Initial dose of tapentadol and concomitant use of duloxetine are associated with delirium occurring after initiation of tapentadol therapy in cancer patients

Takeshi Nakamura; Tomoyoshi Miyamoto; Daisuke Tanada; Rie Nishii; Saki Okamura; Takae Inui; Yoko Doi; Kuniyoshi Tanaka; Mina Yanai; Munetaka Hirose; Takeshi Kimura

doi:10.5055/jom.0859

Authors

Takeshi Nakamura, PhD https://orcid.org/0009-0007-0978-9019
Tomoyoshi Miyamoto, PhD https://orcid.org/0000-0001-5593-1046
Daisuke Tanada, MD
Rie Nishii, MD, PhD
Saki Okamura, BS
Takae Inui, RN, CN
Yoko Doi, RN, CN
Kuniyoshi Tanaka, BS
Mina Yanai, MS
Munetaka Hirose, MD, PhD
Takeshi Kimura, PhD

DOI:

https://doi.org/10.5055/jom.0859

Keywords:

cancer-related pain, delirium, duloxetine, opioid, palliative care, tapentadol

Abstract

Objective: Tapentadol causes fewer gastrointestinal adverse events than other potent opioid analgesics because of its low affinity for opioid receptors; however, development of symptoms related to central nervous system disorders, including delirium, has not been well-studied. This study aimed to identify the factors that influence the development of delirium after initiation of tapentadol therapy in hospitalized patients with cancer.

Design: Retrospective study.

Setting/patients: Among 93 patients, for whom treatment using tapentadol was initiated between December 1, 2017, and November 30, 2019, at a single center in Japan, 86 met the inclusion criteria and were enrolled in this study.

Main outcome measures: Delirium occurring within 2 weeks of initiation of the tapentadol treatment was diagnosed by a physician or nurse. Patient background information was obtained, including data on age, sex, medical history, adverse events, starting dose of tapentadol, and concomitant medications.

Results: Age ≥ 67 years, male sex, somnolence after initiation of tapentadol therapy, dose of ≥300 mg/day at the beginning of tapentadol therapy, switching from potent opioids, and concomitant use of duloxetine were associated with delirium occurring after tapentadol therapy initiation.

Conclusions: Among the factors associated with the incidence of delirium after the initiation of tapentadol therapy, patients whose starting dose of tapentadol was 300 mg/day or higher and those receiving concomitant duloxetine, a serotoninnoradrenaline reuptake inhibitor, were at high risk of developing delirium. These findings will help healthcare providers, including pharmacists, in development of treatment plans for preventing delirium when initiating tapentadol therapy in patients with cancer.

Author Biographies

Takeshi Nakamura, PhD

Department of Pharmacy, Palliative Care Center, Hyogo Medical University Hospital, Hyogo, Japan

Tomoyoshi Miyamoto, PhD

School of Pharmacy, Hyogo Medical University, Hyogo, Japan

Daisuke Tanada, MD

Department of Palliative Medicine, Hannan Chuo Hospital, Osaka, Japan

Rie Nishii, MD, PhD

Palliative Care Center, Department of Neuropsychiatry, Hyogo Medical University Hospital, Hyogo, Japan

Saki Okamura, BS

Department of Pharmacy, Palliative Care Center, Hyogo Medical University Hospital, Hyogo, Japan

Takae Inui, RN, CN

Palliative Care Center, Hyogo Medical University Hospital, Hyogo, Japan

Yoko Doi, RN, CN

Palliative Care Center, Hyogo Medical University Hospital, Hyogo, Japan

Kuniyoshi Tanaka, BS

Department of Pharmacy, Hyogo Medical University Hospital, Hyogo, Japan

Mina Yanai, MS

Department of Pharmacy, Hyogo Medical University Hospital, Hyogo, Japan

Munetaka Hirose, MD, PhD

Palliative Care Center, Department of Anesthesiology and Pain Medicine, Hyogo Medical University Hospital, Hyogo, Japan

Takeshi Kimura, PhD

Department of Pharmacy, Hyogo Medical University Hospital, Hyogo, Japan

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