomas

CT.

Drug interaction database sensitivity with oral antineoplastics: an exploratory analysis. J Oncol Pract 2017; 13: e217–e222.

13.

Vonbach

Dubied

Krahenbuhl

, et al. Evaluation of frequently used drug interaction screening programs. Pharm World Sci 2008; 30: 367–374.

14.

Kheshti

Aalipour

Namazi

A comparison of five common drug-drug interaction software programs regarding accuracy and comprehensiveness. J Res Pharm Pract 2016; 5: 257–2630.

15.

Cometriq [package insert]. Alameda, CA: Exelixis, Inc, www.cometriq.com/downloads/Cometriq_Full_Prescribing_Information.pdf (2020, accessed 8 June 2020).

16.

Cabometyx [package insert]. Alameda, CA: Exelixis, Inc, www.cabometyxhcp.com/pi/ (2020, accessed 8 June 2020).

17.

Miles

Lacy

Wada

, et al. Clinical pharmacokinetics and pharmacodynamics of cabozantinib. Cancer Chemother Pharmacol 2017; 80: 295–306.

18.

Tabrecta [package insert]. East Hanover, NJ; Novartis Pharmaceuticals Corp, www.accessdata.fda.gov/drugsatfda_docs/label/2020/213591s000lbl.pdf (2019, accessed 19 October 2020).

19.

Baldo

Fornasier

Ciolfi

, et al. Pharmacovigilance in oncology. Int J Clin Pharm 2018; 40: 832–841.

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Sensitivity and specificity of drug interaction databases to detect interactions with recently approved oral antineoplastics