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Observational Study
. 2025 Aug 12;36(6):373-381.
doi: 10.1515/jbcpp-2024-0104. eCollection 2025 Nov 1.

A cross-sectional observational study of the prevalence and characterization of potential QT-prolonging drug‒drug interactions in oncological outpatients

Akash Agnihotri  1 Biswadeep Das  2 Sachin Manocha  1 Manjunath Bidarolli  1 Bharati Vashisht  3
Affiliations
Observational Study

A cross-sectional observational study of the prevalence and characterization of potential QT-prolonging drug‒drug interactions in oncological outpatients

Akash Agnihotri et al. J Basic Clin Physiol Pharmacol. .

Abstract

Objectives: This study aims to assess the prevalence, characteristics, and risk factors of potential QT-prolonging drug-drug interactions (pQT-DDIs) in cancer patients, including identifying drug combinations contributing to QT prolongation and key predictors.

Methods: In this hospital-based, cross-sectional observational study, all types of cancer patients, irrespective of age or sex, were included over 1 year. pQT-DDIs were identified using four drug interaction checker software tools. Predictors were analyzed using univariate logistic regression.

Results: A total of 1,331 cancer patients were included. The prevalence of pQT-DDIs was 67.6 %. Of these, 606 (45.5 %) had 1-2 pQT-DDIs, 126 (9.5 %) had 3-4, and 78 (5.9 %) had 5-6. Overall, 163 drug combinations were identified as causing QT prolongation; 122 were detected by Drugs.com. Significant predictors included >8 drugs prescribed (OR=6.46; CI=4.87-8.56; p<0.0001), >2 anticancer drugs (OR=1.68; CI=1.14-2.46; p=0.008), >6 adjuvant drugs (OR=6.83; CI=5.17-9.03; p<0.0001), solid cancers (OR=6.59; CI=4.59-8.80; p<0.0001), and cytotoxic drug use (OR=2.40; CI=1.52-3.77; p=0.0001).

Conclusions: There is a high prevalence of pQT-DDIs in cancer patients. Those receiving multiple anticancer and adjuvant drugs are at higher risk. Routine interaction screening is recommended before chemotherapy.

Keywords: QT prolongation; anticancer drugs; drug–drug interactions; polypharmacy.

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References

    1. Siegel, RL, Giaquinto, AN, Jemal, A. Cancer statistics, 2024. CA Cancer J Clin 2024;74:12–49. https://doi.org/10.3322/caac.21820 . - DOI
    1. Wondm, SA, Tamene, FB, Gubae, K, Dagnew, SB, Worku, AA, Belachew, EA, et al.. Potential drug–drug interaction and its determinants among patients with cancer receiving chemotherapy in oncology centres of northwest Ethiopia: an institutional-based cross-sectional study. BMJ Open 2023;13:e077863. https://doi.org/10.1136/bmjopen-2023-077863 . - DOI
    1. van Leeuwen, RWF, Brundel, DHS, Neef, C, van Gelder, T, Mathijssen, RHJ, Burger, DM, et al.. Prevalence of potential drug–drug interactions in cancer patients treated with oral anticancer drugs. Br J Cancer 2013;108:1071–8. https://doi.org/10.1038/bjc.2013.48 . - DOI
    1. Cuni, R, Parrini, I, Asteggiano, R, Conte, MR. Targeted cancer therapies and QT interval prolongation: unveiling the mechanisms underlying arrhythmic complications and the need for risk stratification strategies. Clin Drug Invest 2017;37:121–34. https://doi.org/10.1007/s40261-016-0460-5 . - DOI
    1. Porta-Sánchez, A, Gilbert, C, Spears, D, Amir, E, Chan, J, Nanthakumar, K, et al.. Incidence, diagnosis, and management of QT prolongation induced by cancer therapies: a systematic review. J Am Heart Assoc Cardiovasc Cerebrovasc Dis 2017;6:e007724. https://doi.org/10.1161/jaha.117.007724 . - DOI

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